SKIN 
 

May 2020     Volume 4 Issue 3 
 

Copyright 2020 The National Society for Cutaneous Medicine 288 

BRIEF ARTICLES 
 

 
Erythromelalgia in a Patient with Mast Cell Activation Syndrome: Response 
to Low Dose Naltrexone  
 
Anastasia O. Kurta, DO1, Leonard B. Weinstock, MD, FACG2, Natalie Semchyshyn, MD3 
 
1Saint Louis University, Department of Dermatology, St. Louis, MO 
2Specialists in Gastroenterology, St. Louis, MO 
3Saint Louis University, Department of Dermatology, St. Louis, MO 
 

 
 

 

Erythromelalgia (EM) can be disabling and 
difficult to treat. The incidence is 1.3 per 
100,000 people per year.1 Diagnostic criteria 
include: burning pain and erythema of the  
extremities, pain aggravated by 
warming/relieved by cooling, and increased 
skin temperature.2  Affected areas usually 
appear red and edematous and can have 
associated acrocyanosis, livedo reticularis, 
facial flushing, cutaneous necrosis and 
ulceration. The three major forms include: 
Type 1 – associated with thrombocythemia; 
Type 2 – primary, familial, or idiopathic; and 
Type 3 – associated with vascular and 
autoimmune diseases. Familial EM has been 
linked to dominant gain-of-function missense 
mutations in the SCN9A gene, which 
encodes the voltage-gated sodium channel 
alpha subunit Na(v)1.7, thought to be 
involved in nociception.3  
 
There is no definitive treatment for EM. We 
present a case of a patient with mast cell 

activation syndrome (MCAS) and EM, who 
had a good response to low dose naltrexone 
(LDN).  

A 55-year-old Caucasian female presented 
with an 8-month history of EM prior to our 
evaluation. The patient reported bilateral feet 
symptoms of burning pain, pricking 
sensation, and temperature changes ranging 
from hot to cold. She could not wear shoes 
without severe pain. Treatment with aspirin, 
nortriptyline, diltiazem, and topical nifedipine 
failed to provide relief. Gabapentin marginally 
reduced her pain. Metoprolol worsened the 
pain. She had a history of Raynaud’s 
phenomenon since age 15. Review of 
systems revealed a long history of fatigue, 
eye irritation, mouth sores, chest pain, 
palpitations, near syncope, bloating, 
abdominal pain, alternating diarrhea and 
constipation, heartburn, frequent urination, 
chronic headaches, muscle pain, anxiety, 
depression, brain fog, alopecia, and easy 
bruising.   

INTRODUCTION 

CASE REPORT 

Erythromelalgia is a rare condition that may be associated with a variety of underlying 
conditions and is often refractory to therapy. We report a case of a patient with mast cell 
activation syndrome who developed erythromelalgia and responded to low dose naltrexone. 
 

ABSTRACT 

 



SKIN 
 

May 2020     Volume 4 Issue 3 
 

Copyright 2020 The National Society for Cutaneous Medicine 289 

Physical examination was remarkable for 
symmetrical erythema and edema of bilateral 
lower extremities without evidence of 
temperature difference between the feet and 
legs (Figure 1). 
 
Figure 1. Erythema and edema of right foot. 

 
 
Skin punch biopsies of the calf and thigh were 
performed by her prior clinician to evaluate 
for small fiber neuropathy in the work up of 
dysautonomia, and were negative. Complete 
blood count was within normal limits. Mast 
cell mediators (plasma prostaglandin D2, 
histamine, and heparin; serum tryptase and 
chromogranin A; and 24-hour urine N-
methylhistamine, leukotriene E4, and 
prostaglandin 11-β-PGF2α) were obtained 
when she was feeling generally well and 
were normal. Duodenal biopsies revealed 30-
40 mast cells per high power field. She 
fulfilled the criteria for MCAS by having 
characteristic symptoms in 2 or more 

systems and having a mast cell density ≥20 
per high power field.4 

 
Mast cell-directed therapy was initiated with 
trials of various histamine 1 and 2 receptor 
blockers, including ranitidine, famotidine, 
ketotifen, and loratadine. These medications 
initially helped reduce her allergic, cardiac, 
and gastrointestinal symptoms. After 1 
month, LDN was added at 1 mg daily and 
gradually increased to 3 mg daily over 2 
months. Naltrexone was compounded into 
capsules by a compounding pharmacy. The 
histamine blockers were discontinued due to 
worsening constipation.  
 
