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胸腺上皮细胞控制胸腺细胞白血病前期表型和致白血病逆转录病毒的表达。

Thymic epithelium controls thymocyte expression of preleukemic phenotype and leukemogenic retroviruses.

作者信息

Tempelis L D

出版信息

J Immunol. 1987 May 15;138(10):3555-65.

PMID:3033077
Abstract

Congenitally athymic AKR-streaker (nustr/nustr) mice were grafted separately with syngeneic or allogeneic, irradiated (1200 R) thymic reticuloepithelial (TRE) elements (stroma) or nonirradiated whole thymus grafts (control group) from N-tropic murine leukemia virus (MuLV) infection-susceptible (Fv-1n/n) or N-tropic-MuLV-infection-resistant (Fv-1b/n) murine strains. From 3 to 13 mo after grafting, the mononuclear cells repopulating the thymus grafts were stained with fluorescent monoclonal antibodies to thymocyte differentiation antigens, peanut agglutinin, and an antibody to MuLV antigens and were then analyzed by flow cytometry. Irradiated TRE of the Fv-1n/n genotype, whether from high or low leukemia-incidence strains, contained lymphoid cells of host (nustr/nustr) origin with alterations in thymocyte differentiation and MuLV antigen expression consistent with preleukemic changes. In contrast, transplanted TRE of the low leukemia-incidence Fv-1b/n genotype restricted preleukemic changes in thymocyte differentiation and MuLV antigen expression by lymphoid cells derived from the nustr/nustr host. Thus, nustr/nustr lymphocytes must infect susceptible TRE (Fv-1n/n) with N-tropic-MuLV before preleukemic changes occur in the mustr/nustr lymphocytes that later migrate to the thymus. Therefore, it was the radiation-resistant cells in the thymus that amplified or suppressed expression of AKR MCF retroviruses and the preleukemic phenotype, not the thymic lymphocytes. Thy-1.1+ splenocytes of ungrafted nustr/nustr mice were comparable in percentage to nustr/+ but were deficient in the Lyt-1+2- subpopulation and unresponsive to mitogens or alloantigens in vitro. Analysis of splenocyte cell surface markers, mitogen, MLC, and CML responses of Fv-1n/n-thymus-grafted nustr/nustr mice showed restoration of Lyt-1+2- cells to levels comparable to nustr/+ and reconstitution of in vitro proliferative and cytotoxic responses.

摘要

将先天性无胸腺的AKR条纹鼠(nustr/nustr)分别移植同基因或异基因、经照射(1200拉德)的胸腺网状上皮(TRE)成分(基质),或来自对N-嗜性鼠白血病病毒(MuLV)感染敏感(Fv-1n/n)或对N-嗜性MuLV感染有抗性(Fv-1b/n)鼠品系的未照射全胸腺移植物(对照组)。移植后3至13个月,用针对胸腺细胞分化抗原、花生凝集素和MuLV抗原的荧光单克隆抗体对重新填充胸腺移植物的单核细胞进行染色,然后通过流式细胞术进行分析。Fv-1n/n基因型的经照射TRE,无论来自高白血病发病率还是低白血病发病率的品系,都含有宿主(nustr/nustr)来源的淋巴细胞,其胸腺细胞分化和MuLV抗原表达发生改变,与白血病前期变化一致。相比之下,但低白血病发病率的Fv-1b/n基因型的移植TRE限制了来自nustr/nustr宿主的淋巴细胞在胸腺细胞分化和MuLV抗原表达方面的白血病前期变化。因此,nustr/nustr淋巴细胞必须在后来迁移到胸腺的mustr/nustr淋巴细胞发生白血病前期变化之前,用N-嗜性MuLV感染易感的TRE(Fv-1n/n)。因此,是胸腺中的抗辐射细胞放大或抑制了AKR MCF逆转录病毒的表达和白血病前期表型,而不是胸腺淋巴细胞。未移植的nustr/nustr小鼠的Thy-1.1 +脾细胞在百分比上与nustr/+相当,但Lyt-1 + 2-亚群缺乏,并且在体外对丝裂原或同种异体抗原无反应。对Fv-1n/n胸腺移植的nustr/nustr小鼠的脾细胞表面标志物、丝裂原、混合淋巴细胞培养(MLC)和细胞介导的淋巴细胞毒反应(CML)的分析表明,Lyt-1 + 2-细胞恢复到与nustr/+相当的水平,并重建了体外增殖和细胞毒性反应。

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