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Circumferential scouting punch
biopsies to delineate surgical margin for dermatofibrosarcoma protuberans
2 Department of Plastic and Reconstructive Surgery, National
Cheng Kung University Medical College and Hospital, Tainan, Taiwan
3 Department of
Biochemistry and Molecular Biology, National Cheng Kung University Medical
College, Tainan, Taiwan
4
Institute of
Clinical Medicine, National Cheng Kung University Medical College, Tainan,
Taiwan
ARTICLE INFO
Dermatofibrosarcoma
protuberans (DFSP) is an uncommon soft-tissue tumor involving the dermis and
subcutaneous tissue with a high local recurrence rate after standard excision.
Mohs micrographic surgery offers a lower recurrence rate. However, the procedure
requires multiple stages of excision with intraoperative histopathological
mapping, which is time consuming and expensive. We report our experience of
using circumferential scouting punch biopsy technique in five patients to
determine in advance the resection margins for DFSP prior to wide excision.
Multiple 4 mm punches, usually eight in number, were performed 1—2.5 cm around
the palpable borders of DFSP to delineate the resection margins in five
consecutive patients. Tumors were excised at a later date along the margin
defined by these biopsies and the wounds were repaired with skin graft. The
operation was completed in 2 hours in all cases excluding one that required
frozen sections for deep margin. No recurrence was noted 2—10 years after the operations.
The results suggest that circumferential scouting punch biopsies before wide
excision may be an alternative method to define the resection margins for DFSP
when Mohs surgery is not available.
Copyright © 2011, Taiwanese
Dermatological Association.
Published by Elsevier Taiwan
LLC. All rights reserved.
Dermatofibrosarcoma protuberans (DFSP) is an uncommon
cutaneous soft tissue tumor of intermediate malignancy.1 It is characterized by progressive local growth and a
propensity for local recurrence, but rarely metastasizes. Surgical excision can
be challenging due to the invasive nature that results in high local recurrence
rates.2 Recurrence rates of DFSP range from
30% to 60% with surgical margins less than 3 cm, but reduce to a mean of 18%
with resection margins greater than 3 cm.3 However, wide margins may be difficult to obtain for
lesions on the head and neck due to potential tissue loss equals loss of
critical structures. Mohs surgery is a technique of controlled skin cancer
removal by mapping and serial frozen sections of resection margins. Each stage
of tissue removal and microscopic examination is repeated until all margins are
clear of cancer.4-6 Removal of DFSP by Mohs surgery provides
maximal
(T.-W. Wong).
tissue conservation with a lower
recurrence rate (0—6%).3—6 However, Mohs surgeons are not available
in many medical facilities. Moreover, it may require several hours to complete
a large resection by Mohs surgery.7,8 Longer
operation time may increase medical expense.7,8
Without Mohs surgeons in our region, we
tried a different approach by performing multiple punch biopsies around the
tumor in the clinics to determine the resection margins first and then
performed wide excision at a later date. We treated five consecutive DFSP
patients with this approach.
During a 10-year period
(1999—2009), five patients with DFSP (Table
1) underwent circumferential punch biopsies in the clinic
several days before wide excision. We first outlined the tumor border by
palpation, and then performed multiple 4 mm punches, usually eight in number,
at a distance 1—2.5 cm around the palpable border. For the tumor located near
the nipple, two to three rows of punches were carried out in order to preserve
more normal areolar tissue. The punch specimens were processed for routine
histopathology examination. The whole tumor was then excised in a few days in
the
1027-8117/$ — see front matter Copyright © 2011, Taiwanese
Dermatological Association. Published by Elsevier Taiwan LLC. All rights
reserved. doi:10.1016/j.dsi.2011.09.002
|
Patient/Sex/Age
|
Location
|
Size
|
Numbers of punch
|
Resection margin to tumor:
shortest distance/longest distance
|
Operation time
|
Outcome
|
|
1/F/34
|
Right upper chest near
axilla
|
7.3cm x 6.2 cm
|
8
|
2 cm/2 cm
|
2 hours 5 minutes
|
No recurrence at 10 years
|
|
2/M/37
|
Left thigh
|
4.5cm x 3cm
|
8
|
2 cm/2 cm
|
1 hour 50 minutes
|
No recurrence at 9 years
|
|
3/F/30
|
Right breast
|
2.8cm x 1.5 cm
|
17
|
1 cm/2 cm
|
30 minutes
|
No recurrence at 9 years
|
|
4/F/22
|
Right breast
|
3.5cm x 4.2 cm
|
8
|
1.2 cm/2 cm
|
2 hours 4 minutes
|
No recurrence at 3 years
|
|
5/M/48
|
Scalp
|
5.5cm x 4.5 cm
|
8
|
2.5 cm/2.5 cm
|
4 hours 28 minutes*
|
No recurrence at 2 years
|
|
Mean i standard
|
|
4.7 i 1.8 cm x 3.9
|
10 i 4
|
1.7 i 0.6 cm/2.1 i 0.2 cm
|
2 hours 11 minutes ±1 hour
|
6.4 ± 3.6 years
|
|
deviation
|
|
i 1.8 cm
|
|
|
26 minutes
|
|
|
Age: 34 i 10
|
|
|
|
|
|
|
|
* Including 2 hours
waiting for frozen section results during operation.
|
operating room along the lines drawn by connecting the
tumor-free dots determined by punch biopsy. Frozen sections were completed
during operation to check the deep margin when necessary.
Patient 1 was
an otherwise healthy 34-year-old woman who presented with a small scar-like
nodule that had been enlarging slowly for 17 years on her right upper chest
near the axilla (Figure 1A).
Histopathologically, the tumor showed a diffuse, extensive proliferation of
spindle cells throughout the dermis with invasion to the subcutaneous tissue (Figure 1B). The findings were consistent with DFSP. In
this case, we tried photodynamic diagnosis, a technique that utilizes
the preferential accumulation of photosensitizer in tumor cells with a 6-hour
occlusion of 2% 5-aminolevulinic acid (Merck, Darmstadt, Germany) to define the
tumor margin.9 It was based on
the fact that tumor cells tend to accumulate more protoporphyrin IX, the active
metabolic product of 5-aminolevulinic acid, and emits red fluorescence under
Wood’s light excitation.10 However, no
visible fluorescence was detected. The negative results might be attributed to
insufficient transepidermal
delivery of photosensitizer through an intact stratum corneum10 or the deep location of the tumor. Eight
circumferential
4
 |
mm punch biopsies were performed 2 cm beyond the palpable border of the mass (Figure 1C). Patient 2, a 37-year-old man, with a DFSP on his left thigh for 10 years was treated with same technique to delineate the tumor before excision (data not shown).
Patients 3 and 4 had pathology
proven DFSP on the breast (Figures
2 and 3) where maximal preservation of breast tissue was
desirable. In Patient 3, the tumor margin toward the nipple was delineated by
performing a total of seven punch biopsies in three
rows (1 cm, 1.5 cm and 2 cm, respectively) from the tumor (Figure 2A). Additional 10 biopsies were taken 2 cm beyond the palpable tumor margin in other directions. In Patient 4, eight punch biopsies were performed 2 cm from the palpable border of the tumor except for the areola border where the punch was done 1.2 cm from the tumor (number 6, Figure 3B). Patient 5’s DFSP was located on his scalp. There was no palpable lymphadenopathy in the neck, submental and postauricular areas. Computed tomography scan revealed no direct bony destruction from the scalp tumor. Eight punch biopsies were performed with 2.5 cm distance beyond the border of the palpable mass because tumor of this location was reported to be more invasive.11
rows (1 cm, 1.5 cm and 2 cm, respectively) from the tumor (Figure 2A). Additional 10 biopsies were taken 2 cm beyond the palpable tumor margin in other directions. In Patient 4, eight punch biopsies were performed 2 cm from the palpable border of the tumor except for the areola border where the punch was done 1.2 cm from the tumor (number 6, Figure 3B). Patient 5’s DFSP was located on his scalp. There was no palpable lymphadenopathy in the neck, submental and postauricular areas. Computed tomography scan revealed no direct bony destruction from the scalp tumor. Eight punch biopsies were performed with 2.5 cm distance beyond the border of the palpable mass because tumor of this location was reported to be more invasive.11
 |
All biopsy specimens were negative for tumor cells. The tumors were excised along the margin connected by these biopsies and to the depth of fascia except in Patient 5. Frozen section during operation confirmed that the lateral resection margins were free of tumor but the horizontal sections of the tumor base showed tumor invasion into the deep subcutaneous fat. The underlying periosteum was removed. Skin defects were repaired with split thickness skin graft (STSG) in all patients. The total operation times ranged from 30 minutes to 4 hours 28 minutes (mean: 2 hours 11 minutes ±1 hour 26 minutes). The longest operation time was with Patient 5 where a frozen section was required which took 2 hours. No clinical recurrence was noted in all patients during 2 years to 10 years (mean: 6.4 ± 3.6 years) of follow-up after operation.
