1Department of Dermatology, Rustaq Extended Health Institute, Rustaq, Oman; 2Department of Medicine, Rustaq Hospital, Rustaq, Oman
*Corresponding Author’s e-mail: raqiya.al-rajaibi@mail.mcgill.ca 

Carbamazepine-Induced Stevens-Johnson 
Syndrome/Toxic Epidermal Necrolysis Overlap 

Treated Successfully with Oral Cyclosporin
Case report and literature review

*Raqiya Al Rajaibi,1 Thuraiya Al Rumhi,1 Al Mur Al Abri2

Sultan Qaboos University Med J, August 2021, Vol. 21, Iss. 3, pp. 491–494, Epub. 29 Aug 21
Submitted 22 Apr 20
Revisions Req. 1 Jul & 13 Sep 20; Revisions Recd. 12 Aug & 26 Sep 20
Accepted 21 Oct 20

facility where she was prescribed intravenous (IV) 
hydrocortisone and IV antibiotics and her intake of 
carbamazepine was discontinued. Unfortunately, 
her condition deteriorated and she subsequently 
developed dysphagia. She decided to leave, against 
medical advice, to seek a second medical opinion. 
Consequently, she was re-admitted to Ar Rustaq 
Hospital after three days of her symptoms.

The initial examination of the patient revealed her 
to be very ill, dehydrated, febrile and tachycardiac. Her 
skin examination revealed multiple maculopapular 
rashes covering over 50% of body surface area (BSA; 
using the rule of nines), with some dusky areas. There 
was skin peeling over the ear pinna, cheeks and 
abdomen (around 15% of her BSA) with some flaccid 
bullae over the anterior part of the neck and acral areas 
[Figure 1]. The blistered area was positive for Nikolsky’s 
sign. Red conjunctival mucosa with multiple erosions 
in the mouth and genital mucosa were also noted.

Initial laboratory results revealed elevated C-re- 
active protein levels (139 mmol/L), elevated erythro- 
cyte sedimentation rate (49 mm/h), a normal white 
blood cell count of 4.7 x 103/uL with normal differential 
counts (neutrophils 2.89 x 103/µl and eosinophil 0.05 x 
103/µl), normal random blood sugar levels and normal 
renal (including electrolytes, creatinine and urea) and 
liver function tests.

A multidisciplinary team was involved in patient 
management, including those drawn from the fields of 
ophthalmology, dentistry, ear, nose and throat (ENT), 
internal medicine and dermatology. The patient had 

Stevens johnson syndrome (sjs) and toxic epidermal necrolysis (TEN) are skin conditions that have been observed following reactions 
to certain drugs.1–4 Several therapies can be used to 
treat SJS/TEN; however, there is currently no standard 
treatment option.5 Previous studies have shown that 
cyclosporine (CsA) can be used to treat SJS/TEN 
off-label.2 CsA has shown promising therapeutic 
effectiveness in curing similar diseases, although its 
therapeutic role has not yet been fully understood.2,3,6–10 
Here, we present a case from Oman of SJS/TEN being 
successfully treated using oral CsA and providing 
supportive management. The current report will also 
provide a brief review of the literature concerning the 
use of CsA in the treatment of SJS/TEN. 

Case Report 

A 38-year-old female nurse was admitted to Ar 
Rustaq Hospital, Rustaq, Oman, in 2019 with a 
three-day history of fever and sore throat, as well as 
skin eruptions and oral mucosal and conjunctival 
ulcerations. She did not suffer from any chronic 
disease apart from recurrent arthralgia and was not 
on any regular medication except various pain killers 
for her arthralgia as required. Additionally, she did not 
have any drug allergies. Her symptoms began on day 
10 of her using carbamazepine. The patient had been 
taking carbamazepine for the first time as a pain killer 
following several failed pain medications. The patient 
had been admitted for one day to a private healthcare 

This work is licensed under a Creative Commons Attribution-NoDerivatives 4.0 International License.

https://doi.org/10.18295/squmj.4.2021.002

CASE REPORT

abstract: Stevens Johnson syndrome (SJS) and toxic epidermal necrolysis (TEN) are acute life-threatening 
mucocutaneous drug reactions. Several therapies have been used in the treatment of SJS/TEN but none of them 
have yet been established as the gold standard treatment. Studies have shown that cyclosporine (CsA) can be used 
off-label in TEN/SJS, which has shown promising therapeutic effectiveness in such diseases. Here we report a 
38-year-old woman who presented to Ar Rustaq Hospital, Rustaq, Oman in 2019 with SJS/TEN overlap and was 
treated successfully with CsA along with supportive management. This case report also includes a literature review 
on the use of CsA in the treatment of SJS/TEN.

