SKIN 
 

May 2019     Volume 3 Issue 3 
 

Copyright 2018 The National Society for Cutaneous Medicine 215 

BRIEF ARTICLES 
 

 
Fibroelastolytic Papulosis in a Middle-Age Female: Presentation 
and Review of Treatment 
 
Carl Barrick, DO,1 An Guo Michael Chin, DO, MPH, MS2 Veronica Rutt, DO1, Nektarios Lountzis, 
MD3, Cynthia Bartis, MD3 
 
1Lehigh Valley Health Network, Allentown, PA 
2Philadelphia College of Osteopathic Medicine, Philadelphia, PA 
3Lehigh Valley Health Network and Advanced Dermatology Associates, Ltd, Allentown, PA 
 

 
 

Fibroelastolytic papulosis (FEP) is a rare 
acquired, non-systemic, skin disease that 
presents as white-ivory to yellow papules and 
plaques commonly occurring on the neck (1). 
In 1989 Shimizu et al. reported an isolated 
asymptomatic white fibrous plaque with 
histopathological changes of fibrosis in the 
papillary and upper reticular dermis which 
was coined as white fibrous papulosis of the 
neck (WFPN) (2). In 1992 Rongioletti and 
Rebora reported a similar skin lesion 
identifying it as pseudoxanthoma elasticum-

like papillary dermal elastolysis (PXE-PDE), 
which, unlike PXE, does not have systemic 
associations (3). Balus et al. first proposed 
the name “fibroelastolytic papulosis of the 
neck" (FEPN) in 1997 to encompass both 
WFPN and PXE-PDE, since they believed 
these skin disorders were a continuum of a 
single entity (4,5). Despite the name, FEPN 
can occur in other locations besides the neck, 
thus Jagdeo et al. recommended changing 
the name to solely “fibroelastolytic papulosis 
(FEP)” in 2004 (6). 
 
Clinically, FEP presents as multiple (20-100), 
4-6 mm firm papules often coalescing into a 

Fibroelastolytic papulosis (FEP) is a rare, benign, acquired cutaneous disease with a 
histopathology that shows variable fibrosis and elastolysis of the papillary dermis. FEP 
clinically presents as white-ivory to yellow papules and plaques commonly occurring on the 
neck. There are no widely accepted treatment guidelines and several management options will 
be discussed. We present a 62-year-old female with an isolated ivory, cobblestoned plaque 
with open comedones on the left shoulder since childhood. The histopathology confirmed the 
diagnosis of FEP. The patient had been previously treated with topical clindamycin, salicylic 
acid, tretinoin, and tazarotene without success. This case demonstrates the importance of 
recognizing FEP, as clinical presentations can vary. FEP can be distressing to patients, and it 
is important to explore additional treatment options. Treatment options including topical 
retinoids and ablative lasers have been reported, but with limited and inconsistent success. 
However, due to the rarity of the disease there is currently no standard of care for the treatment 
of FEP and additional successful treatment options are needed.  
 

ABSTRACT 

INTRODUCTION 



SKIN 
 

May 2019     Volume 3 Issue 3 
 

Copyright 2018 The National Society for Cutaneous Medicine 216 

cobblestone plaque. They range in color from 
flesh colored to white-ivory to yellow. The 
papules and plaques are generally 
asymptomatic, but inflamed folliculitis-like 
areas and pruritus can occur. FEP is found 
on the posterior and lateral aspects of the 
neck with extension to surrounding areas. 
The histopathology of FEP presents as loss 
or alteration of elastic fibers and fibrosis of 
the papillary and upper reticular dermis(7). 
PXE and PXE-PDE will reveal calcified 
elastic fibers(3). 
 
The pathogenesis of FEP has yet to be 
elucidated, but it is commonly theorized that 
it is related to an intrinsic photo-aging 
process. FEP most often occurs in patients 
over the age of 40 with a predilection for 
females of European ancestry (7). The 
lesions of FEP are benign, but can often 
progress and be cosmetically distressing to 
patients. There are no standard FEP 
treatments established at this time due to its 
rarity. We report an interesting case of FEP 
in a 62-year-old Caucasian female and 
explore treatment options.  

