Hypopigmented lesions in pityriasis lichenoides chronica patients: Are they only post‐inflammatory hypopigmentation?

Elbendary, Amira; Abdel‐Halim, Mona R. E.; Youssef, Randa; Halim, Dalia Abdel; Elmasry, Maha Fathy; Gad, AbdAllah; Sharkawy, Dina Ahmed El

doi:10.1111/ajd.13746

Cited by 3 publications

(3 citation statements)

References 21 publications

(46 reference statements)

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“…Dermoscopy of the leucomelanodermic form has not been described in the literature and in the case of our patient was not of diagnostic help. According to the study conducted by Elbendary et al in 2022, the average duration of depigmentation in the absence of primary lesions is 35 to 20 months for patients with PLC [6]; this duration is longer in patients with a dark phototype [7] confirming the data of the study carried out on PLC in black patients in 2010. This suggests that long-lasting pigmentary change in the absence of apparent primary lesions may represent ongoing disease activity rather than a scarring reaction [8].…”

Section: Presentation Of the Casementioning

confidence: 76%

Chronic and Stubborn Leuco-melanoderma in a Child: A Case Study

Khabba

Asermouh²,

Znati³

et al. 2023

AJPR

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Aims: Pityriasis lichenoides chronic is a rare inflammatory dermatosis, unusually hypochromic in dark phototypes. The evolution of the disease is usually benign, but a malignant transformation in mycosis fungoides is reported. You have to know how to think about it when faced with a generalized hypochromic macular eruption in children. Case Report: We report a case of a 13-years-old child, photo type 4.He presented for 8 months hypochromic macular lesions, located initially at the face. The evolution was marked by the extension at the trunk and the limbs. He was treated for pityriasis versicolor but without improvement. A skin biopsy was then performed, in favor of Pityriasis Lichenoides Chronica (PLC) with a lymphoid infiltrate made up mainly of CD4 T lymphocytes. The child was put on cyclin associated with heliotherapy with a moderate improvement after 3 months of treatment. The patient was followed for 2 years during which he did not present any malignant transformation. Discussion: Pityriasis Lichenoides is less frequent in the pediatric population.Its etiopathogenesis is still incompletely elucidated. The basic lesion is an erythematous-squamous papule in the trunk. Hypochromic macules can also be observed, either at the cicatricial stage of the disease, or they occur immediately, especially in subjects with dark skin. The histology of PLC reveals perivascular lymphocytic infiltrate in the superficial dermis..The adopted therapeutic is based on heliotherapy or an antibiotic from the macrolide or cyclin family. Evolution towards Mycosis Fungoides has been rarely described. Conclusion: PLC is exceptionally hypopigmented from the outset. We report a case of chronic leucomelanodermic pityriasis lichenoides in a child posing a problem of differential diagnosis.

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Section: Presentation Of the Casementioning

confidence: 76%

Chronic and Stubborn Leuco-melanoderma in a Child: A Case Study

Khabba

Asermouh²,

Znati³

et al. 2023

AJPR

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“…Pityriasis lichenoides chronica is also one of the diseases that can cause a lot of confusion with HMF as it can present with hypopigmented macules and patches affecting the trunk and extremities of children and young adults with dark skin type 13 . Furthermore, hypopigmented lesions seen in PLC have been found to represent an active or residual disease that shows vacuolar interface dermatitis along with variable degrees of spongiosis, keratinocyte necrosis, and lymphocyte exocytosis 14 . The presence of lymphoid atypia, Pautrier's‐like microabscesses, and wiry fibroplasia in some lesions, 15 and the inability of immunohistochemical and molecular studies to differentiate between PLC and HMF 16,17 can lead to a diagnostic dilemma.…”

Section: Discussionmentioning

confidence: 99%

“…13 Furthermore, hypopigmented lesions seen in PLC have been found to represent an active or residual disease that shows vacuolar interface dermatitis along with variable degrees of spongiosis, keratinocyte necrosis, and lymphocyte exocytosis. 14 The presence of lymphoid atypia, Pautrier's-like microabscesses, and wiry fibroplasia in some lesions, 15 and the inability of immunohistochemical and molecular studies to differentiate between PLC and HMF 16,17 can lead to a diagnostic dilemma.…”

Section: Hypopigmented Interface T-cell Dyscrasia Presents As Hypo-mentioning

confidence: 99%

Basement membrane thickness helps to differentiate hypopigmented mycosis fungoides from clinical and pathological mimickers

Abdelkader

2023

Int J Dermatology

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Background Hypopigmented mycosis fungoides (HMF) is a relatively rare subtype of mycosis fungoides (MF). The diagnosis of HMF can be quite challenging in case of insufficient diagnostic criteria due to the diverse conditions that present with hypopigmented lesions. This study aimed to evaluate the usefulness of the assessment of the basement membrane thickness (BMT) in the diagnosis of HMF.Methods A retrospective study was conducted on biopsy specimens of 21 HMF and 25 non-HMF cases who presented with hypopigmented lesions. The thickness of the basement membrane was evaluated in periodic acid-Schiff (PAS)-stained sections. ResultsThe mean BMT was significantly higher in the HMF group than in the non-HMF group (P < 0.001). The best cut-off value of mean BMT for the detection of HMF verified in ROC analysis was 32.7 lm (P < 0.001) with a sensitivity of 85.7% and a specificity of 96%. ConclusionEvaluation of BMT can be a useful tool to distinguish HMF from other causes of hypopigmented lesions in doubtful cases. We suggest the use of " BMT more than 33 lm" as a histopathologic criterion of HMF. P < 0.05 is significant. HMF, hypopigmented mycosis fungoides; BMT, basement membrane thickness; SD, standard deviation.

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Post-Inflammatory Hypopigmentation: Review of the Etiology, Clinical Manifestations, and Treatment Options

Rao

Young

Jackson-Cowan

et al. 2023

JCM

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Post-inflammatory hypopigmentation is a common acquired pigmentary disorder that is more prominent in skin of color, leading to great cosmetic and psychosocial implications. Often, a diagnosis with a pigmentary disorder can negatively impact an individual’s health-related quality of life and may result in stigma. Although most cases of post-inflammatory hypopigmentation resolve spontaneously over time, a systematic diagnostic approach can help with identifying the underlying etiology and informing treatment strategies. It can be due to cutaneous inflammation, sequelae of inflammatory or infectious dermatoses, or dermatologic procedures. Therefore, a thorough understanding of the epidemiology, patient history, physical exam findings, and clinical features of post-inflammatory hypopigmentation phenomenon can explain the primary cause to providers and allow for patient education. It is also important to understand the various therapeutic approaches available and the efficacy of these options, which will inform providers to choose the appropriate therapy for patients. Although algorithms exist for classifying acquired disorders of hypopigmentation, there are no established algorithms for the diagnosis and treatment of post-inflammatory hypopigmentation, which warrants further exploration and discourse.

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Hypopigmented lesions in pityriasis lichenoides chronica patients: Are they only post‐inflammatory hypopigmentation?

Cited by 3 publications

References 21 publications

Chronic and Stubborn Leuco-melanoderma in a Child: A Case Study

Chronic and Stubborn Leuco-melanoderma in a Child: A Case Study

Basement membrane thickness helps to differentiate hypopigmented mycosis fungoides from clinical and pathological mimickers

Post-Inflammatory Hypopigmentation: Review of the Etiology, Clinical Manifestations, and Treatment Options

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