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Observation Letters
87 (
4
); 555-557
doi:
10.25259/IJDVL_396_20

Graft versus host disease localized to striae distensae: An example of locus minoris resistentiae

Department of Dermatology, Venereology and Leprology, Postgraduate Institute of Medical Education and Research, Chandigarh, India
Department of Clinical Haematology Postgraduate Institute of Medical Education and Research, Chandigarh, India
Department of Histopathology, Postgraduate Institute of Medical Education and Research, Chandigarh, India

Corresponding author: Dr. Keshavamurthy Vinay, Department of Dermatology, Venereology and Leprology, Postgraduate Institute of Medical Education and Research, Sector 12, Chandigarh - 160 012, India. vinay.keshavmurthy@gmail.com

Licence
This is an open-access article distributed under the terms of the Creative Commons Attribution-Non Commercial-Share Alike 4.0 License, which allows others to remix, tweak, and build upon the work non-commercially, as long as the author is credited and the new creations are licensed under the identical terms.

How to cite this article: Bishnoi A, Lad D, Ashraf R, Banerjee N, Saikia UN, Vinay K. Graft versus host disease localized to striae distensae: An example of locus minoris resistentiae. Indian J Dermatol Venereol Leprol 2021;87:555-7.

Sir,

Allogeneic stem cell transplantation is frequently used in the treatment of hematologic malignancies. Graft versus host disease is among the common morbid complications that affect transplant recipients and is caused by the recognition of host antigens as foreign by the transplanted cells.1 Locus minoris resistentiae is a Latin term denoting a skin segment that presents lesser resistance to the development of disease as compared to the rest of the skin.2 This enhanced susceptibility of some cutaneous segments to develop a dermatosis is explained by the interplay of various cutaneous, immunological and neurological factors. Herein, we report a case of chronic graft versus host disease preferentially involving the sites of striae distensae as an example of locus minoris resistentiae.

A 13-year-old girl, with a prior diagnosis of acute myeloid leukemia, presented with itchy, erythematous papules on her back on day 128 of myeloablative, haploidentical hematopoietic cell transplantation. Her past history was significant for the development of acute cutaneous graft versus host disease and steroid-refractory, severe acute liver and gut graft versus host disease 1-month post-transplant, which had responded to antithymocyte globulin.

Examination revealed multiple fragile, erythematous to violaceous, scaly papules and plaques on her back, prominently localized to atrophic striae distensae, conforming precisely to their topography [Figure 1]. Her back also showed diffuse background post-inflammatory hyperpigmentation, reminiscent of acute cutaneous graft versus host disease. Nails and mucosae were normal. The rest of the skin was normal, and there was no obvious poikiloderma or sclerosis elsewhere on the skin. At that point of time, the patient was on tapering doses of prednisolone and mycophenolate mofetil. A diagnosis of late acute graft versus host disease (recurrent type) and chronic lichenoid graft versus host disease was considered, and skin biopsy was obtained from the papulosquamous lesions located on the striae.

Graft versus host disease localized to striae distensae. Multiple fragile, erythematous to violaceous, scaly papules and plaques are present on the back, prominently localized to atrophic striae distensae. Diffuse background post-inflammatory hyperpigmentation is reminiscent of acute cutaneous graft versus host disease
Figure 1:
Graft versus host disease localized to striae distensae. Multiple fragile, erythematous to violaceous, scaly papules and plaques are present on the back, prominently localized to atrophic striae distensae. Diffuse background post-inflammatory hyperpigmentation is reminiscent of acute cutaneous graft versus host disease

Histopathology from a skin biopsy obtained from the lesions on the back showed hyperkeratosis, mild hypergranulosis and dense interface dermatitis with multiple apoptotic bodies, foci of satellite cell necrosis, pigment incontinence and fragmented collagen fibers [Figures 2a-c]. A diagnosis of lichenoid chronic graft versus host disease was confirmed. She was advised topical mometasone furoate 0.1% cream and tacrolimus 0.1% ointment for local application. The dose of prednisolone was increased. Sirolimus was added to mycophenolate mofetil and the lesions resolved within a month.