In this small case series, we
demonstrated that peripheral resection margins of DFSP can be drawn in advance
by multiple punch biopsies around the tumor before performing wide excision in
the operating room. This procedure saved time and the expense of surgery, and
the outcome appeared satisfactory. There is a concern that this scouting punch
biopsy can only check a small fraction of
the lateral margins and does not check the deep margin. However, the purpose of using this scouting biopsy technique is to find a reasonable estimation of resection margins so that maximal tissue preservation can be achieved when Mohs surgery is not available. With this approach, the resection margins of the excised tumor can then be checked by routine histopathological study. If necessary, additional tissue may be excised in a follow-up surgery. Clearly, this scouting punch biopsy technique does not check the deep margin of DFSP, which can be determined by frozen section during surgery when necessary after the tumor has been removed by wide excision. Confirmation of free deep margin is critical in tumors that are associated with increased risk of local recurrence in specific locations, such as the scalp, due to higher incidence of deep tissue involvement.11 This is exemplified in the scalp tumor in Patient 5.
the lateral margins and does not check the deep margin. However, the purpose of using this scouting biopsy technique is to find a reasonable estimation of resection margins so that maximal tissue preservation can be achieved when Mohs surgery is not available. With this approach, the resection margins of the excised tumor can then be checked by routine histopathological study. If necessary, additional tissue may be excised in a follow-up surgery. Clearly, this scouting punch biopsy technique does not check the deep margin of DFSP, which can be determined by frozen section during surgery when necessary after the tumor has been removed by wide excision. Confirmation of free deep margin is critical in tumors that are associated with increased risk of local recurrence in specific locations, such as the scalp, due to higher incidence of deep tissue involvement.11 This is exemplified in the scalp tumor in Patient 5.
Appert et al
reported that multiple scouting biopsies before Mohs micrographic surgery has
been used in extramammary Paget’s disease to define the peripheral surgical
margin.12 In extramammary Paget’s disease, the
tumor infiltration at the periphery primary involves the epidermis. This is in
contrast to DFSP where the tumor infiltrates the dermis and subcutaneous
tissue. The tumor cells in the infiltrating border of DFSP may be few in number
and show little dysplastic changes, thus may be difficult to be differentiate
from normal dermal fibroblasts in hematox- ylin—eosin sections. Even with CD34
staining, it may be difficult to differentiate infiltrating tumor cells from
the normal CD34-positive interstitial dendritic cells and cells around hair
follicles and sweat glands in normal dermis.
For most of our patients,
eight punches were sufficient for delineation of lateral resection margin and
the surgery had been shortened to approximately 2 hours. The surgery time for
Patient 5 was 4.5 hours because of the extra time required for an intraoperative
frozen section to evaluate the deep resection margin and the removal of the
underlying periosteum.
In DFSP, initial
adequate excision is critical because metastasis is invariably preceded by two
or more local recurrences.3 Insidious spread
of a tumor into the clinically normal appearing skin around the tumor is not
uncommon.13 Most surgeons
suggested that a margin of at least 3 cm around the tumor with tissue down to
the fascia should be removed to minimize the risk of recurrence.4 Even with such wide excisions,
recurrence rates from 11% to 20% have been reported.4 The closest margin in our case was 1 cm and no recurrence
has been noted 2—10 years postoperatively (mean 6.4 ± 3.6 years). It is
possible that the favorable outcome in our patients might be because of the
tumors had less infiltrative borders. More case studies are needed before a
definite conclusion can be made. A proposed approach of surgical intervention
of this tumor is shown in Figure 4.
In summary, we reported five patients
with DFSP successfully treated with surgical excision in which the lateral
resection margin was predetermined before excision by scouting punch biopsy
technique in the outpatient clinics. The patients remained tumor free from 2
years to 10 years after tumor excision. The results suggest the lateral
resection margins of DFSP can be determined by this type circumferential
scouting punch biopsy technique in selected tumors when maximal normal skin
preservation is highly desirable and Mohs surgery is unavailable. However,
studies of more cases are needed to evaluate the value of this approach.
2.
Arnaud EJ, Perrault M, Revol M, Servant JM,
Banzet P. Surgical treatment of dermatofibrosarcoma protuberans. Plast Reconstr Surg 1997;100:884—95.
3.
Nelson RA, Arlette JP. Mohs micrographic surgery
and dermatofibrosarcoma protuberans: a multidisciplinary approach in 44
patients. Ann Plast Surg 2008;60:667—72.
4. Ratner
D, Thomas CO, Johnson TM, et al. Mohs micrographic surgery for the treatment of
dermatofibrosarcoma protuberans. Results of a multiinstitutional series with an
analysis of the extent of microscopic spread. JAm Acad Dermatol 1997;37:600—13.
5. Gloster
Jr HM, Harris KR, Roenigk RK. A comparison between Mohs micrographic surgery
and wide surgical excision for the treatment of dermatofibrosarcoma protuberans. J Am Acad Dermatol 1996;35:82—7.
6.
Snow SN, Gordon EM, Larson PO, Bagheri MM, Bentz
ML, Sable DB. Dermatofibrosarcoma protuberans: a report
on 29 patients treated by Mohs micrographic surgery with long-term follow-up
and review of the literature. Cancer 2004;101:28—38.
7. Smeets
NW, Krekels GA, Ostertag JU, et al. Surgical excision vs Mohs’ micrographic
surgery for basal-cell carcinoma of the face: randomised controlled trial. Lancet
2004;364:1766-72.
8.
Essers BA, Dirksen CD, Nieman FH, et al.
Cost-effectiveness of Mohs micrographic surgery vs surgical excision for basal
cell carcinoma of the face. Arch Dermatol
2006;142:187—94.
9.
Becker-Wegerich PM, Fritsch C, Schulte KW, et
al. Carbon dioxide laser treatment of extramammary Paget’s disease guided by
photodynamic diagnosis. Br J Dermatol
1998;138:169-72.
10. Wong
TW, Sheu HM, Lee JY, Fletcher RJ. Photodynamic therapy for Bowen’s disease (squamous
cell carcinoma in situ) of the digit. Dermatol Surg 2001;27:452—6.
11. Loss
L, Zeitouni NC. Management of scalp dermatofibrosarcoma protuberans. Dermatol Surg 2005;31:1428-33.
12. Appert
DL, Otley CC, Phillips PK, Roenigk RK. Role of multiple scouting biopsies
before Mohs micrographic surgery for extramammary Paget’s disease. Dermatol Surg 2005;31:1417-22.
13. Sondak
VK, Cimmino VM, Lowe LM, Dubay DA, Johnson TM. Dermatofibrosarcoma protuberans: what is the best surgical
approach? Surg
Oncol 1999;8:183—9.
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 |
Reports of treating large facial skin cancers by
radiotherapy are scant.1-3 Complete
resolution of a huge exophytic angiosarcoma of the central face could be
achieved by radiotherapy with relapse- free survival of 5 years.3 In this report, we describe two cases of
large squamous cell carcinoma (SCC) and basal cell carcinoma (BCC) treated by
radiotherapy with good clinical and cosmetic results. Although these tumors
might be amenable to conventional surgery or Mohs micrographic surgery followed
by reconstruction surgery, the cosmetic and functional outcomes may not be
satisfactory.
An 88-year-old woman was referred from a
local hospital for a 4.5 cm x 3.0 cm
dehiscent wound after wide excision of a moderately differentiated squamous
cell carcinoma 2 weeks earlier (Figure 1A). Examination revealed intense inflammation
of the right cheek with multiple keratotic tumors near or contiguous to
the ulcer. Considering the extent of tumor involvement, the size of dehiscent
wound and old age of the patient, radiotherapy was suggested. A computed
tomography scan for tumor staging revealed residual tumor mass up to 2.0 cm in
diameter with focal skin thickening without invasion of deeper tissues or
metastasis. The radiation field included the gross tumor, the neighboring area
of skin thickening and a 1.5-cm free margin. Using intensity-modulated
radiation therapy, a total dose of 7000 cGy (in 200 cGy daily fraction) by 6
MV photons was initiated. Substantial clinical improvement was noted after
eight fractions (1600 cGy administered) (Figure
1B), and a complete healing of the ulcer with resolution of
the tumors and inflammation was noted 6 weeks postradiotherapy (Figure 1C). There was no tumor
recurrence at a 15- month follow-up.
 |
A 42-year-old woman presented with a 10-year history of a slowly enlarging keloid-like tumor with a shiny, nodular surface and telangiectasia (Figure 2A). The tumor was 2.5 cm x 3.0 cm x 0.4 cm in size, and occupied the entire left nasolabial area, including the
philtrum and vermilion border of the upper lip with partial
obstruction of the nostril. A skin biopsy revealed nodular basal cell carcinoma
extending to the dermo-subcutaneous junction. The patient opted for
radiotherapy. The radiation field encompassed a 2-cm free margin around the
tumor with a customized Ceroband® block to shield the right nasal alar
cartilage and lower lip. Radiation therapy with 6 MeV electrons was prescribed
to an 80% depth to a total dose of 7000 cGy in 200 cGy daily fractions. After
radiotherapy, the tumor resolved completely with residual scarring. There was
no local recurrence at a 2.5-year follow-up (Figure
2B).
Radiation therapy is an important
treatment modality for nonmelanoma skin cancers (NMSC), especially in cases
where surgery, cryotherapy, electrodesiccation and topical chemotherapy are constrained
by the tumor’s size, depth or location (such as the lip, ear, nose and
periorbital region) or the patient’s age, medical co-morbidity or personal
preference.
Radiation
therapy for cutaneous malignancy has declined in recent decades because of
drawbacks (such as radiodermatitis and radiation-induced malignancy), and the
advent of other therapeutic modalities. However, the risk of radiodermatitis
and radiation-induced malignancy has been much reduced with modern and
fractionated radiation therapy. This treatment option is often overlooked by
dermatologists nowadays, and radiotherapy is more commonly administered as an
adjuvant therapy in highrisk
NMSC or when tumor-free margins are inadequate.
