循环免疫球蛋白G在清除肠道呼肠孤病毒感染中可发挥关键作用。
Circulating immunoglobulin G can play a critical role in clearance of intestinal reovirus infection.
作者信息
Barkon M L, Haller B L, Virgin H W
机构信息
Center for Immunology, Washington University School of Medicine, St. Louis, Missouri 63110, USA.
出版信息
J Virol. 1996 Feb;70(2):1109-16. doi: 10.1128/JVI.70.2.1109-1116.1996.
Reoviruses are encapsidated double-stranded RNA viruses that cause systemic disease in mice after peroral (p.o.) inoculation and primary replication in the intestine. In this study, we define components of the immune system involved in the clearing of reovirus from the proximal small intestine. The intestines of immunocompetent adult CB17, 129, and C57BL/6 mice were cleared of reovirus serotype 3 clone 9 (T3C9) within 7 days of p.o. inoculation. Antigen-specific lymphocytes were important for the clearance of intestinal infection, since severe combined immunodeficient (SCID) mice failed to clear T3C9 infection. To define specific immune components required for intestinal clearance, reovirus infection of mice with null mutations in the immunoglobulin M (IgM) transmembrane exon (MuMT; B cell and antibody deficient) or beta 2 microglobulin gene (beta 2-/-; CD8 deficient) was evaluated. beta 2-/- mice cleared reovirus infection with normal kinetics, while MuMT mice showed delayed clearance of T3C9 7 to 11 days after p.o. inoculation. Adoptive transfer of splenic lymphocytes from reovirus-immune CB17 mice inhibited growth of T3C9 in CB17 SCID mouse intestine 11 days after p.o. inoculation. The efficiency of viral clearance by adoptively transferred cells was significantly diminished by depletion of B cells prior to adoptive transfer. Results in SCID and MuMT mice demonstrate an important role for B cells or IgG in clearance of reovirus from the intestines. Polyclonal reovirus-immune rabbit serum, protein A-purified immune IgG, and murine monoclonal IgG2a antibody specific for reovirus outer capsid protein sigma 3 administered intraperitoneally all normalized clearance of reovirus from intestinal tissue in MuMT mice. This result demonstrates an IgA-independent role for IgG in the clearance of intestinal virus infection. Polyclonal reovirus-immune serum also significantly decreased reovirus titers in the intestines of SCID mice, demonstrating a T-cell-independent role for antibody in the clearance of intestinal reovirus infection. B cells and circulating IgG play an important role in the clearance of reovirus from intestines, suggesting that IgG may play a more prominent functional role at mucosal sites of primary viral replication than was previously supposed.
呼肠孤病毒是一种衣壳包裹的双链RNA病毒,经口接种后在小鼠肠道内进行初次复制,并引发全身性疾病。在本研究中,我们确定了参与从小肠近端清除呼肠孤病毒的免疫系统组成部分。免疫功能正常的成年CB17、129和C57BL/6小鼠在经口接种后7天内,其肠道内的呼肠孤病毒3型克隆9(T3C9)被清除。抗原特异性淋巴细胞对于清除肠道感染很重要,因为严重联合免疫缺陷(SCID)小鼠无法清除T3C9感染。为了确定肠道清除所需的特定免疫成分,我们评估了免疫球蛋白M(IgM)跨膜外显子(MuMT;B细胞和抗体缺陷)或β2微球蛋白基因(β2-/-;CD8缺陷)发生无效突变的小鼠的呼肠孤病毒感染情况。β2-/-小鼠以正常动力学清除呼肠孤病毒感染,而MuMT小鼠在经口接种后7至11天显示出T3C9清除延迟。在经口接种11天后,将来自呼肠孤病毒免疫的CB17小鼠的脾淋巴细胞进行过继转移,可抑制CB17 SCID小鼠肠道内T3C9的生长。在过继转移前通过耗尽B细胞,过继转移细胞清除病毒的效率显著降低。SCID和MuMT小鼠的结果表明B细胞或IgG在从小肠清除呼肠孤病毒中起重要作用。腹腔注射多克隆呼肠孤病毒免疫兔血清、蛋白A纯化的免疫IgG以及针对呼肠孤病毒外衣壳蛋白σ3的鼠单克隆IgG2a抗体,均可使MuMT小鼠肠道组织中呼肠孤病毒的清除恢复正常。这一结果证明了IgG在清除肠道病毒感染中不依赖IgA的作用。多克隆呼肠孤病毒免疫血清也显著降低了SCID小鼠肠道内的呼肠孤病毒滴度,证明了抗体在清除肠道呼肠孤病毒感染中不依赖T细胞的作用。B细胞和循环IgG在从小肠清除呼肠孤病毒中起重要作用,这表明IgG在原发性病毒复制的黏膜部位可能发挥比以前认为的更突出的功能作用。
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