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氨肽酶A对B细胞前体增殖的调节

Regulation of B cell precursor proliferation by aminopeptidase A.

作者信息

Welch P A

机构信息

Department of Pediatrics, University of Alabama, Birmingham 35294, USA.

出版信息

Int Immunol. 1995 May;7(5):737-46. doi: 10.1093/intimm/7.5.737.

DOI:10.1093/intimm/7.5.737
PMID:7547701
Abstract

The BP-1/6C3 molecule expressed by early B lineage cells and some stromal cells has been identified as aminopeptidase A (APA). We have previously demonstrated that IL-7 selectively induces BP-1/APA expression by pre-B cells coincident with their growth. Here we directly demonstrate that BP-1 is preferentially expressed by the proliferating subpopulation of normal B cell progenitors. Furthermore, when non-adherent BALB/c bone marrow cells were incubated with IL-7 in the presence of purified BP-1 antibody, B cell precursor proliferation was markedly inhibited. Modulation of the BP-1/6C3 antigen did not occur in the presence of the BP-1 antibody, but APA enzymatic activity was significantly inhibited. The 6C3 antibody, which recognizes a different epitope on the APA molecule, had no effect on either B cell precursor proliferation or APA enzyme activity. We hypothesized that neutralization of APA by the BP-1 antibody results in inhibition of IL-7 driven B cell precursor proliferation. However, when isolated 14.8+ bone marrow cells were cultured with IL-7 in the presence of the BP-1 antibody, no inhibition of proliferation occurred. This data suggested that the effect of the BP-1 antibody might be related to the action of APA on peptides in the marrow microenvironment which are not present in cultures of isolated B cell precursors. The addition of irradiated non-adherent bone marrow cells to the 14.8+ cell cultures restored the inhibitory effect of the BP-1 antibody. Based on these observations, we propose that APA cleaves a small peptide which serves as a natural inhibitor of B cell precursor proliferation.

摘要

早期B淋巴细胞系细胞和一些基质细胞表达的BP-1/6C3分子已被鉴定为氨肽酶A(APA)。我们之前已经证明,IL-7在pre-B细胞生长的同时选择性诱导其BP-1/APA表达。在此我们直接证明,BP-1在正常B细胞祖细胞的增殖亚群中优先表达。此外,当非贴壁的BALB/c骨髓细胞在纯化的BP-1抗体存在的情况下与IL-7一起孵育时,B细胞前体增殖受到明显抑制。在BP-1抗体存在的情况下,BP-1/6C3抗原未发生调节,但APA酶活性受到显著抑制。识别APA分子上不同表位的6C3抗体对B细胞前体增殖或APA酶活性均无影响。我们推测,BP-1抗体对APA的中和作用导致IL-7驱动的B细胞前体增殖受到抑制。然而,当分离的14.8+骨髓细胞在BP-1抗体存在的情况下与IL-7一起培养时,增殖未受到抑制。该数据表明,BP-1抗体的作用可能与APA对骨髓微环境中肽的作用有关,而这些肽在分离的B细胞前体培养物中不存在。向14.8+细胞培养物中添加经辐照的非贴壁骨髓细胞可恢复BP-1抗体的抑制作用。基于这些观察结果,我们提出APA裂解一种小肽,该小肽作为B细胞前体增殖的天然抑制剂。

相似文献

1
Regulation of B cell precursor proliferation by aminopeptidase A.氨肽酶A对B细胞前体增殖的调节
Int Immunol. 1995 May;7(5):737-46. doi: 10.1093/intimm/7.5.737.
2
Bone marrow stromal cells and interleukin-7 induce coordinate expression of the BP-1/6C3 antigen and pre-B cell growth.骨髓基质细胞和白细胞介素-7诱导BP-1/6C3抗原的协同表达和前B细胞生长。
Int Immunol. 1990;2(8):697-705. doi: 10.1093/intimm/2.8.697.
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The enigmatic role of glutamyl aminopeptidase (BP-1/6C3 antigen) in immune system development.谷氨酰胺氨基肽酶(BP-1/6C3抗原)在免疫系统发育中的神秘作用。
Immunol Rev. 1998 Feb;161:71-7. doi: 10.1111/j.1600-065x.1998.tb01572.x.
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Aminopeptidase A activity of the murine B-lymphocyte differentiation antigen BP-1/6C3.小鼠B淋巴细胞分化抗原BP-1/6C3的氨肽酶A活性
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T and B cell development in BP-1/6C3/aminopeptidase A-deficient mice.BP-1/6C3/氨肽酶A缺陷小鼠中T细胞和B细胞的发育
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The mouse BP-1 gene: structure, chromosomal localization, and regulation of expression by type I interferons and interleukin-7.小鼠BP-1基因:结构、染色体定位以及I型干扰素和白细胞介素-7对其表达的调控
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Widespread tissue distribution of aminopeptidase A, an evolutionarily conserved ectoenzyme recognized by the BP-1 antibody.氨肽酶A在组织中广泛分布,它是一种由BP-1抗体识别的进化保守的胞外酶。
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Molecular cloning of the murine BP-1/6C3 antigen: a member of the zinc-dependent metallopeptidase family.小鼠BP-1/6C3抗原的分子克隆:锌依赖性金属肽酶家族的一员。
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Normal B cell precursors responsive to recombinant murine IL-7 and inhibition of IL-7 activity by transforming growth factor-beta.对重组小鼠白细胞介素-7有反应的正常B细胞前体以及转化生长因子-β对白细胞介素-7活性的抑制作用。
J Immunol. 1989 Jun 1;142(11):3875-83.

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