For the
treatment of BCC, surgery appears to have the lowest recurrence or failure
rates, and thus is more effective than radiotherapy according to a Cochrane
Review.4 Nevertheless, radiotherapy is a good option
for elderly patients with tumors on the mid-face, including the nose, inner
canthus and lower eyelid.1 In a series
of 115 previously untreated or recurrent basal cell carcinomas treated with
radiation therapy, the local control rates at
5 years were
95% for the stage I and II tumors and 56% for the stage III and IV tumors.5 The authors concluded that radiation
therapy can achieve high cure rates for stage I and II basal cell carcinomas
and is a relatively effective method for treating recurrent basal cell
carcinomas, with cure rates surpassed only by Mohs micrographic surgery.5
In cases of SCC,
radiotherapy can be a definitive treatment option when considering cosmetic
appearance and function, but high-risk SCC should ideally be excised with the
aim to obtain adequate margins.1 In the guidelines
proposed by the National Comprehensive Cancer Network for treating SCC, wide
excision (10-mm margins if achievable) or Mohs micrographic surgery are
recommended for high-risk tumors (>4 mm in thickness, Clark level IV to V,
moderate to poor differentiation, presence of perineural invasion and
recurrent tumors). Radiotherapy is kept as an adjuvant treatment if clinically
warranted.6
No randomized
controlled trials (RCT) have examined the effectiveness of radiotherapy in
comparison with other treatments for SCC,7 and there was only one RCT comparing surgical excision
with frozen-section margin control to radiotherapy in primary facial BCC. 8 According to recent statistical data,
the 5-year recurrence rates of Mohs surgery and the standard excision were 1%
and 5.3% respectively for BCC, and 3% and 8% respectively for SCC.9 In comparison, radiotherapy alone had
higher 5-year recurrence rates of 7 to about 10% for both BCC and SCC.7 Further clinical follow-up data from
604 cases of BCCs and 104 cases of SCCs treated by office-based radiation
therapy showed 5-year cure rates of 92.7% and 94.4%, respectively, and attained
78.6% to about 84% cure rates in 15 years.10
In our first patient, the treatment posed
a significant challenge because of the large dehiscent wound and the presence
of multiple SCCs on the face. Radiotherapy was considered, but there was a
concern for poor skin tolerance because of the severe atrophy and inflammation.
To our surprise, the wound healed rapidly with resolution of the tumors and
inflammation. In our second patient, the large BCC was located in a
cosmetically and functionally critical area of the face. Disfigurement would be
inevitable even if the tumor were excised by tissue-sparing micrographic
surgery followed by reconstructive surgery. The two cases illustrated that
modern fractionated radiation therapy can be an effective alternative to
surgery with good cosmetic results in treating large, disfiguring facial
tumors.
Yi-Pei
Lee, J. Yu-Yun Lee* Department of
Dermatology, National Cheng Kung University, College of Medicine and Hospital,
Tainan, Taiwan
Helen H.W. Chen
Department
of Radiation Oncology, National Cheng Kung University, College of Medicine and
Hospital, Tainan, Taiwan
Tak-Wah Wong
Department
of Dermatology, National Cheng Kung University, College of Medicine and
Hospital, Tainan, Taiwan
Forn-Chia Lin, Yuan-Hua Wu
Department
of Radiation Oncology, National Cheng Kung University, College of Medicine and
Hospital, Tainan, Taiwan
* Corresponding
author. J. Yu-Yun Lee, 138 Sheng-Li Road, Tainan, Taiwan Tel.: +886 6 2004326;
fax: +886 6 2766180.
1. Veness
MJ. The important role of radiotherapy in patients with non-melanoma skin
cancer and other cutaneous entities. J Med Imaging Radiat
Oncol 2008;52: 278-86.
2. de
Giorgi V, Sestini S, Campolmi P. Radiotherapy for giant squamous cell carcinomas.
Int J Dermatol
2007;46(5):546-7.
3. Gkalpakiotis
S, Arenberger P, Vohradnikova O, Arenbergerova M. Successful radiotherapy of
facial angiosarcoma. Int J Dermatol
2008;47(11):1190-2.
4. Bath
FJ, Perkins W, Bong J, Williams HC. Interventions for basal cell carcinoma of
the skin (Cochrane review). Cochrane Database Syst
Rev 2007;1: CD003412.
5. Wilder
RB, Kittelson JM, Shimm DS. Basal cell carcinoma treated with radiation
therapy. Cancer
1991;68(10):2134-7.
6. Miller
SJ. The National Comprehensive Cancer Network (NCCN) Guidelines of care for
nonmelanoma skin cancers. Dermatol Surg
2000;26:289-92.
7.
Liegeois NJ, Seo SJ, Olbricht S. Squamous cell
carcinoma. In: Williams H, Bigby M, Diepgen T, Herxheimer A, Naldi L,
Rzany B, editors. Evidence-based
dermatology. 2nd ed. London: BMJ Books; 2008. p. 248-55.
8.
Bath-Hextall F, Perkins W. Basal cell carcinoma.
In: Williams H, Bigby M, Diepgen T, Herxheimer A, Naldi L, Rzany B, editors. Evidence-based dermatology. 2nd ed.
London: BMJ Books; 2008. p. 256-71.
9.
Neville JA, Welch E, Leffell DJ. Management
of nonmelanoma skin cancer in 2007. Nat Clin Pract Oncol
2007;4:462-9.
10. Hernández-Machin B, Borrego L, Gil-García
M, Hernández BH. Office-based radiation
therapy for cutaneous carcinoma: evaluation of 710 treatments. Int J Dermatol 2007;46:453-9.
Received:
Jan 17, 2011 Revised: May 5, 2011 Accepted: May 10, 2011
Contents lists available
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1 Department of Dermatology, National Cheng Kung University
Medical College and Hospital, Tainan, Taiwan
3 Department of Biochemistry and Molecular Biology, National
Cheng Kung University Medical College, Tainan, Taiwan
ABSTRACT
Background/Objectives:
Recently, fibrotic diseases such as hypertrophic scar, keloid, and scleroderma
have been treated with UV-A1 radiation with encouraging results. However,
conventional UV light sources are bulky and expensive. In this study, we aimed
to verify the effectiveness of a portable UV-A1 radiation device in treating
hypertrophic scars.
Materials and methods:
A light-emitting diode array that emitted 365 ± 5 nm (UV-A1) was used to
irradiate fibroblasts and hypertrophic scar in a rabbit model.
Results: In cell
cultures, UV-A1 light exposure inhibited post-wound cell migration and reduced
the total amount of soluble collagen production in fibroblasts. Type I
collagenase production and its activity increased after treatment. On the
rabbit ear, UV-A1 light irradiation reduced the thickness of hypertrophic
scars, confirming the antifibrotic effect in
vivo.
Conclusion: These
results support the potential of a portable UV-A1 light device in treating
hypertrophic scar.
Copyright © 2014, Taiwanese
Dermatological Association. Published by Elsevier Taiwan LLC. All rights
reserved.
Fibrotic diseases in humans,
including lung fibrosis,1 liver
cirrhosis,2 scleroderma,3 and keloid,4-6 occur as a result of deposition of collagen in tissues
or organs due to an imbalance of fibrogenesis and fibrolysis. No effective cure
is available to treat these fibrotic diseases. Immunosuppressive agents are
usually recommended but they may have significant adverse effects.1 For skin fibrosing diseases, a safer
and effective treatment is UV irradiation. UV-A light is an electromagnetic
radiation with a wavelength of 320-400 nm. Phototherapy with UV-A to treat
different skin diseases is usually accompanied by a systemic or topical
photosensitizer to enhance the efficacy of the irradiation.7 The development of a lamp emitting radiation
predominantly in the long-wavelength UV-A1 (340-400 nm), was described in 1981.8
High-dose-UV-A1 irradiation without
photosensitizer emerged a decade later to treat atopic dermatitis.9,10
Hypertrophic scars
and keloid result from excessive extracellular matrix deposition in the dermis
after wound healing.6 Hypertrophic
scars are limited to the wound area and usually resolve spontaneously with
time. Keloid is defined as scar tissues growing beyond original wounds and is
challenging to treat. Large scars may cause disfiguration and loss of function
due to scar contracture. Both scars may be complicated with pruritus and pain.11 Traditional scar treatments include
pressure garments, silicone gel sheeting, silicone cream and gel, local steroid
injection, and excision and repair with/without skin graft and/or radiation.5,12 Pressure garments are inconvenient
and uncomfortable especially in tropical and subtropical countries due to humid
and hot weather. Surgical removal of keloid, although temporarily rewarding, is
almost invariably followed by even more aggressive regrowth of scar tis- sue.12 The combination of radiation and
surgery provides a higher success rate to cure keloid. However, long-term
safety has not been established and invasive tumor may develop after this
regimen.13 Intralesional steroid injections are
probably the most common therapy clinically. Many patients are reluctant to
undergo this painful therapy, especially for children and patients with large
keloid.5,14 Recently, UV-A1 has been used in
treating localized15 and
generalized scleroderma16 with
encouraging results. UV-A1
1027-8117/Copyright
© 2014, Taiwanese Dermatological Association. Published by Elsevier Taiwan LLC.
All rights reserved.
Y.-C. Huang et al. / Dermatologica Sinica xxx (2014) 1—5
 |
irradiation has been shown to
stimulate collagenase production by human fibroblasts in vitro.17 Asawanonda et al18 demonstrated that UV-A1 with a cumulative dose of
2860J/cm2 was helpful in treating keloid in a 37-year-old man. The
results were not supported in a subsequent study in which three keloid patients
showed no response after receiving UV-A1 irradiation with cumulative doses of
1500—1800 J/cm2.19 Moreover, the
application of UV-A1 therapy is limited to a few centers because of the large
size and high cost of the machines.20
To develop the application of UV therapy
for larger groups of patients, smaller and more economical UV devices are in
demand. One potential candidate is the light-emitting diode (LED) light source
which has the advantages of portability, high luminance, a relatively narrow
spectrum, long lifespan, and low cost. In fact, LEDs in the visible spectrum
have been applied to phototherapy in several other skin diseases such as wound
healing,21 acne,22 and photodynamic therapy.23 In this study, we tested the efficacy of UV- A1 LEDs
in treating hypertrophic scar on rabbit ear.
