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小鼠白血病细胞和胸腺细胞上胸腺白血病抗原体内调节的血清需求

Serum requirements for in vivo modulation of thymus-leukemia antigens on mouse leukemia cells and thymocytes.

作者信息

Stackpole C W

出版信息

J Natl Cancer Inst. 1979 Jun;62(6):1529-36.

PMID:312352
Abstract

Mouse leukemia cells and normal thymocytes bearing thymus-leukemia (TL) cell surface antigens were previously shown to acquire resistance to lysis by guinea pig complement (C) during incubation with TL alloantiserum in vitro at 37 degrees C due to heat-labile serum activity resulting in deposition of mouse C3 onto the cell surface. The role of heat-labile serum activity and C3 in modulation of TL+ cells in vivo in mice actively or passively immunized against TL antigens was investigated. Mice of the TL-/TL+ C57BL/6J (B6) strain and the B6 congenic strain B6-Tiaa possessed poorly modulating sera, and the radiation-induced A-strain leukemia RADA1 transplanted into B6 mice passively immunized with heated (56 degrees C) TL antiserum failed to modulate; thymocytes of B6-Tiaa mice immunized similarly also did not modulate. A specific requirement for mouse C3 deposition onto RADA1 cells to achieve a modulated state was demonstrated in actively immunized TL- (B6 X A-Tiab)F1 mice in which circulating C3 and modulating activity were depleted by administration of cobra venom factor. In immunized (B6 X A-Tiab)F1 mice bearing RADA1 transplants and repeatedly given injections of B6 serum, tumor cells escaped immune destruction despite a lack of modulation. Thus modulation of TL antigenicity on tumor cells in vivo, but not tumor escape, required cell-bound C3.

摘要

先前已表明,携带胸腺白血病(TL)细胞表面抗原的小鼠白血病细胞和正常胸腺细胞,在37℃体外与TL同种异体抗血清孵育期间,由于热不稳定血清活性导致小鼠C3沉积在细胞表面,从而获得对豚鼠补体(C)裂解的抗性。研究了热不稳定血清活性和C3在主动或被动免疫TL抗原的小鼠体内对TL+细胞调节中的作用。TL-/TL+C57BL/6J(B6)品系和B6同源品系B6-Tiaa的小鼠血清调节能力较差,移植到用加热(56℃)TL抗血清被动免疫的B6小鼠体内的辐射诱导A品系白血病RADA1未能被调节;同样免疫的B6-Tiaa小鼠的胸腺细胞也未被调节。在主动免疫的TL-(B6×A-Tiab)F1小鼠中证实了小鼠C3沉积到RADA1细胞上以达到调节状态的特定要求,在这些小鼠中,通过给予眼镜蛇毒因子消耗了循环C3和调节活性。在携带RADA1移植瘤并反复注射B6血清的免疫(B6×A-Tiab)F1小鼠中,尽管缺乏调节,肿瘤细胞仍逃脱了免疫破坏。因此,体内肿瘤细胞上TL抗原性的调节而非肿瘤逃脱需要细胞结合的C3。

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