A 62-year-old female patient with a past 
medical history significant for hypothyroidism 
and hyperparathyroidism presented with a 
large lesion on her left shoulder since 
childhood. The patient described it as 
generally asymptomatic but reported 
intermittent pimple-like lesions within the 
plaque that developed later in life.  
 
Physical exam revealed multiple 2-4 mm 
flesh-colored to ivory papules coalescing into 
a large cobblestone, well-defined plaque with 
inflammatory papules and open comedones 
on the left shoulder extending on to the left 
upper back and proximal left upper extremity 
(Figure 1). 
 

 
Figure 1: Clinical image demonstrating multiple 2-
4mm fleshed colored to ivory papules coalescing into 
a large cobblestone-pattern plaque with dilated 
comedonal openings on the left shoulder and proximal 
left arm.  
 
The histopathology revealed intradermal 
proliferation of variably sized tubular 
structures lined by a multi-cell layered 
epithelium and filled with amorphous 
basophilic material. Distinct small areas of 
superficial dermal collagen thickening with 
some of the collagen bundles becoming 
hyalinized, thickened and amorphous were 
present (Figures 2, 3). Focal patchy 
inflammation was noted within portions of the 
dermis surrounding the hyalinized nodules. 
Considering the clinical presentation and 
histopathological correlation, the diagnosis of 
FEP was made. 
 
Due to the acneiform nature of the lesions 
within the plaque the following treatments 
were attempted; topical clindamycin 1% 
lotion, salicylic acid wash, benzoyl peroxide 
5% wash, tretinoin 0.5% cream, and 
tazarotene 0.1% without considerable 
improvement. Patient refused all additional 
treatment including fractionated carbon 
dioxide laser treatments.  
 
 
 

CASE REPORT 



SKIN 
 

May 2019     Volume 3 Issue 3 
 

Copyright 2018 The National Society for Cutaneous Medicine 217 

Figure 2: Hematoxylin and Eosin (4x) slide from a 
punch biopsy of left mid superior scapula 
demonstrating superficial dermal collagen thickening, 
some of which are sharply defined, with some of the 
collagen bundles becoming hyalinized, thickened and 
amorphous. Some focal patchy inflammation is noted 
within portions of the dermis surrounding the 
hyalinized nodules as well.  

  
Figure 3: Hematoxylin and Eosin (20x) slide from a 
punch biopsy of left mid superior scapula 
demonstrating hyalinized, thickened and amorphous 
superficial dermal collagen. Some focal patchy 
inflammation is noted within portions of the dermis 
surrounding the hyalinized nodules as well. 

 
 

 
FEP is a rare acquired skin disorder that 
shows elastolysis of the papillary dermis. 
FEP encompasses WFPN and PXE-PDE 
due to considerable overlap in clinical 

presentations and histopathology. The 
pathogenesis of FEP is not well understood, 
but may be secondary to intrinsic and photo-
aging processes (8). FEP is a non-life 
threatening skin disease, nevertheless it can 
be distressing for many patients due to 
cosmesis. In the case reported the patient 
experienced discomfort due to inflammatory 
lesions. There are currently no standard 
treatment guidelines established for FEP.  
 
Considering the benign nature of FEP, 
treatment is not necessary. However, many 
patients are cosmetically concerned with 
FEP and seek treatment. Tretinoin may be a 
viable non-invasive, well-tolerated option for 
patients with FEP, but results are 
inconsistent and often not curative. One case 
report documented the use of topical tretinoin 
0.05% cream twice a day with significant 
improvement after five weeks (8). Similarly, 
another case of FEP treated with topical 
tretinoin 0.1% gel improved after three 
months and revealed complete resolution in 
one year (9). In contrast, a case reported by 
Lueangarum, et al., did not improve with 
tretinoin in their patient (10).The patient we 
presented also did not show improvement 
with tretinoin. The exact mechanism by which 
tretinoin acts on FEP is unknown (8). 
 