Materials and methods UV-A1-LED light source
A commercial UV-A1-LED light source (Figure 1B) composed of 18 LEDs (LH365BG02) in a 5-cm
circle was bought from Clearstone
Technologies Inc. (Hopkins, MN, USA). This device emits wavelengths
of 365 ± 5 nm with a total optical power of 2500 mW. The uniformity and intensity of light
was confirmed by an UV-A meter (UV-Meter HighEnd, Hoenle UV Technology Inc., Grafelfing,
Germany). The light intensity was set at 30 mW/cm2 for in vitro
and 100 mW/cm2 for in vivo experiments by adjusting the
distance from the light source to the treated surface. An electric fan was used
to disperse heat during irradiation.
Cells
Human fetal skin fibroblasts (WS1) were obtained from the Bioresource Collection
and Research Center (BRCB, Taipei, Taiwan) and were maintained in Eagle’s
Minimum Essential Medium supplemented with 10% fetal bovine serum, 2.5 mM
HEPES, and 100 U/mL penicillin/streptomycin at 37°C in 5% CO2.
UV-A1 phototoxicity
in fibroblasts
 |
The purpose of the study was to determine the optimal UV-A1 dose to inhibit scar formation without damaging cells. The phototoxicity of UV-A1 in fibroblasts was determined by exposing cells to different UV doses after seeding 1 x 104 cells in 100 mL medium per well of a 96-well plate for 16 hours. Cell survival was determined with WST-1 assay25 24 hours after treatment. The irradiation dose
that was not phototoxic to cells was selected for further experiments.
Supernatant was collected 24 hours
after treating cells with UV-A1. Total soluble collagen content in the
supernatant was measured with Sircol assay (Biocolor Ltd., Carrickfergus,
Antrim, UK).26 Since type I
collagen is overproduced in keloid and hypertrophic scar,6 we measured type I collagenase (MMPI)26 and its activity27 in the supernatant with ELISA kits
(Biotrak-ELISA System, Amersham, GE Inc., Piscataway, NJ, USA) following the
manufacturer’s instructions.
cm2) while the scars on the other ear served as a
control. The scar thickness was measured with a caliper (Mitutoyo Inc.,
Kawasaki, Japan) and digital images were recorded and assessed by observers
blinded to the study.
One-way analysis of variance
(ANOVA) was used for multiple group comparisons. Unpaired Student’s t test was
used to compare between two groups. Dose dependence was analyzed by linear
regression. At least two separate independent experiments in triplicate were
done for the in
vitro studies. A p value <0.05 was considered
statistically significant.
Cell migration |
Cell migration was assessed by creating a 0.5-mm wound with
a 200-mL pipette tip on the center of a confluent cell sheet.27 Cells were treated with mitomycin C (10
mg/mL) to inhibit cell proliferation for 2 hours at 37° C and 5% CO2
prior to scratching the cell sheet. The damaged area was recorded over time
with a digital camera coupled to a microscope and analyzed with Image-J software
(National Institutes of Health, Bethesda, MD, USA).
Five full-thickness dermal wounds
were created on the ventral site of each ear of three New Zealand white rabbits
(3—6 months of age,
2—
2.5 kg) with a 6-mm punch.28 All
study protocols were in compliance with and approved by the Animal Center
Review Board of the institution. Wounds were left open and hypertrophic scars
formed in 28 days. Scars on one ear were irradiated every 2 days with 150 J/cm2
at 100 mW/cm2 UV-A1 for 30 days (total: 2250 J/
As expected,29 the phototoxicity of UV-A1 on human
fibroblasts was dose dependent (Figure 2A),
with a lethal dose beginning at 9 J/ cm2. We therefore adopted UV
light doses <9 J/cm2 in the rest of the experiments. The main
product of fibrosis, the total collagen content, was reduced by UV-A1
irradiation (40% at 3 J/cm2, p < 0.05; 70% at 6 J/cm2, p <
0.001, one-way ANOVA; Figure 2B).
UV-A1 irradiation enhanced collagenase I production in a dose- dependent manner
(Figure 2C) and improved the enzyme
activity significantly (Figure 2D).
The collagenase I in the supernatant increased 33% at 3 J/cm2 and
44% at 6 J/cm2 compared to the control (p < 0.05, one-way ANOVA; Figure 2C). The enzyme activity
increased 25% at 3 J/cm2 (p < 0.01) and 21% at 6 J/cm2
(p < 0.05), respectively (Figure 2D).
These results demonstrated the anti- fibrotic effects of UV-A1.
Fibroblast migration
may also play a critical role in fibrotic diseases such as active
keloid. In the clinic, keloid spreads beyond the margins of the original wound.
The fibroblasts proliferate, migrate, and lay down collagen on their path and
generate tongue-like fibrotic tissue advancing edges under the microscope.4 Fibroblast migration induced by an
artificial wound in culture was similarly inhibited in a dose-dependent manner
by UV-A1 irradiation (Figure 3).
On the rabbit ear, the minimal dose of UV
radiation producing erythema was 150—200J/cm2 (data not shown). We
therefore chose 150 J/cm2 to test the effect on the scar (n = 15).
After multiple treatments (irradiation every 2 days, cumulative dose 2250 J/cm2),
scar tissue became thinner on Day 20 after the onset of irradiation and the
change of thickness became statistically significant on Day 84 (Figure 4). The treated scars continued to resolve even
after UV therapy was discontinued. The time course of the responses observed in
this study (35—84 days after onset of treatment) was consistent with the slow
response of fibrotic tissues to other forms of treatment.5
|
A 0 J/cm2 3 J/cm2 6 J/cm2
Figure 3 Effects of UV-A1 on fibroblast migration. Fibroblasts
were exposed to different UV-A1 doses after a wound was created on the center
of the cell sheet. Cell migration was inhibited by UV-A1 irradiation in a
dose-dependent manner (A). Data are mean ± standard error of three separate
experiments performed in triplicate (*p < 0.05) (B).
|
|
A B
 |
Day 0 Day 4 Day 20 Day 28 Day 84 Day 112
Figure 4 Efficacy of UV-A1 irradiation on hypertrophic scars. Five
hypertrophic scars were created on each ear in three New Zealand white
rabbits. Control scar (A) was hypertrophic while treated scars were reduced
in thickness (B) after treatment. The p value
was <0.05 compared to the control at 84 days and 112 days after wounding
(C). Bar = 6 mm.
|
 |
Our study demonstrates the beneficial
effects of LED UV-A1 irradiation on hypertrophic scar. The efficacy of this
small portable, inexpensive LED light source on treating fibrosis tissue is
comparable to a large UV-A1 machine.18 Various UV-A1 sources are available, such as
fluorescent lamp cubicles which allow only low (10—30 J/cm2) to
medium (40—70 J/cm2) individual treatment doses to be administered.
High-output metal halide sources allow high doses (up to 130 J/cm2)
for a single treatment session. Low and medium UV-A1 dose shows minimal to
moderate effects in treating atopic dermatitis, and high UV-A1 dose provides
better control of the disease. High UV-A1 dose is particularly promising for
localized scleroderma including widespread, pansclerotic, and linear morphea
because there is no reliable treatment available.30 Setge et al31 showed that a high dose (130 J/cm2
for 30 times, cumulative dose 3900 J/cm2, n = 10)
was more effective than a low dose (20 J/cm2, cumulative dose
600J/cm2, n = 7) of UV-A1 in treating 17 patients with localized
scleroderma. Four of 10 patients in the high-dose group showed complete
clearance. A higher UV-A1 dose is also required for treating keloid.18 The higher dose required for
treating fibrosing diseases suggests the existence of one effective threshold
dose of UV-A1 irradiation, probably higher than 2250 J/cm2. The
thicker collagenous tissue may need a higher light dose to achieve therapeutic
results. It is also likely that an optimal dose may exist along with a temporal
course of treatment in relation to the onset time of scar tissue. In the
present study, hypertrophic scar was treated after it was established. Whether
early UV-A1 intervention prevents hypertrophic scar formation or enhances wound
healing remains to be explored.
 |
This rabbit scar model parallels hypertrophic scar in humans and has been used to study potential therapeutic modalities.28 However, the model cannot study the safety of chronic UV-A1
therapy.9 Patient data on safety such as
carcinogenic effects need to be determined before extensive use of UV-A1 on
humans.9,30 The major acute adverse effects of
UV-A exposure are erythema and pigmentation. The erythema response can be
avoided by giving a minimal erythema dose test before treatment and adjusting
doses according to the response. Pigmentation of the skin is reversible. The
major potential chronic adverse effects are photoaging and skin cancer.32,33 Although it is unclear whether or not
UV-A1 increases the risk of melanoma, a case of cutaneous melanoma diagnosed
after 18 months intensive UV-A1 and psoralen UV-A (PUVA) for urticaria
pigmentosa has been reported. In this report, the total dose of UV-A1 was 910
J/cm2, while the total dose of PUVA was 2144J/cm2. A role
for UV-A in causing malignant melanoma cannot be excluded.34 However, UV-A irradiation causing skin
cancer is not detected in persons who are pigmented, tan easily, or are of
Asian or African ancestry (Fitzpatrick Skin Type IV or higher). The effective
cumulative dose of UV-A1 required for treating keloid in our study was
~2000J/cm2 without psoralen. This treatment may be relatively safe
in our population. Similarly, the risk of UV-A1 inducing non-melanoma skin
cancers, particularly squamous cell carcinoma, is not known, although UV-A
induces squamous cell carcinoma-like tumors in mice.32 Another limitation of our study was the lack of
fibroblasts from human hypertrophic scar for mechanistic studies. Nevertheless,
WS1 fibroblasts are a commercial cell line derived from 12-week gestation
fetal skin. These cells are highly proliferative and senescent around 70
passages. It has been widely used as a model in wound healing studies.35 Hypertrophic scar, unlike keloid,
usually spontaneously resolves with time. In case of limited resources of human
tissue, using WS1 fibroblasts may be an alternative model.
