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病毒诱导的免疫复合物疾病:持续感染淋巴细胞性脉络丛脑膜炎病毒的小鼠循环中C1q结合复合物的遗传控制

Virus-induced immune complex disease: genetic control of C1q binding complexes in the circulation of mice persistently infected with lymphocytic choriomeningitis virus.

作者信息

Oldstone M B, Tishon A, Buchmeier M J

出版信息

J Immunol. 1983 Feb;130(2):912-8.

PMID:6217255
Abstract

Virus-antibody immune complex formation, deposition, and disease is a common manifestation in most mice persistently infected with lymphocytic choriomeningitis virus (LCMV). Although mice of several strains persistently infected with LCMV mount continuous anti-LCMV immune responses to the three virion structural polypeptides, the amount of antibody(s) made varies among strains. The formation of antibody to LCMV correlates with the detection of C1q binding materials (immune complexes) in the circulation; however, there is no correlation between the total amount of IgG and the C1q binding material. SWR/J mice (H2qq) are high responders (high levels of anti-LCMV antibodies, high C1q binding responses), whereas BALB/W mice (H-2dd) are low responders (low levels of anti-LCMV antibodies, low C1q binding responses). Sera from 37 SWR/J mice, 12 wk of age, bound 55.1% of offered 125I C1q compared to 8.4% for 37 age and sex-matched BALB/W mice. SWR/J mice made approximately 60-fold more antibody to LCMV than did BALB/W mice. To define the genetic factors involved, we used the C1q binding assay, high responder and low responder mice, their hybrid offspring, backcrosses of the hybrids to both high and low responder parents, and selected recombinant inbred mouse strains. From studies with BALB/W mice persistently infected with LCMV, we defined low C1q responder mice as those having binding activity of 18.4% or less (BALB/W mean C1q binding value + 2 SD). By using this criteria for 12-wk-old mice, 55/57 (96%) of SWR/J, 27/37 (73%) of F1(SxB or BxS), 13/21 (62%) of qq or 11/20 (55%) qd from F1 x SWR/J, and 6/13 (45%) qd from F1 x BALB/W were high C1q responders. In contrast, none of the 17 dd mice from the F1 x BALB/W cross were high responders. Thus, F1 hybrid mice are high responders (dominant) and data from backcrossing F1 hybrids to either high or low responder parents suggested the complexes associated with C1q binding was controlled by gene(s) in the H-2 complex. Support for the role of Ir gene(s) was provided by experiments showing LCMV persistently infected BALB/kae (H-2 KkIkDk) and recombinant inbred strains B10.A (KkIkDd) and A.TL (KsIkDd) were high C1q responders, whereas B10.A(5R) (KbIbDd) and BALB/cby (KdIdDd) were not. The wide scatter in C1q binding levels observed among C1q high responder mice and the production of C1q binding levels in F1 mice that are intermediate between high and low responder strains suggested that, in addition to H-2-linked genes, other non-H-2-linked genes also play a role in this response. The amount of C1q binding complexes in LCMV persistently infected mouse strains and their crosses was unrelated to the amounts of infectious virus carried in their sera. Despite the low C1q binding by sera of H-2dd mice that originated from mating F1 hybrid (qd) x BALB/WEHI (dd), these mice carried equivalent amounts of infectious virus as their qd littermates or qd and qq mice originated from F1 x SWR/J mice.

摘要

病毒 - 抗体免疫复合物的形成、沉积及相关疾病是大多数持续感染淋巴细胞性脉络丛脑膜炎病毒(LCMV)的小鼠的常见表现。尽管几种持续感染LCMV的品系小鼠对三种病毒粒子结构多肽持续产生抗LCMV免疫反应,但不同品系产生的抗体量有所不同。针对LCMV的抗体形成与循环中C1q结合物质(免疫复合物)的检测相关;然而,IgG总量与C1q结合物质之间并无关联。SWR/J小鼠(H2qq)是高反应者(抗LCMV抗体水平高,C1q结合反应高),而BALB/W小鼠(H - 2dd)是低反应者(抗LCMV抗体水平低,C1q结合反应低)。37只12周龄SWR/J小鼠的血清结合了所提供的125I C1q的55.1%,而37只年龄和性别匹配的BALB/W小鼠的血清仅结合了8.4%。SWR/J小鼠产生的针对LCMV的抗体比BALB/W小鼠多约60倍。为了确定其中涉及的遗传因素,我们使用了C1q结合试验、高反应者和低反应者小鼠、它们的杂交后代、杂交后代与高反应者和低反应者亲本的回交后代,以及选定的重组近交小鼠品系。通过对持续感染LCMV的BALB/W小鼠的研究,我们将低C1q反应者小鼠定义为那些结合活性为18.4%或更低的小鼠(BALB/W平均C1q结合值 + 2个标准差)。对于12周龄的小鼠使用此标准,55/57(96%)的SWR/J小鼠、27/37(73%)的F1(SxB或BxS)小鼠、13/21(62%)的F1×SWR/J杂交后代中的qq或11/20(55%)的qd以及13/21(62%)的F1×SWR/J杂交后代中的qd是高C1q反应者。相比之下,F1×BALB/W杂交后代中的17只dd小鼠均不是高反应者。因此,F1杂交小鼠是高反应者(显性),将F1杂交后代与高反应者或低反应者亲本回交的数据表明,与C1q结合相关的复合物由H - 2复合物中的基因控制。对Ir基因作用的支持来自实验,实验表明持续感染LCMV的BALB/kae(H - 2 KkIkDk)以及重组近交品系B10.A(KkIkDd)和A.TL(KsIkDd)是高C1q反应者,而B10.A(5R)(KbIbDd)和BALB/cby(KdIdDd)则不是。在C1q高反应者小鼠中观察到的C1q结合水平的广泛分散以及F1小鼠中C1q结合水平处于高反应者和低反应者品系之间的情况表明,除了与H - 2连锁的基因外,其他非H - 2连锁的基因也在这种反应中起作用。持续感染LCMV的小鼠品系及其杂交后代中C1q结合复合物的量与它们血清中携带的感染性病毒量无关。尽管源自F1杂交后代(qd)×BALB/WEHI(dd)交配的H - 2dd小鼠血清的C1q结合水平较低,但这些小鼠携带的感染性病毒量与它们的qd同窝小鼠或源自F1×SWR/J小鼠的qd和qq小鼠相当。

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