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在出生后的整个生命过程中,胸腺细胞生成由血源性前体细胞维持。联体小鼠研究。

Thymocytopoiesis is maintained by blood-borne precursors throughout postnatal life. A study in parabiotic mice.

作者信息

Donskoy E, Goldschneider I

机构信息

Department of Pathology, Newington Children's Hospital, CT 06111.

出版信息

J Immunol. 1992 Mar 15;148(6):1604-12.

PMID:1347301
Abstract

This study was designed to resolve the long standing controversy as to whether hematogenous precursors or resident intrathymic precursors maintain thymocytopoiesis in postnatal life. The kinetics of thymic chimerism was examined over a 21-wk period in 105 pairs of nonirradiated, Thy-1-alloantigen-disparate, parabiotic B10.S mice. Thymic chimerism reached reached maximum levels of 25% in the Thy-1b and 16% in the Thy-1a partners (mean 20.5% and 9.8%, respectively) 6 to 7 wk after parabiotic union. Most of the donor-origin thymocytes were located in the thymus cortex and expressed high levels of Thy-1 Ag and terminal deoxynucleotidyl transferase. Thymic chimerism did not reach 50% because circulating prothymocytes, unlike peripheral T cells, do not distribute randomly in the blood of parabiotic partners. This was shown in irradiated pairs of Thy-1-alloantigen-identical parabiotic mice, one member of which was injected i.v. with Thy-1-alloantigen-disparate bone marrow cells. Only 10% of the total donor-origin prothymocyte activity was detected in the opposite parabiont 72 h later. Similarly, the level of thymic chimerism in nonirradiated, Thy-1-alloantigen-disparate parabionts closely corresponded to the donor: host ratio of prothymocytes in the blood (i.e., between 10 and 20%), as determined directly by an intrathymic adoptive transfer assay. The continued dependence of thymic chimerism on blood-borne precursors was formally demonstrated by surgically separating mice 9 wk after parabiosis. Twelve weeks later, thymic chimerism was 50 to 80% lower in the separated parabionts than in sham-operated controls. The possible role of "stress" in initiating or maintaining thymic chimerism during parabiosis appeared to be excluded by the existence of similar kinetics of thymocytopoiesis (including the onset of thymic involution) in parabiotic and nonparabiotic mice; and by the occurrence of similar levels of thymic chimerism in adrenalectomized and nonadrenalectomized parabiotic mice. Thus these experiments demonstrate that the maintenance of thymocytopoiesis in postnatal life, as in prenatal life, is primarily dependent upon blood-borne prothymocytes, and that intrathymic precursors are replaced at an average rate of 2 to 3%/day.

摘要

本研究旨在解决长期以来关于出生后是血源性前体细胞还是胸腺内驻留前体细胞维持胸腺细胞生成的争议。在105对未受照射、Thy-1同种异体抗原不同的联体B10.S小鼠中,观察了21周内胸腺嵌合的动力学变化。联体结合6至7周后,胸腺嵌合在Thy-1b伙伴中达到最高水平25%,在Thy-1a伙伴中达到16%(平均分别为20.5%和9.8%)。大多数供体来源的胸腺细胞位于胸腺皮质,表达高水平的Thy-1抗原和末端脱氧核苷酸转移酶。胸腺嵌合未达到50%,因为与外周T细胞不同,循环中的前胸腺细胞不会在联体伙伴的血液中随机分布。这在受照射的Thy-1同种异体抗原相同的联体小鼠中得到证实,其中一只静脉注射了Thy-1同种异体抗原不同的骨髓细胞。72小时后,在对侧联体中仅检测到10%的总供体来源前胸腺细胞活性。同样,未受照射、Thy-1同种异体抗原不同的联体中胸腺嵌合水平与血液中前胸腺细胞的供体:宿主比例密切相关(即10%至20%之间),这是通过胸腺内过继转移试验直接测定的。联体9周后通过手术分离小鼠,正式证明了胸腺嵌合对血源性前体细胞的持续依赖性。12周后,分离的联体中胸腺嵌合比假手术对照组低50%至80%。联体期间“应激”在启动或维持胸腺嵌合中的可能作用似乎被排除,因为联体和非联体小鼠胸腺细胞生成的动力学相似(包括胸腺退化的开始);并且肾上腺切除和未肾上腺切除的联体小鼠中胸腺嵌合水平相似。因此,这些实验表明,出生后如同出生前一样,胸腺细胞生成的维持主要依赖于血源性前胸腺细胞,并且胸腺内前体细胞以平均每天2%至3%的速率被替代。

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