In summary, we showed in in vitro
and in vivo
systems that UV- A1 irradiation using an LED light source was effective in
treating hypertrophic scars. However, the long-term side effects need to be
explored in future experiments.
We thank Professor Paul Poon for comments, Prof. Iain C.
Bruce, Ms. Stephanie Tsao for reading the manuscript, and Ms. Shu-Fen Ko for
technical assistance. The work was supported by Taiwan National Science Council
grant 1002314B006018MY2 to T.-W.W.
1. Nagai S, Handa T, Kim D. Pharmacotherapy in
patients with idiopathic pulmonary fibrosis. Expert Opin Pharmacother
2008;9:1909—25.
3. Chung L, Lin J, Furst DE, Fiorentino D.
Systemic and localized scleroderma. Clin Dermatol 2006;24:374—92.
4. Lee JY, Yang CC, Chao SC, Wong TW.
Histopathological differential diagnosis of keloid and hypertrophic scar. Am J
Dermatopathol 2004;26:379—84.
5. Wong TW, Chiu HC,
Chang CH, Lin LJ, Liu CC, Chen JS. Silicone cream occlusive dressing—a novel
noninvasive regimen in the treatment of keloid. Dermatology 1996;192:329—33.
6. Ehrlich
HP, Desmouliere A, Diegelmann RF, et al. Morphological and immunochemical
differences between keloid and hypertrophic scar. Am J Pathol 1994;145:105—13.
7. Parrish JA,
Fitzpatrick TB, Tanenbaum L, Pathak MA. Photochemotherapy of psoriasis with
oral methoxsalen and longwave ultraviolet light. N Engl J Med 1974;291:1207—11.
8. Mutzhas MF, Holzle E, Hofmann C, Plewig G.
A new apparatus with high radiation energy between 320-460 nm: physical
description and dermatological applications. J Invest Dermatol 1981;76:42—7.
9. KrutmannJ, Czech W, Diepgen
T, Niedner R, Kapp A, Schopf
E. High-dose UVA1 therapy in the treatment of patients with
atopic dermatitis. JAm Acad Dermatol 1992;26:225—30.
10. Gambichler T,
Terras S, Kreuter A. Treatment regimens, protocols, dosage, and indications for
UVA1 phototherapy: facts and controversies. Clin Dermatol 2013;31:438—54.
11. Wong TW, Lee JY, Sheu HM, Chao SC.
Relief of pain and itch associated with keloids on treatment with oxpentifylline.
Br J Dermatol 1999;140:771—2.
12. Gauglitz GG, Korting HC, Pavicic
T, Ruzicka T, Jeschke MG. Hypertrophic scarring and keloids: pathomechanisms and current
and emerging treatment strategies. Mol Med 2011;17:113—25.
13. Fish LM, Duncan L, Gray KD, Bell
JL, Lewis JM. Primary cutaneous melanoma arising in a long-standing irradiated keloid.
Case Rep Surg 2012;2012:165319.
14. Chen YH, Wong TW, Sheu HM, Tsai JC, Li SF.
Iontophoretic local anesthesia to ameliorate
painful intralesional injection in treating keloid. Dermatol Sinica 2001;19:1—7.
15. Gruss C, Reed JA, Altmeyer P, McNutt NS,
Kerscher M. Induction of interstitial collagenase (MMP-1) by UVA-1 phototherapy in
morphea fibroblasts. Lancet 1997;350:1295—6.
16. von Kobyletzki G, Uhle A, Pieck
C, Hoffmann K, Altmeyer P. Acrosclerosis in patients with systemic sclerosis responds to
low-dose UV-A1 phototherapy. Arch Dermatol 2000;136:275—6.
17. Wefers H, Melnik BC, Flur
M, Bluhm C, Lehmann P, Plewig G. Influence of UV irradiation on the composition of human stratum
corneum lipids. J Invest Dermatol 1991;96:959—62.
18. Asawanonda P, Khoo LS, Fitzpatrick TB, Taylor
CR. UV-A1 for keloid. Arch Dermatol 1999;135:348—9.
19. Hannuksela-Svahn A, Grandal OJ, Thorstensen
T, Christensen OB. UVA1 for treatment of keloids. Acta Derm Venereol
1999;79:490.
20. Kerr AC, Ferguson J, Attili SK, et al.
Ultraviolet A1 phototherapy: a British Photodermatology Group workshop report. Clin
Exp Dermatol 2012;37: 219—26.
21. Al-Watban FA, Andres BL. Polychromatic LED in
oval full-thickness wound healing in non-diabetic and diabetic rats.
Photomed Laser Surg 2006;24:10—6.
22. Lee SY, You CE, Park MY. Blue and red light
combination LED phototherapy for acne vulgaris in patients with skin phototype
IV. Lasers Surg Med 2007;39: 180—8.
23. Wong TW, Sheu HM, Lee
JY, Fletcher RJ. Photodynamic therapy for Bowen's disease (squamous cell carcinoma in situ) of
the digit. Dermatol Surg 2001;27: 452—6.
24. Houreld N, Abrahamse H. Irradiation with a
632.8 nm helium-neon laser with 5 J/cm2 stimulates proliferation and expression
of interleukin-6 in diabetic wounded fibroblast cells. Diabetes Technol Ther
2007;9:451—9.
25. Bogdanovic G, Kojic V, Dordevic A,
Canadanovic-Brunet J, Vojinovic- Miloradov M, Baltic VV. Modulating activity of
fullerol C60(OH)22 on doxorubicin-induced cytotoxicity. Toxicol In
Vitro 2004;18:629—37.
26. Keyszer G, Lambiri I, Nagel R, et al.
Circulating levels of matrix metal- loproteinases MMP-3 and MMP-1, tissue inhibitor
of metalloproteinases 1 (TIMP-1), and MMP-1/TIMP-1 complex in rheumatic
disease. Correlation with clinical activity of rheumatoid arthritis
versus other surrogate markers. J Rheumatol 1999;26:251—8.
27. Liang CC, Park AY, Guan JL. In vitro scratch
assay: a convenient and inexpensive method for analysis of cell migration in vitro.
Nat Protoc 2007;2:329—33.
28. Saulis AS, Mogford JH, Mustoe TA. Effect of
Mederma on hypertrophic scarring in the rabbit ear model. Plast
Reconstr Surg 2002;110:177—86.
29. Leccia MT, Richard MJ, Favier A, Beani JC. Zinc
protects against ultraviolet A1- induced DNA damage and apoptosis in cultured
human fibroblasts. Biol Trace Elem Res 1999;69:177—90.
31. Stege H,
Berneburg M, Humke S, et al. High-dose UVA1 radiation therapy for localized
scleroderma. J Am Acad Dermatol 1997;36:938—44.
32. de Laat A, van der Leun JC, de Gruijl FR.
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Contents lists available
at
journal
homepage: http://www.derm-sinica.com
1 Department of Dermatology, National Cheng Kung University
Medical College and Hospital, Tainan, Taiwan 2Department
ofOtolaryngology, National Cheng Kung University Medical College and Hospital,
Tainan, Taiwan
3
Department of
Biochemistry and Molecular Biology, National Cheng Kung University Medical
College, Tainan, Taiwan
ARTICLE INFO
Secondary intention
healing on concave areas of the face may provide acceptable cosmetic outcome
after tumor excision but is underused. We evaluated cosmetic outcome and tumor
recurrence of this technique in 10 patients with nodular basal cell carcinoma
and one patient with basosquamous carcinoma on the face. The average size of
these tumors was 1 cm. Subjective evaluations included patients' satisfaction
on the degree of wound pain, ease of wound care, and satisfaction with cosmetic
outcome. Objective evaluations included physician's scoring on the time to
complete wound healing, wound infection, cosmetic outcome, and tumor recurrence
after operation. The operations were completed in 30 minutes on average. All
wounds healed well without infection within 4 weeks. Postoperation wound pain
was absent to mild. Wound care was neither difficult nor troublesome. All
patients were satisfied with the cosmetic outcome. Physicians scored good or
excellent cosmetic outcome in 91% of patients. No tumor recurred during 3—60
months (median, 13 months) of follow-up. Secondary intention healing appears to
be a good option after excision of nodular basal cell carcinomas located on
concave areas of the face. Good to excellent cosmetic results can be expected
after wound healing.
Copyright © 2012, Taiwanese
Dermatological Association.
Published by Elsevier Taiwan
LLC. All rights reserved.
 |
Introduction
Surgical removal of cutaneous
neoplasms from the head and neck region creates a variety of cutaneous defects
requiring tissue reconstruction. The ideal reconstruction of skin defects aims
to close the defects with good cosmesis and without morbidity. Wound
reconstruction techniques include primary closure; healing by secondary
intention; skin grafts; and local, regional, and sometimes free flaps. The
choice of reconstruction method often depends on the preference and experience
of the surgeon and patients’ expectations.
