CELLULAR-RESPONSES TO THE INTRADERMAL INJECTION OF RECOMBINANT HUMAN GAMMA-INTERFERON IN LEPROMATOUS LEPROSY PATIENTS
- 1 August 1987
- journal article
- research article
- Vol. 128 (2), 345-353
Abstract
The local response to a single intradermal injection of 10 .mu.g recombinant .gamma.-interferon (rIFN.gamma.) has been studied in 17 patients with lepromatous leproxy. Of these, 2 patients additionally received two intradermal injection of 10 .mu.g rIFN.gamma. at another site. The results were compared with those of 3 patients who received three injections of the same dose at a single site in an earlier study. One to 7 days after lymphokine administration 4-mm punch biopsies were obtained and examined for cellular alterations in the dermis and epidermis. This allowed a kinetic analysis of mononuclear cell infiltration, keratinocyte proliferation and differentiation, and Langerhans cell redistribution. At 24 hours, the migration of large numbers of helper T cells and monocytes was already prominent and associated with induration. Mononuclear cell accumulation peaked at 72 hours but then persisted for 5-7 days. Only small numbers (one-third or less of total T cells) of suppressor/cytotoxic T cells were present at any time, and granulocytes were absent. Two daily injections of rIFN.gamma. led to a more intense accumulation of cells. Ten .mu.g of rIFN.gamma. resulted in enhanced keratinocyte proliferation, Ia expression, and thickening of the epidermis. At 24-48 hours major histocompatibility Class II (Ia) antigen was first noted on the dividing cells of the basal layer. By 72-96 hours the entire epidermis exhibited strong expression of Ia antigen on cell surfaces. Repeated doses of lymphokine accentuated these changes and resulted in a more prompt keratinization and sloughing of this layer. Whereas a single dose of rIFN.gamma. resulted in the upward movement of T6+ Langerhans cells (LCs) in the epidermis, two injections led to a 50% reduction in their numbers and three doses were associated with an almost total loss of detectable T6+ LCs from the epidermis. These are probably sloughed along with keratinocytes. In contrast to the situation with a delayed immune response in the skin (purified protein derivative), no LCs accumulated in the dermis in association with helper T cells.This publication has 30 references indexed in Scilit:
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