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与肠道蠕虫感染相关的慢性免疫激活会导致信号转导受损和无反应性。

Chronic immune activation associated with intestinal helminth infections results in impaired signal transduction and anergy.

作者信息

Borkow G, Leng Q, Weisman Z, Stein M, Galai N, Kalinkovich A, Bentwich Z

机构信息

R. Ben-Ari Institute of Clinical Immunology and AIDS Center, Kaplan Medical Center, Hebrew University Hadassah Medical School, Rehovot, Israel.

出版信息

J Clin Invest. 2000 Oct;106(8):1053-60. doi: 10.1172/JCI10182.

Abstract

Helminthic parasites cause widespread, persistent infections in humans. The immigration of Ethiopians to Israel (a group denoted here by "Eth."), many of them infested with helminths and in a chronic immune-activation state, enabled us to investigate the effects of such immune activation on immune responses. We studied the immune profile and immune functions of 190 Eth. and Israeli non-Eth. (Isr.) highly, partially, or non-immune-activated individuals. Immune cells from highly immune-activated individuals were defective in several signaling responses, all of which were restored gradually following anti-helminthic treatment. These cells showed poor transmembrane signaling, as seen by the phosphorylation of various tyrosine kinases and of the MAPK kinases, ERK1/2 and p38; deficient degradation of phosphorylated IkappaBalpha; increased expression of cytotoxic T lymphocyte-associated antigen 4 (CTLA-4), which appears to block proliferative responses in these cells; decreased beta-chemokine secretion by CD8(+) cells after stimulation; and reduced proliferation to recall antigen stimulation. Highly immune-activated individuals also showed decreased delayed-type skin hypersensitivity responses to recall antigen before deworming. These findings support the notion that chronic helminthic infections cause persistent immune activation that results in hyporesponsiveness and anergy. Such impaired immune functions may diminish the capacity of these individuals to cope with infections and to generate cellular protective immunity after vaccination.

摘要

蠕虫寄生虫在人类中引起广泛的持续性感染。埃塞俄比亚人移民到以色列(这里用“Eth.”表示这一群体),其中许多人感染了蠕虫并处于慢性免疫激活状态,这使我们能够研究这种免疫激活对免疫反应的影响。我们研究了190名埃塞俄比亚人和以色列非埃塞俄比亚人(“Isr.”)高度、部分或未免疫激活个体的免疫特征和免疫功能。高度免疫激活个体的免疫细胞在几种信号反应中存在缺陷,在抗蠕虫治疗后所有这些缺陷都逐渐恢复。这些细胞表现出较差的跨膜信号传导,如各种酪氨酸激酶以及丝裂原活化蛋白激酶(MAPK)激酶ERK1/2和p38的磷酸化所示;磷酸化的IκBα降解不足;细胞毒性T淋巴细胞相关抗原4(CTLA-4)表达增加,这似乎会阻断这些细胞的增殖反应;刺激后CD8(+)细胞分泌β趋化因子减少;对回忆抗原刺激的增殖减少。高度免疫激活个体在驱虫前对回忆抗原的迟发型皮肤超敏反应也降低。这些发现支持了慢性蠕虫感染会导致持续性免疫激活,进而导致反应低下和无反应性的观点。这种受损的免疫功能可能会削弱这些个体应对感染以及接种疫苗后产生细胞保护性免疫的能力。

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