Healing by
secondary intention offers the advantages of optimal cancer surveillance,
simplified wound management, and avoidance of sophisticated reconstructive
procedures. In the early days of tumor removal using Mohs' fixed tissue
technique, most of the surgical wounds were allowed to heal by secondary
intention.1
Although there are many reports on secondary intention healing
(SIH) in the literature, data with a sound statistical basis are limited.2,3 In 1983, Zitelli4 reviewed facial defects managed by
SIH comprehensively and found that the anatomic location of surgical wounds was
the most important predicting factor for the cosmetic outcome (Figure 1). Wounds
located on the concave surfaces of the nose, eye, ear, and temple areas usually
heal with functional and cosmetic outcomes that equal or are superior to those
achieved by grafts and flap transpositions.4—6 However, SIH is usually underused after surgery. In this
study, we evaluated SIH in 11 patients with basal cell carcinoma on the face.
Patients
and methods Patients
All facial reconstructions after
tumor excision that healed with SIH in one medical center between 1990 and 2010
were reviewed. Photos of patients before and after operation were reviewed from
a database (Crux system) of the department. Eleven patients, eight males and
three females, aged 57—86 years (mean age, 73 years), with nonmelanoma skin
cancers on the face were included
Figure 1 Acceptable cosmetic outcome of
secondary intention healing on a particular anatomic area of the face. The
location of tumors in our patients (red spots) is shown on the figure. Note. From “Wound healing by secondary
intention: a cosmetic appraisal” by JA Zitelli, 1983. J Am Acad Dermatol 9, p 407—15. Adapted with
permission.
|
(Table 1). All
tumors were basal cell carcinoma except for one basosquamous carcinoma that was
confirmed histopathologically. The tumors of 10 patients were located on the
concave areas of the face and one patient’s tumor was on the convex area (Figure 1). The
sizes of the tumors ranged from 0.3 to 3 cm (average, 1 cm) and were noted for
4 months to 10 years (mean, 2.8 years) by the patients before operation. The
benefits and risks of SIH were well explained to patients before surgery.
The facial tumors were excised
with adequate free margins, usually
3— 
5 mm. The skin defect after tumor excision ranged from 1.3 to 4 cm. Primary closure or closure by skin graft or flap were considered to be less ideal than SIH. All patients were instructed to change the wound dressing once daily with topical antibiotic ointment after gentle cleansing with normal saline, and then cover the wound with gauze. All patients were prescribed oral cephalexin and acetaminophen four times daily for 1 week after operation.
5 mm. The skin defect after tumor excision ranged from 1.3 to 4 cm. Primary closure or closure by skin graft or flap were considered to be less ideal than SIH. All patients were instructed to change the wound dressing once daily with topical antibiotic ointment after gentle cleansing with normal saline, and then cover the wound with gauze. All patients were prescribed oral cephalexin and acetaminophen four times daily for 1 week after operation.
The subjective
evaluations included degree of wound pain (none, mild, moderate, and severe);
ease of wound care (easy, fair, difficult, and troublesome); and satisfaction
with cosmetic outcome (satisfied or not satisfied). Objective evaluations,
including time to complete wound healing, wound infection, tumor recurrence,
and cosmetic outcome with photographs using a categorical judgment
scale
(poor, average, good, and excellent), physicians blinded to the study.
were assessed by two
All patients were followed up 3—65
months (median, 13 months) after surgery (Table
1). All tumors were located at concave areas of the face
except for one on the forehead (Figure 2C). One tumor (in patient 4) had been treated with
liquid nitrogen spray and one (in patient 5) had been partially excised at
another clinic.
The operation was
completed in 30 minutes on average. The wounds needed 2—6 weeks (average, 4
weeks) to heal completely. No recurrence of tumor was found during 3—65 months’
(mean, 22.3 months) follow-up.
Postoperative wound care was neither
difficult nor troublesome for all patients (easy in two patients [18.2%] and
fair in nine patients [81.9%]). Analgesic agents other than acetaminophen was
not required because there was no wound pain in seven patients (63.3%) and only
mild pain in four patients (36.4%). No wound infection was observed and all
patients were satisfied with the cosmetic outcome. Objective cosmetic outcome
was good to excellent in 91% of patients (good, 77.3%; excellent, 13.6%) (Figure 2). In
particular, patient 10 had two facial tumors. The tumor on the left nasofacial
sulcus was excised earlier and the wound was closed with primary closure, which
resulted in mild nostril deformity. The tumor on the left nasolabial fold was
left to SIH. Both the patient and surgeon were more satisfied with the cosmetic
result of SIH (Figure 3).
 |
We reported the success and satisfactory results of SIH in a series of patients with basal cell carcinoma of the face after excision. In the current era of elegant and elaborate reconstructive techniques, SIH is often underutilized. However, under certain circumstances, SIH can offer functional and cosmetic outcomes that equal or are superior to those achieved by primary closure, grafts, and flaps.4—6 This simple reconstructive method allows optimal wound bed
surveillance for tumor recurrence with a low complication rate, and the avoidance of complex procedures in patients who are at risk of long operation time.8 However, SIH in anatomic areas with high contractile forces, such as eyelid margins and eyebrow and lip vermilion borders, may result in retraction of free tissue margins. Thus, this technique is not recommended in these anatomic areas. Disadvantages of SIH include prolonged healing time, the need for daily wound care, and occasionally unpredictable cosmetic results.9,10 The cosmetic outcome can only be assessed after complete wound healing.
 |
There are some factors to consider when choosing patients for SIH. Location is probably the most important predictive factor for the esthetic outcome SIH.4,11 Wound contraction is usually more favorable in concave areas. The extent of wound contraction depends on the initial wound size and is positively correlated with the degree of surface concavity, adjacent skin laxity, and the
action of underlying skeletal muscles.12 The favorable outcome in our patients may relate to relatively small tumor sizes in our series (average, 1 cm). A small wound (<1 cm) can heal more than 70% by wound contracture with acceptable cosmetic outcome in comparison with a larger wound (>2.5 cm in diameter).13,14 A superficial defect, even on a convex surface, may also heal with acceptable cosmesis as illustrated by the wound on the forehead in patient 3 (Figure 2C).4,15 Aged skin (in patients with mean age 73 years) may be another factor attributed to a more favorable outcome in our patients. Skin in elderly patients is more relaxed and the presence of irregular contour and pigment can readily camouflage operation scars. Indeed, several authors suggested that elderly patients are better candidates for SIH.5,8,14,15
The traditional
wound dressing for an incisional wound contains three layers — a nonadhering
layer in contact with the wound, an absorptive layer that absorbs wound
exudates, and a binding layer to fix the dressing in place.16 However, the dressings may be too bulky
and cumbersome for patients and the relatively dry environment is not optimal
for wound healing. An occlusive or semiocclusive dressing that provides a moist
healing environment is believed to facilitate wound healing by accelerating
reepithelialization and minimizing desiccation, necrosis, and pain.16,17 For our patients, the goal was a simple
wound dressing that could be done by the patient at home. We educated the
patients on how to clean the wound with normal saline and cover with gauze
after filling the wound with antibiotic ointment. The ointment provides a
semiocclusive environment for the wound. Indeed, all wounds healed without
complications within 4 weeks.
In conclusion, our results suggest that
SIH is a simple technique for wound closure after excision of nodular basal
cell carcinoma if the wound is smaller than 2.5 cm and located over concave
areas of the face. In such clinical settings, SIH proved to be an alternative
for wound closure, with good to excellent cosmetic results.
The study was supported by the National Science Council of
Taiwan grants NSC992627E033001 and NSC1002627E033001 to Dr Tak- Wah Wong.
1.
Mohs FE. Chemosurgery for the microscopically
controlled excision of skin cancer. J Surg Oncol
1971;3:257—67.
3. Shriner
DL, McCoy DK, Goldberg DJ, Wagner Jr RF. Mohs micrographic surgery. J Am Acad Dermatol
1998;39:79—97.
4. Zitelli
JA. Secondary intention healing: an alternative to surgical repair. Clin Dermatol
1984;2:92—106.
5. Moscona
R, Pnini A, Hirshowitz B. In favor of healing by secondary intention after
excision of medial canthal basal cell carcinoma. Plast Reconstr Surg 1983;71:189—95.
7. van
der Eerden PA, Lohuis PJ, Hart AA, et al. Secondary intention healing after
excision of nonmelanoma skin cancer of the head and neck: statistical
evaluation of prognostic values of wound characteristics and final cosmetic
results. Plast
Reconstr Surg 2008;122:1747—55.
8.
Goldwyn RM, Rueckert F. The value of healing by
secondary intention for sizeable defects of the face. Arch Surg 1977;112:285—92.
9.
McGrath MH, Simon RH. Wound geometry and the
kinetics of wound contraction. Plast Reconstr Surg
1983;72:66—73.
10. Cordoro
KM, Russell MA. Minimally invasive options for cutaneous defects: secondary
intention healing, partial closure, and skin grafts. Facial Plast Surg Clin
North Am 2005;13:215—30. v.
11. Diwan
R, Tromovitch TA, Glogau RG, Stegman SJ. Secondary intention healing. The
primary approach for management of selected wounds. Arch Otolaryngol Head
Neck Surg 1989;115:1248—9.
12. Hinrichsen
N, Birk-Sorensen L, Gottrup F, Hjortdal V. Wound contraction in
an experimental porcine model. Scand J Plast Reconstr
Surg Hand Surg 1998;32:243-8.
13. Mott
KJ, Clark DP, Stelljes LS. Regional variation in wound contraction of mohs
surgery defects allowed to heal by second intention. Dermatol Surg 2003;29: 712-22.
14. Lawrence
CM, Comaish JS, Dahl MG. Excision of skin tumours without wound closure. Br J Dermatol 1986;115:563-71.
15. Zitelli
JA. Wound healing by
secondary intention: a cosmetic appraisal. J Am Acad Dermatol 1983;9:407-15.
17. Dziewulski
P, James S, Taylor D, et al. Modern
dressings: healing surgical wounds by secondary intention. Hosp Med
2003;64:543-7.
