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The effect of long‐term treatment with tacalcitol on the psoriatic epidermis. A flow cytometric analysis
Author(s) -
J.M. Mommers,
F.A.C.M. Castelijns,
B.A.M.P.A. Seegers,
Michelle M. van Rossum,
C.A.E.M. van Hooijdonk,
P.E.J. van Erp,
P.C.M. van de Kerkhof
Publication year - 1998
Publication title -
british journal of dermatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.304
H-Index - 179
eISSN - 1365-2133
pISSN - 0007-0963
DOI - 10.1046/j.1365-2133.1998.02411.x
Subject(s) - medicine , psoriasis , epidermis (zoology) , inflammation , lesion , population , dermatology , basal (medicine) , gastroenterology , pathology , environmental health , anatomy , insulin
During the last decade, novel analogues of 1α,25‐dihydroxy vitamin D 3 have been developed for the treatment of psoriasis. Recently, the efficacy of short‐term treatment with the novel derivative tacalcitol (1α,24‐dihydroxy vitamin D 3 ) has been documented. However, data on the long‐term effect of tacalcitol on psoriatic skin are sparse. In this study, we assessed the cell characteristics of the psoriatic epidermis after treatment with tacalcitol for up to 24 weeks. We investigated how long‐term treatment with tacalcitol modulates the percentages of differentiated keratinocytes, inflammation cells and basal keratinocytes, and the percentage of cells in the SG 2 M phase in the basal cell population. From 11 patients who were treated with tacalcitol for up to 18 months, we obtained single‐cell suspensions of a representative psoriatic lesion after 0, 8, 12, 18 and 24 weeks of treatment. A Psoriasis Area and Severity Index was performed at each visit as well. Cell suspensions were stained with markers for inflammation (Vim3B4), differentiation (RKSE60) and proliferation (TO‐PRO‐3 iodide) and analysed flow cytometrically. Clinically, patients improved significantly after 8 weeks of treatment. This clinical effect was preserved for the rest of the period of treatment with no further significant improvement. Proliferative activity also decreased significantly after 8 weeks of treatment. Proliferation did not show further significant decreases or habituation after 12, 18 and 24 weeks. For inflammation, no statistically reliable trends could be seen. Differentiation improved significantly after 8 weeks of treatment, but decreased again significantly after 12 weeks. In the period from 12 to 24 weeks, no further significant change was observed. We conclude that tacalcitol is an effective antipsoriatic drug. Prolonged treatment with tacalcitol will generally maintain improvement at the level reached after 8 weeks. Owing to the beneficial effect on both clinical state and proliferation, tacalcitol is likely to be an adequate maintenance therapy.