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NZB 小鼠和 DBA/2 小鼠之间可克隆 B 淋巴细胞和髓系祖细胞异常的相互转移。

Reciprocal transfer of abnormalities in clonable B lymphocytes and myeloid progenitors between NZB and DBA/2 mice.

作者信息

Jyonouchi H, Kincade P W, Good R A, Fernandes G

出版信息

J Immunol. 1981 Sep;127(3):1232-5.

PMID:6973583
Abstract

Previous studies in this laboratory revealed that NZB mice have abnormalities of myeloid progenitor populations from an early age such that they are poorly responsive to a particular type of colony-stimulating activity (CSA). In addition, these mice develop abnormally high numbers of B cells that can be cloned in semisolid agar cultures and that are atypical in resisting inhibition by anti-mu antibodies. To investigate whether these abnormalities, like other autoimmune phenomena studied previously, are transferrable with hemopoietic cell grafts, we performed reciprocal bone marrow transplants between NZB and normal DBA/2 mice. Irradiated control mice given syngeneic marrow did not change with respect to any of the parameters that were measured. In contrast, DBA/2 recipients of NZB marrow were indistinguishable from NZB mice in terms of CSA responses and incidences of anti-mu resistant B cells. The proportions but not total numbers of clonable B cells ere elevated in these mice until at least 16 wk after grafting. Conversely, NZB mice given DBA/2 cells had all of the normal characteristics of DBA/2 mice. Transplantation did not cause significant changes in hematocrits, reticulocyte counts, or spleen weights. Therefore, all elements necessary for expression of these lymphoid and nonlymphoid abnormalities of NZB mice are intrinsic to radiosensitive hemopoietic cells.

摘要

本实验室先前的研究表明,NZB小鼠从幼年起就存在髓系祖细胞群体异常,以至于它们对特定类型的集落刺激活性(CSA)反应不佳。此外,这些小鼠体内可在半固体琼脂培养中克隆的B细胞数量异常增多,且这些B细胞具有非典型性,能抵抗抗μ抗体的抑制作用。为了研究这些异常情况是否像先前研究的其他自身免疫现象一样,可通过造血细胞移植进行转移,我们在NZB小鼠和正常DBA/2小鼠之间进行了相互骨髓移植。接受同基因骨髓的经照射对照小鼠在所测量的任何参数方面均未发生变化。相比之下,接受NZB骨髓的DBA/2受体小鼠在CSA反应和抗μ抗性B细胞发生率方面与NZB小鼠并无差异。在这些小鼠中,可克隆B细胞的比例而非总数在移植后至少16周内一直升高。相反,接受DBA/2细胞的NZB小鼠具有DBA/2小鼠的所有正常特征。移植并未导致血细胞比容、网织红细胞计数或脾脏重量发生显著变化。因此,NZB小鼠这些淋巴样和非淋巴样异常表达所必需的所有要素都存在于对辐射敏感的造血细胞中。

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