Contents lists available
at
journal
homepage: http://www.derm-sinica.com
1 Department of Dermatology, National Cheng Kung University
Medical College and Hospital, Tainan, Taiwan
2 Department of Biochemistry and Molecular Biology, National
Cheng Kung University Medical College and Hospital, Tainan, Taiwan
3 Research Center of
Wound Regeneration and Repair, National Cheng Kung University Medical College
and Hospital, Tainan, Taiwan
4 Department of Biology, Marshall College, University of
California San Diego, La Jolla, CA, USA
ABSTRACT
In situ
photoimmunotherapy (ISPI) can be a treatment option for selected cutaneous
malignancies in patients who are not surgical candidates. We herein report the
case of a large, ulcerating poorly differentiated squamous cell carcinoma (SCC)
affecting the foot of an elderly woman with chronic arsenicosis. The tumor
failed radiotherapy, intralesional methotrexate, and 5-aminolevulinic acid
photodynamic therapy (PDT). Because the patient was reluctant to undergo
amputation, the recurrent tumor was treated with ISPI using topical imiquimod
application followed by PDT. Despite some initial improvement in the
superficial part of the tumor, tumor invasion to the underlying bone was
detected. This case illustrates the lack of efficacy of ISIP in treating a
high-risk invasive SCC.
Copyright © 2013, Taiwanese
Dermatological Association.
Published by Elsevier Taiwan
LLC. All rights reserved.
 |
Squamous cell carcinoma (SCC) in
patients with chronic arsenicosis is believed to be more invasive.1 The treatment of choice is surgical
excision.2 However,
alternative treatments may be needed for patients who cannot tolerate or
refuse surgery. Imiquimod is a topical immune modifier acting mainly by
exhibiting agonistic activity toward Toll-like receptors 7 and 8.3 Initially, it was approved to treat
genital and perianal warts. In recent years, imiquimod has been used as a safe
and effective treatment option for a variety of skin cancers including actinic
keratosis, basal cell carcinoma, SCC in situ (Bowen’s disease), lentigo
maligna, and extramammary Paget’s disease.4 Although studies of imiquimod in treating invasive SCC
are limited, some case reports showed encouraging outcomes.5-7 For example, Hengge and Schaller5 treated a 65-year-old man with a 4 cm x 3 cm SCC
on the temple area. The tumor was treated by applying 5% imiquimod cream
overnight three times a week. At week 16, the tumor was cured completely, which
was also confirmed by a histopathological analysis. There was no tumor
recurrence at the 16-month follow-up examination.5
Photodynamic therapy (PDT) destroys tumor
cells by activating a photosensitizer by a specific wavelength of light after
selective accumulation of the photosensitizer in cancer cells.8 In situ photoimmunotherapy (ISPI), which
comprises PDT and topical imi- quimod, has shown promising results in patients
with highly aggressive cancers including metastatic melanoma9,10 and angio- sarcoma.11 A patient with cutaneous metastasizing melanoma
preserved his left foot after ISPI.12 Although there is no report concerning ISPI in
treating invasive SCC, these results encouraged us to treat our patient with
ISPI as a limb-sparing approach.
 |
An 85-year-old female with chronic arsenicosis visited our clinic in 2005 with an 8-year history of chronic nonhealing ulcer over her right dorsal foot. A physical examination revealed a large ulcer (7.2 cm x 5 cm; Figure 1A), which proved to be a poorly differentiated SCC with minimal dermal invasion histopathologically. She refused surgical intervention or chemotherapy but accepted radiation therapy. There was approximately 90% improvement of the tumor (Figure 1B) with re-epithelization after radiotherapy with a total dose of 4000 cGy over 4 months. However, local recurrence with ulceration occurred 3 months later. Both the radiologist and surgeon suggested amputation but the patient refused. She preferred less invasive approaches, such as local chemotherapy and/or PDT. Since then, she has received weekly or biweekly injections of 0.5 mL intratumoral methotrexate (Emthexate, 25 mg/ mL; ASTA Medica Pty Limited, Auckland, Australasia) and PDT. The
PDT was done by occluding the
ulcer with 4% 5-aminolevulinic acid for 6 hours prior to exposing it to 120
J/cm2 at 120 mW/cm2 red light (PDT 1200 lamp; Waldmann, Villingen-Schwenningen, Germany).13 The ulcer showed a partial response
(Figure 1C)
after she received 62 mg methotrexate and 660 J/cm2 over 4 months,
but it relapsed soon after. In an attempt to stimulate host immune response
against the tumor, 250 mg (5%) imiquimod cream (Aldara; 3M Pharmaceuticals, St.
Paul, MN, USA) was evenly applied on the ulcer, which was subsequently occluded
with an air-permeable water-resistant membrane (Tegaderm; 3M Pharmaceuticals)
for 12 hours daily over 12 days. One additional PDT (120 J/cm2) was
performed on Day 6 during imiquimod therapy. She tolerated the treatments well
and the tumor improved clinically (Figure 1D). Regrettably, a follow-up
radiographic examination showed evidence of tumor invasion to the underlying
metatarsal bone, which was intact 5 months prior to ISPI (arrows, Figure 1E and F).
She finally underwent below the knee amputation and was disease free at a
4-year follow-up after surgery.
It is well documented that both
arsenic and human papillomavirus (HPV) are strong carcinogens in humans. A
history of arsenic exposure and HPV seropositivity were associated with
increased nonmelanoma skin cancer risks.14 However, the mechanisms by which HPV and
arsenic interact remain to be established. Even though we did not examine HPV
titer in this patient, it is of interest to investigate the role of HPV in skin
cancer arising in patient with chronic arsenicosis.
Topical imiquimod
without PDT has shown significant efficacy in treating superficial skin
cancers.3 However,
there is a risk of incomplete eradication of the deeper penetrating portion of
the tumor. This can result in the invasion of the underlying bone and cause
bone fracture and bone pain.15 A similar case
of SCC invading the bone of a digit was reported previously.16
ISPI is a new
anticancer therapy, which intends to boost the host immune response against
cancer. This is achieved by the activation of innate and cellular immune responses
with imiquimod when tumor antigens have been generated by tumor cell
destruction with PDT.3 The tumor
antigens are strong and specific. A systemic immune response specifically
against a distant tumor can be elicited by treating a tumor locally with PDT
and imiquimod. The failure of ISPI in our patient might be attributed to the
following reasons. (1) The tumor was naturally less responsive to ISPI. (2) The
absorption peak (635 nm) of the photosensitizer protoporphyrin IX, the active
metabolite of 5-aminolevulinic acid, only penetrates the superficial dermis
leaving the deeper part of the tumor untouched. By comparison, the infrared
absorption peak of indocyanine green used in treating melanomas can penetrate
deeper tissues. The immune responses elicited by ISPI may depend on the dose
and strength of the antigens generated from tumor destruction. The insufficient
destruction of the tumor might have limited the release of tumor antigens in our
patient. It is well known that tumor antigens of malignant melanoma are highly
immunogenic. Melanoma- associated vitiligo is the best studied example of the
linkage between tumor immunity and autoimmunity.17 The tumor antigens of SCC released after ISPI might
not be as immunogenic as in melanoma. The patient had three small Bowen’s
diseases (SCC in
situ) on her trunk. The lesions were treated with cryotherapy and
healed without recurrence prior to ISPI. Otherwise, we could observe the
systemic effects of ISPI. (3) The amount of imiquimod absorbed might not be
sufficient to initiate antitumor immunity. Naylor et al10 did not quantify the amount of imiquimod they used in
ISPI. Nevertheless, they applied 20 cm2 x 20 cm2
imiquimod on their patient’s skin, an area that was approximately three times
larger than our patient.
In conclusion, though ISPI may have
significant efficacy on the treatment of metastatic melanoma, physicians should
be aware of the limitations of ISPI in treating aggressive or deeply invasive
SCCs in which the deeply invasive part of the tumor may be beyond the
penetration limit of ISPI despite positive treatment response in the superficial
part of the tumor.
This work was supported by the Taiwan Science Council grants
(grant nos. NSC992627E033001 and NSC1002627E033001) and the Taiwan Department
of Health grant to establish centers of excellence for cancer research in
Taiwan (grant no. DOH101TDC111003 toT.-W.W.). The authors also thank Dr Michael
W. Hughes for his critical review of this article.
2. Belkin D, Carucci JA.
Mohs surgery for squamous cell carcinoma. Dermatol Clin 2011;29:161—74. vii.
4. Cohen PR, Schulze
KE, Tschen JA, Hetherington GW, Nelson BR. Treatment of extramammary
Paget disease with topical imiquimod cream: case report and literature
review. South Med J 2006;99:396—402.
5. Hengge UR, Schaller J. Successful treatment of
invasive squamous cell carcinoma using topical imiquimod. Arch Dermatol
2004;140:404—6.
6. Nouri K, O’Connell C, Rivas MP. Imiquimod
for the treatment of Bowen’s disease and invasive
squamous cell carcinoma. J Drugs Dermatol 2003;2:669—73.
7. Eklind J, Tartler
U, Maschke J, Lidbrink P, Hengge UR. Imiquimod to treat different cancers
of the epidermis. Dermatol Surg 2003;29:890—6. discussion 896.
8. Zeitouni NC, Oseroff AR, Shieh S. Photodynamic
therapy for nonmelanoma skin cancers. Current review and update. Mol
Immunol 2003;39:1133—6.
9. Li X, Naylor MF, Le H, et al. Clinical effects
of in situ photoimmunotherapy on late-stage melanoma patients: a preliminary
study. Cancer Biol Ther 2010;10: 1081—7.
10. Naylor MF, Chen WR, Teague TK, Perry LA,
Nordquist RE. In situ photoimmunotherapy: a tumour-directed treatment for
melanoma. Br J Dermatol 2006;155:1287—92.