Histopathological findings of skin biopsy of lesion on the back. The epidermis shows spongiosis with diffuse basal cell vacuolization and perivascular lymphocytic cell infiltration in the superficial dermis (H and E, ×100)
Figure 2a:
Histopathological findings of skin biopsy of lesion on the back. The epidermis shows spongiosis with diffuse basal cell vacuolization and perivascular lymphocytic cell infiltration in the superficial dermis (H and E, ×100)
Histopathological findings of skin biopsy of lesion on the back. The epidermis shows dyskeratotic keratinocyte (red arrow), satellite cell necrosis (blue circle) and lymphocytic exocytosis in the epidermis (H and E, ×200)
Figure 2b:
Histopathological findings of skin biopsy of lesion on the back. The epidermis shows dyskeratotic keratinocyte (red arrow), satellite cell necrosis (blue circle) and lymphocytic exocytosis in the epidermis (H and E, ×200)
Histopathological findings of skin biopsy of lesion on the back. Interface changes accompanied by basal cell vacuolization and apoptotic keratinocytes are seen in the epidermis (arrows) (H and E, ×400)
Figure 2c:
Histopathological findings of skin biopsy of lesion on the back. Interface changes accompanied by basal cell vacuolization and apoptotic keratinocytes are seen in the epidermis (arrows) (H and E, ×400)

Graft-versus-host disease represents one of the most common complications of allogeneic hematopoietic stem cell transplantation.1 Its classification was previously based on the time point of 100 days (acute 100 days); though this was later revised to include cases of acute graft versus host disease that occurred beyond this time-point (persistent, recurrent and de-novo). Though acute graft-versus-host disease can be usually diagnosed clinically depending upon skin, liver and gastrointestinal manifestations, the same is not true for chronic graft versus host disease, where diagnosis relies on the presence of either diagnostic manifestations (classical lichen planus, poikiloderma or sclerosis), or distinctive manifestations that are subsequently proven to be chronic graft versus host disease on histopathology (lichenoid or sclerotic features in the skin).3 For our patient, since she presented on day 128 post-transplant, and the lesions were not very suggestive of classic lichen planus; both diagnoses were considered; that is, late acute (recurrent) or chronic lichenoid graft versus host disease, and histopathology established the diagnosis to be chronic lichenoid graft versus host disease.

The index patient had also developed classic acute graft versus host disease (affecting skin, liver and gut) initially (after 1 month of transplant); following which she gradually developed extensive striae distensae probably because of the concomitant pubertal growth spurt and intake of systemic corticosteroids. Striae distensae represent traumatized dermal collagen zones, and their selective affliction by chronic lichenoid graft versus host disease in the index patient aptly demonstrates the phenomenon of locus minoris resistentiae. An easy transit and access of lymphocytes to cutaneous antigens through the damaged dermal matrix in the striae might be a plausible explanation for this occurrence. Chemotherapy-induced skin eruptions localized to radiotherapy site4 and melanoma metastasis;5 as well as infective conditions like verruca6 and tinea barbae7 localized to verrucous epidermal nevus and scar tissue, respectively, are other examples of locus minoris resistentiae. Fixed drug reaction secondary to minocycline localizing to areas of herpes zoster and burn scars has also been described.8 Vitiligo,9 psoriasis,10 plane xanthomas,11 drug-induced exanthems12 leukemia cutis13 and lichen sclerosus14 are some of the other dermatosis that have been reported to localize to striae distensae.

Though graft versus host disease is a systemic affliction, the skin is affected preferentially; in both acute and chronic forms. Atypical cutaneous variants have been previously described [Table 1]15-18 highlighting the effect of the microenvironmental and constitutional factors on the final presentation of the disease. Blaschkoid (both acute and chronic)19 and chronic sclerotic graft versus host disease conforming to the sites of the waistband, radiotherapy, needle sticks and healed herpes zoster has been previously reported.20 Lichenoid graft versus host disease localizing to striae has been sparingly reported before.21 All these cases highlight previously described Wolf’s isotopic or Koebner’s isomorphic response; both of which can now be clubbed into the unifying concept of an immunocompromised cutaneous district or the locus minoris resistantiae,22 which the index case aptly represents, though for a rarer disease.

Table 1: Atypical cutaneous manifestations of graft-versus-host disease15-18
Acute graft-versus-host disease Chronic graft-versus-host disease
Psoriasiform Psoriasiform
Follicular erythema/lichenoid Follicular erythema/lichenoid
Contact dermatitis Acral keratosis
Type-II pityriasis rubra pilaris-like Pityriasis rosea-like
Hand-foot-mouth disease-like Annular scleroderma-like plaques
Localized to tattoo skin Eczematoid
Atopic dermatitis-like
Exfoliative dermatitis
Dermatomyositis-like
Lupus erythematosus-like
Hypertrophic lupus erythematosus-like
Erythema multiforme-like
Total body leukoderma
Koebner isomorphic pattern
Blaschko-linear
Black hairy tongue
Nodular/keloidal scleroderma-like

Declaration of patient consent

The authors certify that they have obtained all appropriate patient consent.

Financial support and sponsorship

Nil.

Conflicts of interest

There are no conflicts of interest.

References

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