Keywords: Stevens Johnson Syndrome; Toxic Epidermal Necrolysis; Drug-Induced Abnormality; Cyclosporine; 
Drug Eruption; Case Report; Oman.

https://creativecommons.org/licenses/by-nd/4.0/


Carbamazepine-Induced Stevens-Johnson Syndrome/Toxic Epidermal Necrolysis Overlap Treated Successfully with 
Oral Cyclosporin 

Case report and literature review

492 | SQU Medical Journal, August 2021, Volume 21, Issue 3

initially been admitted to the intensive care unit for 
monitoring purposes and was then shifted to the 
medical ward. She was managed with IV hydration, 
frequent petroleum jelly application on the skin 
lesions and heparin prophylaxis. Furthermore, she 
was started on an oral dose of CsA of 5 mg/kg/day. 
At Ar Rustaq Hospital, CsA is considered to be cost-
effective and readily available compared to other 
alternative therapies such as IV immunoglobulin 
(IVIg), Etanercept and plasmapheresis. The patient 
gradually improved and showed skin re-epithelisation 
on day three of CsA administration. Additionally, no 
new skin lesions were noted. She was then discharged 
on day six when her dose was reduced to 3 mg/kg/day. 

In a follow-up appointment in the dermatology 
clinic after nine days, the patient showed remarkable 
improvement. Subsequently, the CsA was discontinued. 

In total, she had received a gradually decreasing dose 
of CsA for 15 days [Figure 2]. 

The patient has given informed consent for the 
publication of her case in a medical journal.

Discussion

SJS and TEN are severe mucocutaneous drug reactions. 
The difference between these two conditions is based 
on the percentage of BSA involvement and type of 
skin lesions. SJS involves detachment 10% of BSA, 
plus widespread erythematous, purpuric macules 
or flat atypical target lesions. An overlap of the two 
conditions, SJS/TEN, involves detachment 10–30% 
of BSA, plus widespread erythematous, purpuric 
macules or atypical target-like annular patches. TEN, 
alone, is detachment of 30% of BSA, plus widespread 
erythematous, purpuric macules or atypical target 
lesions. TEN without spots leads to large epidermal 
sheets, of around 10% BSA, without purpuric macules 
or target lesions.1,3 The overall combined incidence 
of SJS, SJS/TEN overlap and TEN is estimated to be 
2–7 per million cases per year, with a mortality rate 
of approximately 25–35%.1,2 SJS/TEN can manifest 
through varying symptoms such as fever, mucositis, 
anorexia, and skin tenderness. These symptoms 
are then followed by cutaneous lesions, such as 
targetoid lesions, vesicles and bullae in addition to 
rapidly progressing sloughing of the skin within a few 
days.1,6 The case detailed here fits the category of SJS/
TEN overlap, given that the patient had peeling and 
blistering of around 10–15% of BSA and widespread 
maculopapular skin lesions.

The pathogenesis of SJS/TEN has not yet 
been sufficiently understood.3 Most of the cases are 
preceded by exposure to certain medications.1,3 Many 
medications have been identified as the likely cause of 
SJS/TEN, such as NSAIDs, anticonvulsants, antibiotics 
and allopurinol.1,2 Other non-drug causes of SJS/

Figure 2: Image of a 38-year-old female patient at 
recovery (achieved mainly through the use of oral 
cyclosporine), two months after the first presentation.

Figure 1: Maculopapular rash of the skin of a 38-year-old female patient with some dusky areas and skin peeling (as seen 
during admission).



Raqiya Al Rajaibi, Thuraiya Al Rumhi and Al Mur Al Abri

Case Report | 493

TEN include mycoplasma pneumonia infection, HIV, 
dengue virus, the mumps-rubella vaccination and the 
use of contrast agents for imaging purposes.1 Certain 
genetic factors have also been found to be associated 
with an increased risk of SJS/TEN.3 The patient, in 
this case, was of Indian origin and developed SJS/TEN 
after taking carbamazepine. Being of Indian or Asian 
origin increases the risk of anticonvulsant-induced 
SJS/TEN, as individuals of these nationalities have 
a high prevalence of the HLA-B*1502 phenotype.4 
Unfortunately, the HLA phenotyping for this patient 
could not be sent for due to technical and financial 
reasons.

