In the doses and schemes used in this study, co-administration of oral tamoxifen and Sb resulted in higher cure rates in comparison with the standard scheme of treatment, although not to statistically significant levels.
Melanomas can arise either de novo (70%) or from pre-existing
melanocytic lesions (30%). Of the latter, most cases arise at the dermoepidermal
junction from small congenital or acquired non-blue nevi while only a few arise
from blue nevi, notably the cellular subtype and less commonly the common
(dendritic) type. Melanomas that arise from blue nevi usually occur on the scalp
with greater frequency, as in the case described. Although previous studies have
discussed melanoma arising from giant congenital blue nevi, few have discussed
those arising from intermediate blue nevi. We present a case of a 52-yearold man
with melanoma on the scalp evolving from an intermediate congenital common blue
nevus.
Background
The treatment of cutaneous leishmaniasis is a challenge. A better understanding of the in situ mechanisms involved in the evolution and cure of the disease is essential for the development of new therapies.
Objective
Correlate histopathological and immunological characteristics of cutaneous leishmaniasis lesions with clinical outcome after different treatment regimens.
Methods
The authors analyzed cellular infiltration and immunohistochemistry staining for CD4, CD8 and IL-17 in biopsy samples from 33 patients with cutaneous leishmaniasis before treatment. All patients were recruited in a randomized clinical trial at Corte de Pedra (Bahia-Brazil) and assigned to receive Glucantime®, Glucantime® + Oral Tamoxifen or Glucantime® + Topical Tamoxifen. Patients were followed for 2 to 6 months to define disease outcome.
Results
A similar expression of CD4, CD8 and IL-17 was observed in lesion samples regardless of clinical outcome. In general, a higher amount of CD8 cells were observed compared with CD4 cells. An important observation was that all patients whose cellular infiltrate did not contain plasma cells were cured after treatment.
Study limitations
Isolated quantification of TCD8 and IL-17 using immunohistochemistry is insufficient to analyze the role of these molecules in the immunopathogenesis of cutaneous leishmaniasis. In addition, the expansion of the immunohistochemistry panel would allow a more complete analysis of the immune response in situ.
Conclusions
The absence of plasma cells in cutaneous leishmaniasis lesions was related to a favorable therapeutic outcome.
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