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兔慢性同种异型抑制维持中自身抗同种异型机制的细胞基础。

Cellular basis of an auto-anti-allotypic mechanism for the maintenance of chronic allotype suppression in the rabbit.

作者信息

Adler L T, Claassen E

机构信息

Department of Immunology, St Jude Children's Research Hospital, Memphis, Tennessee.

出版信息

Immunology. 1989 Feb;66(2):238-45.

Abstract

Immunocytochemical identification of antibody-forming cells (AFCs) in situ was used to test the hypothesis that the maintenance of chronic allotype suppression in heterozygous rabbits is the result of an autoimmune B-cell-mediated response. Appreciable numbers of B cells with antibody activity directed against the suppressed allotypic determinant were found in spleen and bone marrow sections of all chronically suppressed rabbits examined. Appropriate double-staining was used to determine that such cells were of the non-suppressed allotype. These cells were indistinguishable from anti-allotypic AFCs found in larger numbers in spleens of normal heterozygous rabbits that had been immunized against a heterologous allotypic determinant. Auto-anti-allotypic AFCs were not found in suppressed rabbits less than 8 week old, nor were they found in normal (non-suppressed) heterozygous rabbits or chimeric rabbits formed by the injection of histocompatible but allotype-mismatched lymphoid cells at birth. The findings reported here support the hypothesis that the long-term maintenance of allotype suppression in the rabbit may result from the suppressive activities of autoimmune B cells. It is suggested that the suppression of an allotype during the first few weeks of life could result in a loss of tolerance to a self-determinant. The kinetics of auto-anti-AFC production support this idea in showing that such cells are generated following the decline of the antibody used to induce suppression. The triggering event may be the emergence of B cells expressing the previously suppressed gene product.

摘要

采用原位免疫细胞化学鉴定抗体形成细胞(AFC),以检验如下假说:杂合兔慢性同种异型抑制的维持是自身免疫性B细胞介导反应的结果。在所检查的所有慢性抑制兔的脾脏和骨髓切片中,发现了相当数量的针对被抑制同种异型决定簇具有抗体活性的B细胞。采用适当的双重染色来确定这些细胞为非抑制同种异型。这些细胞与在针对异源同种异型决定簇免疫的正常杂合兔脾脏中大量发现的抗同种异型AFC没有区别。在8周龄以下的抑制兔中未发现自身抗同种异型AFC,在正常(非抑制)杂合兔或出生时注射组织相容性但同种异型不匹配淋巴细胞形成的嵌合兔中也未发现。此处报告的结果支持如下假说:兔同种异型抑制的长期维持可能源于自身免疫性B细胞的抑制活性。有人提出,在生命的最初几周对同种异型的抑制可能导致对自身决定簇的耐受性丧失。自身抗AFC产生的动力学支持这一观点,表明此类细胞是在用于诱导抑制的抗体下降后产生的。触发事件可能是表达先前被抑制基因产物的B细胞的出现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a38b/1385094/bd901121408a/immunology00146-0082-a.jpg

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