Moreover, two case reports, one by Chong et 
al., and the other by Ho et al., documented 
successful treatment of FEP with fractionated 
carbon dioxide (CO2) laser (SmartXide 
DEKA DOT® Laser)(1) (11), with 
improvement after three successive laser 
treatments and complete resolution within a 
year. Another case report highlighted the 
successful treatment of FEP utilizing a non-
ablative fractional photo thermolysis laser 
(Fractionated 1550-Erbium Glass laser) (10). 
Based on these findings, it appears that laser 
treatment may be a viable treatment option 
for FEP. Surgical excision can also be 

DISCUSSION 



SKIN 
 

May 2019     Volume 3 Issue 3 
 

Copyright 2018 The National Society for Cutaneous Medicine 218 

considered in a small well-defined lesion of 
FEP (10). 
 

 
Fibroelastolytic papulosis (FEP) is a rare 
benign skin disorder that can be distressing 
to patients, and has no established treatment 
guidelines to date. Our case demonstrates a 
unique clinical presentation and the need to 
explore additional treatment options for FEP. 
There have been few successful FEP 
treatments documented but ablative lasers 
appear promising.  Despite inconsistent 
results with topical retinoids, this modality 
could also still be considered as a 
conservative first line approach to therapy. 
No single treatment has been thoroughly 
studied for its efficacy in FEP, therefore 
treating each case on an individual basis with 
patient consideration is recommended.  
 
Conflict of Interest Disclosures: None. 
 
Funding: None. 
 
Corresponding Author: 
Carl Barrick, DO 
Lehigh Valley Health Network 
Allentown, PA 
barriccj@gmail.com  
  

References: 
1. Chong S, Woodley D, Kim G, Shim E. 

Treatment of Fibroelastolytic papulosis 
with fractionated carbon dioxide laser. 
J Cosmet Laser Ther. 2015;17(2):90-92.  

2. Shimizu H, Kimura S, Harada T, 
Nishikawa T, White fibrous papulosis of 
the neck: a new clinicopathologic 
entity? J Am Acad Dermatol. 
1989;20:1073-1077. 

3. Rongioletti F, Rebora A. 
Pseudoxanthoma elasticum-like 

papillary dermal elastolysis. J Am Acad 
Dermatol. 1992;26: 648-50.  

4. Balus L, Amantea A, Donati P, Fazio M, 
Guiliano MC, Bellocci M. 
Fibroelastolytic papulosis of the neck: a 
report of 20 cases. Br J Dermatol 1997; 
137:461-466 

5. Patterson A, Beasley K, Kobayashi T. 
Fibroelastolytic papulosis: 
histopathologic confirmation of disease 
spectrum variants in a single case. J 
CutanPathol. February 
2016;43(2):142-147.  

6. Jagdeo J, Ng C, Ronchetti IP, Wilkel C, 
Betcovitch L, Robinson-Bostom L. 
Fibroleastolytic papulosis. J Am Acad 
Dermatol. 2004;51:958-964 

7. Song YC, Oh BH, Ko JH, Kim JY, Hwang 
YJ, Lee YW, et al. A case of 
Fibroelastolytic papulosis on the neck 
of a young man. Ann Dermatol. 
2011;23:193-197 

8. Maione V, Errichetti E, Stinco G, Orsaria 
M, and Patrone P. Fibroelastolytic 
papulosis of the neck treated with 
topical tretinoin. J Dermatol. Aug 
2014;(8):758-759 

9. Wang AR, Lewis K, Lewis M, Robinson-
bosom L. Papillary dermal elastosis: a 
unique elastic tissue disorder or an 
unusual manifestation of 
pseudoxanthoma elasticum-like 
papillary dermal elastolysis? J 
CutanPathol. 2009;36:1010-1013 

10. Lueangarum S. Panchaprateep, R. White 
fibrous papulosis of the neck treated 
with fractionated 1550-nm erbium 
glass laser: a case report. J Lasers in Med 
Sci. 2016;7940: 256-258 

11. Ho, D., &Jagdeo, J. Fractionated Carbon 
Dioxide Laser Treatment of 
Fibroelastolytic Papulosis with 
Excellent Cosmetic results and 
Resolution of Pruritus. JDrugs Dermatol. 
Nov 2015; 14(11):1354-1357 

 

CONCLUSION 

mailto:barriccj@gmail.com