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银屑病的光化学疗法:血液淋巴细胞中的DNA损伤

Photochemotherapy of psoriasis: DNA damage in blood lymphocytes.

作者信息

Friedmann P S, Rogers S

出版信息

J Invest Dermatol. 1980 Jun;74(6):440-3. doi: 10.1111/1523-1747.ep12544632.

Abstract

DNA synthesis assessed by 3H thymidine incorporation was measured in lymphocytes from patients with psoriasis receiving photochemotherapy with 8-methoxypsoralen (8-MOP) and UV-A (PUVA). The emission from the UVA source contained sufficient short wavelengths (UV-B) to impair 3H-thymidine incorporation but could be screened out with clear plastic screens. When lymphocytes were irradiated in vitro in a 1/10 dilution of plasma containing 8-MOP, increasing doses of UV-A produced progressive inhibition of phytohaemagglutinin (PHA)-induced DNA synthesis. Cells from patients given several previous treatments were inhibited significantly more than those from patients receiving their first exposure. This was also true for unirradiated cells sugesting either an accumulation of 8-MOP within cells, persistence of DNA damage or alteration of the lymphocyte population. Lymphocytes removed immediately after patients were irradiated showed less 3H thymidine incorporation than cells taken just prior to irradiation, which confirms that PUVA treatment exerts in vivo effects on circulating lymphocytes.

摘要

通过³H胸苷掺入法评估DNA合成,对接受8-甲氧基补骨脂素(8-MOP)和紫外线A(PUVA)光化学疗法的银屑病患者的淋巴细胞进行检测。紫外线A光源发出的光线含有足够的短波长(紫外线B),会损害³H-胸苷掺入,但可用透明塑料筛网滤除。当淋巴细胞在含有8-MOP的1/10稀释血浆中进行体外照射时,增加紫外线A剂量会对植物血凝素(PHA)诱导的DNA合成产生渐进性抑制。接受过数次治疗的患者的细胞受到的抑制明显大于首次接受治疗的患者的细胞。对于未照射的细胞也是如此,这表明细胞内8-MOP的积累、DNA损伤的持续存在或淋巴细胞群体的改变。患者接受照射后立即取出的淋巴细胞显示³H胸苷掺入比照射前刚取出的细胞少,这证实PUVA治疗对循环淋巴细胞有体内效应。

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