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小鼠中的移植物抗宿主反应。IV. 胸腺细胞对抗体形成的抑制作用。

Graft-versus-host reactions in mice. IV. Thymus cell suppression of antibody formation.

作者信息

Bennett M, Sturgeon M, Engler J P

出版信息

Am J Pathol. 1973 Apr;71(1):135-50.

Abstract

The ability of transplanted marrow-thymus cell mixtures to generate antibody-forming cells in irradiated syngeneic or F(1) hybrid mice when immunized with sheep erythrocytes 18 hours later was determined. Much fewer anti-sheep plaque-forming cells (PFC) were detected in spleens of F(1) hybrid mice. Adrenalectomy, use of infant recipient mice, or preimmunization of donors or hosts did not prevent the suppression; the grafting of irradiated donor-type spleen cells (source of "accessory" cells) produced only an additive effect. Parental marrow and thymus cells were able to generate new precursors of PFC and specific inducer cells, respectively, in spleens of F(1) hybrid mice, as detected by two-step experiments utilizing parent-strain secondary recipient mice. The suppression depended upon transferring parental strain thymus cells into F(1) hybrid mice and was seen irrespective of the marrow donor strain. When irradiated mice were immunized twice (on the day of transplantation and 4 days later), there was only marginal suppression of antibody production when marrow cells only or marrow plus thymus cells were transplanted. Thus, it appears that an excess of thymus-derived "suppressor" cells is generated upon exposure to alloantigens and inhibit terminal differentiation of antibody-forming cells in a noncytotoxic manner. Mature PFC themselves were not the targets of suppression. The method of immunization probably determines the relative functional capacity of thymus-derived "helper" and suppressor cells.

摘要

测定了移植的骨髓 - 胸腺细胞混合物在18小时后用绵羊红细胞免疫照射后的同基因或F(1)杂交小鼠中产生抗体形成细胞的能力。在F(1)杂交小鼠的脾脏中检测到的抗绵羊空斑形成细胞(PFC)要少得多。肾上腺切除术、使用幼龄受体小鼠或供体或宿主的预先免疫并不能阻止这种抑制作用;照射后的供体型脾细胞(“辅助”细胞来源)的移植仅产生相加效应。通过利用亲本品系二级受体小鼠的两步实验检测到,亲代骨髓和胸腺细胞能够分别在F(1)杂交小鼠的脾脏中产生新的PFC前体和特异性诱导细胞。这种抑制作用取决于将亲本品系胸腺细胞转移到F(1)杂交小鼠中,并且与骨髓供体品系无关。当照射后的小鼠在移植当天和4天后进行两次免疫时,仅移植骨髓细胞或骨髓加胸腺细胞时,抗体产生仅有轻微抑制。因此,似乎在接触同种异体抗原后会产生过量的胸腺来源的“抑制”细胞,并以非细胞毒性方式抑制抗体形成细胞的终末分化。成熟的PFC本身不是抑制的靶点。免疫方法可能决定胸腺来源的“辅助”和抑制细胞的相对功能能力。

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