Figure 1
Impaired negative selection of CCR7-deficient thymocytes in vivo. Nine-week-old C57BL/6 (+/+) and CCR7−/− (−/−) mice were intravenously injected with PBS or 200 μg of anti-CD3 mAb. Forty-two hours after injection, thymocytes were quantified, stained with antibodies to CD3, CD4, CD24, and CD8, and analyzed by flow cytometry. CD24 expression was analyzed to identify the semimature CD4+CD8−CD24high population undergoing negative selection after TCR ligation. (A) Proportions of CD4 SP and DP cells in the thymus of mice injected with PBS and mice injected with anti-CD3 mAb, demonstrating the depletion of the DP population in wild-type but not in mutant animals. (B) Proportions of CD4+CD8−CD24high cells in the thymi of mice injected with anti-CD3 mAb. Note that in contrast to wild-type mice, only a minority of CD4+CD8−CD24high cells have been depleted in CCR7-deficient animals after antibody administration. (C) Bone marrow of CD45.2 CCR7−/− mice was mixed with bone marrow of CD45.1 wild-type mice at ratio of 1:1 and transferred into irradiated CD45.1 wild-type recipients. Lack of depletion of CCR7-deficient DP and CD4+CD8−CD24high cells in a wild-type thymus environment indicates that an intrinsic defect in these thymocytes is responsible for the resistance of these cells to undergo depletion after TCR stimulation.

Impaired negative selection of CCR7-deficient thymocytes in vivo. Nine-week-old C57BL/6 (+/+) and CCR7−/− (−/−) mice were intravenously injected with PBS or 200 μg of anti-CD3 mAb. Forty-two hours after injection, thymocytes were quantified, stained with antibodies to CD3, CD4, CD24, and CD8, and analyzed by flow cytometry. CD24 expression was analyzed to identify the semimature CD4+CD8CD24high population undergoing negative selection after TCR ligation. (A) Proportions of CD4 SP and DP cells in the thymus of mice injected with PBS and mice injected with anti-CD3 mAb, demonstrating the depletion of the DP population in wild-type but not in mutant animals. (B) Proportions of CD4+CD8CD24high cells in the thymi of mice injected with anti-CD3 mAb. Note that in contrast to wild-type mice, only a minority of CD4+CD8CD24high cells have been depleted in CCR7-deficient animals after antibody administration. (C) Bone marrow of CD45.2 CCR7−/− mice was mixed with bone marrow of CD45.1 wild-type mice at ratio of 1:1 and transferred into irradiated CD45.1 wild-type recipients. Lack of depletion of CCR7-deficient DP and CD4+CD8CD24high cells in a wild-type thymus environment indicates that an intrinsic defect in these thymocytes is responsible for the resistance of these cells to undergo depletion after TCR stimulation.

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal