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Immunodeficiency due to a unique protracted developmental delay in the B-cell lineage.由于B细胞谱系中独特的长期发育延迟导致的免疫缺陷。
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Lesions and distribution of viral antigen following an experimental infection of young seronegative calves with virulent bovine virus diarrhea virus-type II.用强毒力的牛病毒性腹泻病毒II型对血清阴性的幼龄犊牛进行实验性感染后病毒抗原的损伤及分布情况
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派尔集合淋巴结中B细胞发育的两条不同途径。

Two distinct pathways of B-cell development in Peyer's patches.

作者信息

Griebel P J, Kugelberg B, Ferrari G

机构信息

Basel Institute for Immunology, Switzerland.

出版信息

Dev Immunol. 1996;4(4):263-77. doi: 10.1155/1995/46974.

DOI:10.1155/1995/46974
PMID:8924762
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2275965/
Abstract

The developmental biology of sheep ileal and jejunal Peyer's patches (PP) was investigated using corticosteroids to deplete immature B lymphocytes. During a 7-day treatment with dexamethasone, ileal PP follicular (iPf)B-cell proliferation was arrested and most iPfB-cells died. This resulted in follicular involution with the survival of mesenchymal cells. No iPfB-cell proliferation was detected in follicular remnants for 4 weeks postdexamethasone treatment, and during a subsequent 3-month period, there was limited iPfB-cell proliferation that resulted in a partial regeneration of follicles. Ileal PP involution was also associated with a severe B lymphopenia that persisted for over 14 weeks and was characterized by the survival of primarily isotype-switched and CD5+ sIgM+ B-cells in blood. In contrast, the size of jejunal PP follicles was reduced following dexamethasone treatment, but intrafollicular B-cell proliferation was not arrested. Furthermore, within 4 weeks, the jejunal PP follicles had recovered in size and cellularity and there was no disruption in IgA plasma-cell production. Thus, dexamethasone selectively depleted iPfB-cells and revealed that the ileal and jejunal PPs contain functionally distinct B-cell populations. The partial regeneration of the iPfB-cell population indicated that either an intrafollicular, corticosteroid-resistant B-stem cell existed or that ileal PP follicles can be repopulated by circulating B-cells. Finally, the association between ileal PP involution and the absence of circulating, CD5- B-cells confirmed that this lymphoid tissue provides an essential environment for conventional sIgM+ B-cell development.

摘要

利用皮质类固醇耗尽未成熟B淋巴细胞,对绵羊回肠和空肠派伊尔结(PP)的发育生物学进行了研究。在用地塞米松进行为期7天的治疗期间,回肠PP滤泡(iPf)B细胞增殖被阻断,大多数iPfB细胞死亡。这导致滤泡退化,间充质细胞存活。地塞米松治疗后4周,在滤泡残余物中未检测到iPfB细胞增殖,在随后的3个月期间,iPfB细胞增殖有限,导致滤泡部分再生。回肠PP退化还与严重的B淋巴细胞减少有关,这种减少持续超过14周,其特征是血液中主要是同种型转换和CD5+sIgM+B细胞存活。相比之下,地塞米松治疗后空肠PP滤泡大小减小,但滤泡内B细胞增殖未被阻断。此外,在4周内,空肠PP滤泡在大小和细胞数量上已恢复,并且IgA浆细胞产生没有受到干扰。因此,地塞米松选择性地耗尽了iPfB细胞,并揭示回肠和空肠PP含有功能不同的B细胞群体。iPfB细胞群体的部分再生表明,要么存在滤泡内抗皮质类固醇的B干细胞,要么回肠PP滤泡可以由循环B细胞重新填充。最后,回肠PP退化与循环中CD5-B细胞缺失之间的关联证实,这种淋巴组织为传统sIgM+B细胞发育提供了必要的环境。