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外周血中的CD34+细胞将单纯疱疹病毒DNA片段转运至多形红斑(HAEM)患者的皮肤。

CD34+ cells in the peripheral blood transport herpes simplex virus DNA fragments to the skin of patients with erythema multiforme (HAEM).

作者信息

Ono Fumitake, Sharma Bhuvnesh K, Smith Cynthia C, Burnett Joseph W, Aurelian Laure

机构信息

Department of Pharmacology and Experimental Therapeutics, The University of Maryland School of Medicine, Baltimore, Maryland 21201, USA.

出版信息

J Invest Dermatol. 2005 Jun;124(6):1215-24. doi: 10.1111/j.0022-202X.2005.23712.x.

Abstract

Herpes simplex virus (HSV)-associated erythema multiforme (HAEM) is a recurrent disease characterized by the presence and expression of HSV DNA fragments in lesional skin. Our studies examined the mechanism of viral DNA transport to the skin of HAEM patients. CD34+ cells were isolated from the blood of normal subjects and HSV and HAEM patients during acute lesions and at quiescence. They were cultured with cytokines that favor their differentiation into Langerhans cells (LC) precursors (CD1a+/CD14-) and examined for HSV replication, HSV-induced cellular alterations, viral DNA fragmentation, and clearance. CD34+ cells from all study groups were non-permissive for HSV replication but infection favored their differentiation into CD1a+/CD14- LC precursors and upregulated E-cadherin expression, thereby assisting LC targeting to the skin. Only HAEM patients had CD34+ cells that retained viral DNA fragments, notably polymerase DNA, for at least 7 d of in vitro culture. The percentages of circulating CD34+ (and CD34+/CLA+) cells were significantly higher in HAEM patients at the time of acute lesions. A similar increase was not seen for HSV patients. The data are the first report implicating CD34+ cells in HAEM pathogenesis, likely by transporting HSV DNA fragments to lesional skin.

摘要

单纯疱疹病毒(HSV)相关的多形红斑(HAEM)是一种复发性疾病,其特征是在皮损中存在并表达HSV DNA片段。我们的研究探讨了病毒DNA转运至HAEM患者皮肤的机制。在急性皮损期和静止期,从正常受试者以及HSV和HAEM患者的血液中分离出CD34+细胞。将它们与有助于其分化为朗格汉斯细胞(LC)前体(CD1a+/CD14-)的细胞因子一起培养,并检测HSV复制、HSV诱导的细胞改变、病毒DNA片段化和清除情况。所有研究组的CD34+细胞均不支持HSV复制,但感染有利于它们分化为CD1a+/CD14- LC前体并上调E-钙黏蛋白表达,从而协助LC靶向至皮肤。只有HAEM患者的CD34+细胞在体外培养至少7天时仍保留病毒DNA片段,特别是聚合酶DNA。在急性皮损期,HAEM患者循环CD34+(和CD34+/CLA+)细胞的百分比显著更高。HSV患者未观察到类似的增加。这些数据首次表明CD34+细胞可能通过将HSV DNA片段转运至皮损皮肤而参与HAEM的发病机制。

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