Management of SJS/TEN should be initiated 
by first discontinuing the suspected agent, along 
with providing comprehensive supportive care.5 A 
multidisciplinary team should be created involving 
critical care experts, including those belonging to 
dermatology, infectious disease, ophthalmology and 
ENT fields along with a wound care nurse and a 
dietician.2,5 Supportive care is best delivered in the 
burn or intensive care unit, which would mainly focus 
on the assessment of airway, renal function, fluid and 
electrolyte balance, nutrition, skin and ocular surfaces, 
pain control and prevention of infection.5

In addition to supportive care, several potential 
therapies have been proposed, including IVIg, 
glucocorticoids, plasmapheresis, CsA and TNF-a 
inhibitors (such as etanercept).5,6 However, none of 
these therapies have yet been established as the gold 
standard treatment for SJS/TEN.5 CsA is a well-
established medication that has been used to cure 
several dermatological diseases.2 A review of the 
current literature indicates that CsA may slow down 
the progression of SJS/TEN.2,7–8 CsA has been found 
to be effective in reducing the mortality rate of SJS/
TEN, the duration of recovery and contributing to 
early discharge from the hospital.7

The proposed mechanism of action of CsA in 
SJS/TEN is through inhibiting the function, reducing 
the production of cytokines by cytotoxic T cells and 
natural killer cells.6 Additionally, it reduces granulysin 
levels, which has recently been noted to have an 
important role in the pathogenesis of SJS/TEN 
related to cell apoptosis.1,3 An observational record-
based study compared the use of CsA and supportive 
treatment with using supportive treatment alone.7 It 
was found that the standardised mortality ratio was 
0.32 in the CsA group, which is nearly 3.3 times lower 
than that in the supportive treatment group. Moreover, 
the time of re-epithelisation of the skin, duration of 
recovery and stabilisation were significantly lower in 
the CsA group, at P = 0.007, P = 0.01 and P < 0.001, 
respectively.7 A meta-analysis by Gonzalez et al. 

assessed 71 patients with epidermal necrolysis. Of 
these, 49 patients were treated with CsA and five of 
the treated patients died (10.2%). It should be noted 
that in this group, 11.8 (24.1%) deaths were expected, 
according to the score for TEN. Of the 22 patients 
who were treated with non-CsA therapies, seven died 
(31.8%), when 6.4 deaths (29.1%) were expected.8

In 2018, a meta-analysis of nine observational 
studies, with a total of 256 SJS/TEN patients, revealed a 
significant reduction in risk of mortality following CsA 
therapy (standardised mortality ratio of 0.320; 95% CI: 
0.119–0.522; P = 0.002).2 In addition, a retrospective 
study from 2014 revealed that the use of CsA over IVIg 
may offer a higher chance of recovery in the SJS/TEN 
treatment (standardised mortality ratio of 0.43 over 
1.43, respectively).9 In 2010, Allanore et al. conducted 
the first open phase II trial to determine the safety and 
possible benefit of CsA treatment for SJS and TEN.10 It 
concluded that CsA lowered both the death rate and 
the progression of detachment to a greater degree than 
expected.10 

The results of these studies support the 
effectiveness of CsA (at a dose of 3–5 mg/kg/day, 
starting treatment at the earliest) in reducing the 
chance of mortality and rapid cessation of the SJS/
TEN disease progression.2–3,6–10

Conclusion 

This case report demonstrates a successful experience 
of the administration of CsA, along with supportive 
care, in the management of SJS/TEN overlap. This 
finding was supported following a thorough review 
of the currently available literature. However, future 
randomised controlled trials would be the most 
effective in confirming the efficacy of CsA. 

a u t h o r s’ c o n t r i b u t i o n
All authors were involved in the treatment of the 
patient. RA collected all the patient’s data and took her 
consent. RA and TA conducted the literature review, 
drafting and revising of the manuscript. All authors 
read and approved the final version of the manuscript

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Carbamazepine-Induced Stevens-Johnson Syndrome/Toxic Epidermal Necrolysis Overlap Treated Successfully with 
Oral Cyclosporin 

Case report and literature review

494 | SQU Medical Journal, August 2021, Volume 21, Issue 3

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