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种间重组细胞中超黑色素合成及形态变化的诱导及其被肿瘤启动子逆转的情况

Induction of supermelanin synthesis and morphological changes in interspecific reconstituted cells and its reversal by tumor promoter.

作者信息

Sekiguchi T, Tosu M, Yoshida M C, Oikawa A, Ishihara K, Fujiki H, Tumuraya M, Kameya T

出版信息

Somatic Cell Genet. 1982 Sep;8(5):605-22. doi: 10.1007/BF01542854.

Abstract

Chloramphenicol-resistant (CAPr) reconstituted cells and cybrids were isolated by fusion of karyoplasts (or intact cells) of mouse amelanotic melanoma B16 cells with cytoplasts of hypoxanthine-guanine phosphoribosyltransferase (HGPRT) -deficient, CAPr rat myoblastic cells, L6TG.CAPr, and double selection in HAT medium containing CAP. Reconstituted cells or cybrids exhibited unique cellular arrangement, and about one third of the isolated clones expressed high tyrosinase activity and marked melanin synthesis, although the parental mouse cells expressed low tyrosinase activity and the parental rat cells did not express tyrosinase activity. These phenotypic changes have been stable for more than a year. The phenotypic reversions of these clonal cells were induced by treatment with a tumor promoter. There were changes in the morphology of the treated cells to that of the mouse B16 cells and extinction of tyrosinase activity and melanin synthesis in pigmented clonal cells. These phenotypic changes and reversions induced by a promoter were repeatedly reversible.

摘要

通过将小鼠无黑色素黑色素瘤B16细胞的核质体(或完整细胞)与次黄嘌呤 - 鸟嘌呤磷酸核糖转移酶(HGPRT)缺陷的耐氯霉素(CAPr)大鼠成肌细胞L6TG.CAPr的细胞质体融合,并在含有氯霉素的HAT培养基中进行双重选择,分离出耐氯霉素(CAPr)的重构细胞和胞质杂种。重构细胞或胞质杂种呈现出独特的细胞排列方式,尽管亲代小鼠细胞酪氨酸酶活性低,亲代大鼠细胞不表达酪氨酸酶活性,但约三分之一的分离克隆表达了高酪氨酸酶活性并显著合成黑色素。这些表型变化已经稳定超过一年。这些克隆细胞的表型逆转是由肿瘤启动子处理诱导的。处理后的细胞形态发生变化,变为小鼠B16细胞的形态,色素沉着克隆细胞中的酪氨酸酶活性和黑色素合成消失。启动子诱导的这些表型变化和逆转可反复逆转。

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