TCF1highPD-1+Ly108+CD8+ T Cells Are Associated with Graft Preservation in Sensitized Mice Treated with Non-Fc Receptor-Binding CD3 Antibodies.

Q3 Medicine ImmunoHorizons Pub Date : 2024-04-01 DOI:10.4049/immunohorizons.2300117
Takuji Ota, R. Goto, Takuya Harada, Agustina Forgioni, Ryo Kanazawa, Yoshikazu Ganchiku, N. Kawamura, Masaaki Watanabe, M. Fukai, Tsuyoshi Shimamura, A. Taketomi
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Abstract

The non-Fc-binding anti-CD3 Ab [anti-CD3F(ab')2] can induce graft acceptance depending on the therapeutic window in a rodent heart transplant model. The delayed protocol allows for early graft infiltration of lymphocytes, which may behave in an inhibitory manner. We investigated the most effective protocol for anti-CD3F(ab')2 in sensitized conditions to confirm the evidence for clinical application. C57BL/6 mice were sensitized with BALB/c tail skin grafts and transplanted with BALB/c heart grafts at 8-12 wk after sensitization. Fifty micrograms of anti-CD3F(ab')2 was administered daily for 5 consecutive days on days 1-5 (day 1 protocol) or days 3-7 (delayed protocol). In nonsensitized mice, the delayed protocol significantly prolonged graft survival after transplantation from BALB/c to naive B6 (median survival time [MST], >100 d). In contrast, the delayed protocol was unable to prevent graft rejection in sensitized mice (MST, 5 d). A significantly increased percentage of granzyme B+ CD8+ T cells was observed in the graft on day 3 posttransplantation in sensitized conditions. Further, the day 1 protocol significantly prolonged graft survival (MST, 18 d), even in sensitized conditions. Day 1 treatment significantly increased the percentage of Foxp3+CD25+CD4+ T cells and phenotypically changed CD8+ T cells in the graft (i.e., caused a significant increase in the proportion of Ly108+TCF1highPD-1+CD8+ T cells). In conclusion, different timings of delayed anti-CD3F(ab')2 treatment promoted allograft preservation in association with phenotypic changes in CD4+ and CD8+ T cells in the graft under sensitized conditions.
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TCF1highPD-1+Ly108+CD8+ T 细胞与非 Fc 受体结合型 CD3 抗体治疗致敏小鼠的移植物保存有关。
在啮齿类动物心脏移植模型中,非 Fc 结合型抗 CD3 Ab [anti-CD3F(ab')2] 可根据治疗窗口期诱导移植物接受。延迟方案可使淋巴细胞早期浸润移植物,而淋巴细胞的浸润可能会产生抑制作用。我们研究了在致敏条件下抗 CD3F(ab')2 的最有效方案,以确认临床应用的证据。用 BALB/c 尾部皮肤移植物致敏 C57BL/6 小鼠,并在致敏后 8-12 周移植 BALB/c 心脏移植物。在第 1-5 天(第 1 天方案)或第 3-7 天(延迟方案)连续 5 天每天注射 50 微克抗 CD3F(ab')2。在非致敏小鼠中,延迟方案显著延长了从 BALB/c 移植到天真 B6 的移植物存活时间(中位存活时间 [MST],>100 d)。相比之下,延迟方案无法防止致敏小鼠的移植物排斥反应(中位存活时间为 5 d)。在致敏条件下,移植后第 3 天,移植物中颗粒酶 B+ CD8+ T 细胞的比例明显增加。此外,即使在致敏条件下,第 1 天方案也能显著延长移植物存活时间(MST,18 d)。第 1 天治疗可明显增加移植物中 Foxp3+CD25+CD4+ T 细胞和表型改变的 CD8+ T 细胞的比例(即导致 Ly108+TCF1highPD-1+CD8+ T 细胞比例明显增加)。总之,在致敏条件下,不同时间的延迟抗CD3F(ab')2治疗可促进异体移植物的保存,并与移植物中CD4+和CD8+ T细胞的表型变化相关。
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3.70
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