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Cell death and thymic export during fetal life

✍ Scribed by Joanne E. Holder; Elizabeth A. Washington; Craig P. Cunningham; Ross N. P. Cahill; Wayne G. Kimpton


Publisher
John Wiley and Sons
Year
2006
Tongue
English
Weight
129 KB
Volume
36
Category
Article
ISSN
0014-2980

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✦ Synopsis


Abstract

In the fetus the peripheral T cell pool expands as the fetus grows, but the mechanisms that regulate T cell homeostasis during fetal life are unknown. Here, we show that the peripheral T cell pool in the sheep fetus is established by the export from the fetal thymus of twice as many CD8^+^ as CD4^+^ thymic emigrants every day. Clonal deletion of CD4^+^ thymocytes in the fetal thymus appeared to be more stringent than was the case for CD8^+^ thymocytes because only 1 in 35 single‐positive CD4 (SPCD4) thymocytes was exported from the thymus whereas the majority (2/3) of the single‐positive CD8 (SPCD8) thymocytes were exported from the fetal thymus each day. Furthermore, within the thymus, the number of apoptotic SPCD4 thymocytes was 40 times greater than the number of apoptotic SPCD8 thymocytes. A tissue‐specific migration of CD8^+^ emigrants localizing in the spleen was also established in the fetus in contrast to CD4^+^ emigrants, which migrated randomly to spleen and LN.


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Changes in thymic export of L-selectin+
✍ Deborah A. Witherden; Nevin J. Abernethy; Wayne G. Kimpton; Ross N. P. Cahill 📂 Article 📅 1994 🏛 John Wiley and Sons 🌐 English ⚖ 646 KB

## Abstract We have used the technique of __in situ__ intrathymic injection of fluorescein isothiocyanate to examine L‐selectin expression on γδ and αβ T cells immediately after emigrating from the thymus of fetal and postnatal animals. We found that the percentage of L‐selectin^+^ thymocytes expor