After two months of LDN therapy, she 
reported moderate improvement in EM 
symptoms with reduced pain flares in her 
feet. At a clinic visit, eleven months after 
initiating LDN, she reported reduced pain, 
erythema, and edema in her feet (Figure 2). 
She estimated a subjective clinical benefit of 
75% that has been maintained with 2 years 
of LDN therapy. She is able to wear shoes 
comfortably most of the time, but reported 
self-limited erythema after exercise walks. 
She was unable to increase the LDN dose to 
4.5 mg due to insomnia but was able to 
tolerate 3 mg each morning. LDN was 
continued at 3 mg for 2 years with continued 
symptom improvement in the extremities 
(Figure 3). LDN also helped reduce bruising, 
chest pain, and mouth sores. 
 

In this case, LDN helped reduce the severity 
of EM in a patient with concomitant MCAS.  
 
MCAS is a chronic multi-system disease of 
abnormal mast cell activation that leads to 
inflammatory and allergic illness. MCAS has 
been estimated to have a prevalence of up to 
17%   (in  the  German  general  population);  

DISCUSSION 



SKIN 
 

May 2020     Volume 4 Issue 3 
 

Copyright 2020 The National Society for Cutaneous Medicine 290 

Figure 2. Improvement after 11 months of LDN 
therapy. 

 
 
Figure 3. Continued improvement after 2 years of 
LDN therapy.

 

however, the actual prevalence is not known, 
as MCAS is often not considered in the 
differential diagnosis of complex patients.4,5 
Unrecognized and untreated, MCAS may 
account for many refractory and vexing 
dermatologic symptoms. These include 
urticaria, pruritis, flushing, hemangiomas, 
and angioedema. The symptoms of MCAS 
can be numerous and affect multiple organs 
and systems which further complicates the 
clinical presentation. 
 
LDN has been successfully used off-label as 
an anti-inflammatory and immunomodulatory 
agent in several dermatologic conditions.6-8 
The LDN dose typically ranges from 1.0 to 4.5 
mg daily. The duration of the opioid receptor 
blockade determines naltrexone’s 
biotherapeutic response.9 Sustained 
inhibition of mu-opioid receptors by high dose 
naltrexone has been shown to increase 
inflammation and proliferation of tumor cells, 
while intermittent blockade by LDN inhibits 
cellular proliferation of T and B cells and 
antagonizes the Toll-like receptor 4 (TLR4)-
mediated pro-inflammatory pathway in 
macrophages and microglia.  Increasing 
evidence suggests that the immune system, 
specifically the TLR4 pathway, plays an 
integral role in maintenance of chronic pain.10 
Mast cells are known to express TLR4 
receptors and participate in nociception.11 

 
Although the pathophysiology of EM is 
multifactorial and poorly understood, there 
may be altered inflammatory mediator 
expression which results from vascular 
and/or neuronal dysfunction and which may 
benefit from immune modulators. A search 
for an underlying cause of presumed 
idiopathic EM should be thoroughly pursued. 
Further studies are necessary to evaluate the 
therapeutic benefit of LDN in patients with 
EM.  
 
 



SKIN 
 

May 2020     Volume 4 Issue 3 
 

Copyright 2020 The National Society for Cutaneous Medicine 291 

Conflict of Interest Disclosures: None 
 
Funding: None 
 
Corresponding Author: 
Anastasia O. Kurta, DO 
Saint Louis University 
Department of Dermatology 
1755 S. Grand Blvd 
St. Louis, MO 63104 
Email: anastasia.kurta@health.slu.edu  

 

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mailto:anastasia.kurta@health.slu.edu