11. Thong PS, Ong KW, Goh NS, et al.
Photodynamic-therapy-activated immune response against distant untreated tumours in
recurrent angiosarcoma. Lancet Oncol 2007;8:950—2.
12. St Pierre SA, Rommel J, Ciurea A, et al. In
situ photoimmunotherapy: a surgery- and limb-sparing approach to the treatment of
cutaneous metastases in advanced melanoma. Arch Dermatol 2010;146:831—4.
13. Wong TW, Sheu HM, Lee JY, Fletcher RJ. Photodynamic
therapy for Bowen’s disease (squamous cell carcinoma in situ) of
the digit. Dermatol Surg 2001;27: 452—6.
14. Rosales-Castillo JA, Acosta-Saavedra LC,
Torres R, et al. Arsenic exposure and human papillomavirus response in non-melanoma
skin cancer Mexican patients: a pilot study. IntArch Occup Environ
Health 2004;77:418—23.
15. Goh MS. Invasive squamous cell carcinoma after
treatment of carcinoma in situ with 5% imiquimod cream. Australas J Dermatol
2006;47:186—8.
DERMATOLOGICA SINICA 28 (2010) 130-132
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|
1,2,3*
|
’Department of Dermatology, National
Cheng Kung University Medical College and Hospital, Tainan, Taiwan
2Department
of Biochemistry and Molecular Biology, National Cheng Kung University Medical
College and Hospital, Tainan, Taiwan 3Institute of Clinical
Medicine, National Cheng Kung University Medical College and Hospital, Tainan,
Taiwan
A 63-year-old retired male teacher presented with
generalized pruritic papules for 4 years. The prurigo was recalcitrant to
treatment and he was admitted for further evaluation and treatment. His medical
history was significant for thyroidectomy for hyperthyroidism 23 years ago
with normal thyroid function after surgery. He had hyperuricemia with gouty
arthritis but received no treatment. He also complained of epigastric
discomfort for several decades. He denied any history of atopy or drug
allergies, and was not on medications before the onset of skin lesions. A
blood examination showed peripheral eosinophilia (1040/mm3). The
serum IgE level was within the normal range. There was no hyperbilirubinemia.
A stool examination showed no evidence of parasite infection. After discharge,
he received treatment at other clinics in his hometown for 7 years.
In 2001, he returned to our clinic because of worsening
of the skin lesions. An examination revealed many licheni- fied and juicy
papules disseminated on his trunk and extremities (Figures 1A-1C). A biopsy
taken from a lichenoid papule showed compact hyperkeratosis, hypergranulosis,
epidermal hyperplasia and fibrotic papillary dermis with dilated blood
vessels, consistent with lichen simplex chronicus or prurigo
histopathologically. The diagnosis of generalized prurigo nodularis was made.
The prurigo showed a poor response to treatments, including topical high
potency steroids, oral antihistamines and narrow band UVB phototherapy. New
lesions continued to erupt despite 18 months of intensive treatments.
Follow-up eosinophil counts were within normal limits. The patient finally gave
up and declined further
^Corresponding author. Department of Dermatology, National Cheng Kung
University Medical College and Hospital, 138 Sheng-Li Rd, Tainan 704, Taiwan.
Received: Jul
27, 2009 • Revised: Oct 5, 2009 • Accepted: Oct 15, 2009
Copyright © 2010, Taiwanese Dermatological Association.
Published by Elsevier Taiwan LLC. All rights reserved.
treatments.
One year after giving up treatments for prurigo, he underwent an endoscopic
retrograde cholangiopancreatography to evaluate his epigastric discomfort. It
revealed a tumor at the ampulla of Vater, which was shown to be an adenoma
pathologically (Figure 2A). Magnetic resonance imaging (Figure 2B) showed a
tumor in the ampulla of Vater region. The patient had no signs of cholestasis.
His serum levels of bilirubin, amylase and lipase were within the normal
range. The tumor was excised and the final pathological diagnosis was
villotubular adenoma with moderate dysplasia. Surprisingly, the prurigo showed
spontaneous improvement and disappeared completely 2 years after an operation
(Figures 3A-3C). He remained free of prurigo at 4 years follow-up.
We report a case with chronic, recalcitrant widespread
prurigo nodularis that resolved spontaneously after resection of an ampulla of
Vater tumor. Adenomas of the ampulla of Vater are rare neoplasms with an
incidence of 0.04-0.12% in a postmortem series.1 The tumor can
obstruct normal drainage of pancreatic or bile secretions and cause jaundice,
cholangitis and pancreatitis. More importantly, these adenomas have the
potential for malignant changes.1 Patients with adenoma of the
ampulla of Vater may complain of nonspecific upper abdominal discomfort.
Pruritus usually occurs in patients with obstructive jaundice and is relieved
by removal of the tumor.2
Prurigo nodularis is
characterized by a papulonodular eruption with intense pruritus. Although the
acute form is often induced by insect stings, most of the subacute and chronic
forms appear to be idiopathic.3 Chronic lesions are usually
difficult to treat and cause frustration to both patients and physicians.
Prurigo nodularis is sometimes associated with atopy, pregnancy, systemic
diseases, malabsorption, or
 |
|
Figure 1 (A-C) A 63-year-old male had progressively worsening generalized prurigo nodularis.
|
 |
|
Figure 2 (A) An endoscopic retrograde cholangiopancreatography
for evaluation of patient's chronic epigastric discomfort reveals a tumor at
the
ampulla of Vater (arrow). (B) Magnetic resonance
imaging (T1 phase) shows a tumor in the ampulla Vater region (arrow).
|
 |
Figure 3 (A-C) The skin lesions were chronic and recalcitrant to
various treatments, but resolved spontaneously in 2 years after resection of a
villotubular
adenoma with moderate dysplasia of the ampulla of Vater.
malignancy.3 Prurigo nodularis has been
reported as an initial presentation of internal malignancies, including
hepatocellular carcinoma,4 metastatic transitional cell carcinoma,5
Hodgkin's disease,6 adult T-cell leukaemia/lymphoma7 and
gastric cancer.8 Prurigo may represent a paraneoplastic sign of
hepatocellular carcinoma in which the skin lesions resolve after tumor removal.4
To the best of our knowledge, generalized prurigo nodularis associated with
adenoma of the ampulla of Vater without obstructive jaundice, as seen in our
patient, has never been reported.2
The prurigo lesions in the
present case were preceded by chronic upper abdominal discomfort for several decades.
The finding of moderate dysplasia in a villotubular
adenoma suggests that the adenoma might have been longstanding and had
undergone malignant transformation, and this might be associated with the
development of prurigo lesions chronologically.
The mechanism of prurigo in
our patient remains elusive. Neuropeptides, including neuronal growth factors,
calcitonin gene-related peptide and substance P, have been proposed as the
pathogenesis of prurigo nodularis.3 Further study is required to
clarify whether the tumor in the present case secreted pruritogenic
neuropeptides. Nevertheless, the spontaneous resolution of the recalcitrant
prurigo after tumor excision suggests that there may have been a causal
relationship between the recalcitrant prurigo nodularis and the ampulla Vater
adenoma.
In summary, we report a
patient with refractory generalized prurigo nodularis, which resolved
spontaneously after excision of a dysplastic ampulla of Vater tumor. We recommend
a thorough survey of internal malignancy for patients with recalcitrant prurigo
as this may be a sign of internal malignancy on rare occasions, and an ampulla
of Vater
tumor should not be
overlooked in patients with chronic
epigastric discomfort.
1.
Yamaguchi K, Enjoji M. Adenoma of the ampulla of Vater:
putative precancerous lesion. Cut 1991;32:1 558-61.
2.
Venu RP, Geenen JE. Diagnosis
and treatment of diseases of the papilla. Clin Gastroenterol 1986;15:439-56.
3.
Lee MR, Shumack S. Prurigo nodularis: a review. Australas J Dermatol 2005;46:211-8; quiz 219-20.
4.
Dalle S, Merle P, Gouillat C, et al. Hepatocellular
carcinoma revealed by prurigo. Ann Dermatol Venereol 2006;1 33:243-5.
5.
Lin JT, Wang WH, Yen CC„ et al. Prurigo nodularis as
initial presentation of metastatic transitional cell carcinoma of the bladder.
J
Urol
2002;168:631-2.
6.
Shelnitz LS, Paller AS. Hodgkin's disease manifesting
as prurigo nodularis. Pediatr Dermatol 1990;7:136-9.
7.
Setoyama M, Mizoguchi S, Kanzaki T. Prurigo as a
clinical prodrome to adult T-cell leukaemia/lymphoma. Br J Dermatol 1998; 138:137-40.
8.
Funaki M, Ohno T, Dekio S, et al. Prurigo nodularis
associated with advanced gastric cancer: report of a case. J Dermatol 1996; 23:703-7.
Conflicts of interest: The authors
declare that they have no financial or non- financial conflicts of interest
related to the subject matter or materials discussed in this article.
[1] Corresponding author. Department of
Dermatology, National Cheng-Kung University Medical College and Hospital, 138
Sheng-Li Road, Tainan 704, Taiwan.
(T.-W. Wong).
[2] Corresponding author. Department of
Dermatology, National Cheng Kung University Medical College and Hospital,
No.138, Sheng Li Road, Tainan 704, Taiwan. Tel.: +886
2353535x5352; fax: +886 6 2004326.
[3] Corresponding author. Department of
Dermatology, National Cheng Kung University Medical College and Hospital,
Number 138, Sheng Li Road, Tainan 704, Taiwan. Tel.: 886 6 2353535x5352; fax:
886 6 2004326.
(T.-W. Wong).
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