Pedram Geraminejad scite author profile

Basal cell carcinoma (BCC) is the most common cutaneous skin malignancy. BCC generally has a clinical course characterized by slow growth, minimal soft tissue invasiveness, and a high cure rate. Occasionally, however, BCC behaves aggressively with deep invasion, recurrence, and potential regional and distant metastasis. Several factors, including tumor size, duration, histology, and perineural spread, have been postulated as markers of the aggressive BCC phenotype. It is undetermined whether intrinsic biological factors within certain subsets of BCC predispose these tumors toward an inherently aggressive behavior, or whether any BCC with inadequate early management may assume this phenotype. Review of the pertinent literature on this topic suggests that both intrinsic biological factors and extrinsic management factors play a role in the development and progression of aggressive BCC.

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Kaposi's sarcoma and other manifestations of human herpesvirus 8

Geraminejad

Memar

Aronson

et al. 2002

Journal of the American Academy of Dermatology

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Alpha-1-antitrypsin associated panniculitis: The MS variant

Geraminejad¹,

DeBloom²,

Walling³

et al. 2004

Journal of the American Academy of Dermatology

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Poxviruses

Memar¹,

Geraminejad²,

Arany³

et al. 2002

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Antimalarial lichenoid tissue reactions in patients with pre-existing lupus erythematosus

Geraminejad

Stone

Sontheimer

2004

Lupus

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Recently a number of cases of drug induction or exacerbation of lupus erythematosus (LE) specific skin disease have been described in the literature. Many of the responsible medications are also known for their ability to induce a lichenoid tissue reaction. Aminoquinoline antimalarials are currently the first line of therapy in cutaneous LE specific skin disease. Lichenoid tissue reactions are among the most common cutaneous side effects of aminoquinolone antimalarials. We report three cases of aminoquinolone antimalarial induced or exacerbated LE specific skin disease. We also review the pathophysiology of LE specific skin disease and propose a mechanism by which induction of the lichenoid tissue reaction may result in Koebnerization of LE specific skin lesions.

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