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Phosphatidyl choline is recognized by a series of Ly-1+ murine B cell lymphomas specific for erythrocyte membranes

机译:磷脂酰胆碱可被一系列对红细胞膜特异的Ly-1 +鼠B细胞淋巴瘤识别

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摘要

Cells from 6 of 14 different Ly-1+ murine B cell lymphomas bound to synthetic liposomes encapsulating fluorescein. The liposomes were made from distearoyl phosphatidyl choline (DSPC), distearoyl phosphatidyl glycerol (DSPG), and cholesterol. In all cases, liposome binding was due to recognition of phosphatidyl choline by the surface IgM on the tumor cells. Liposome binding could be inhibited by DSPC but not by DSPG, and the number of liposomes bound per cell was directly related to the cell surface concentration of IgM. The IgM secreted by a hybridoma derived from one of the lymphomas, CH12, was shown to agglutinate liposomes, and was used in a solid-phase immunoassay to study inhibition of liposome binding by pure phospholipids; DSPC and sphingomyelin both inhibited, whereas DSPG did not. The Ig borne by the six lymphomas that bind phosphatidylcholine also bind to both SRBC and bromelain-treated mouse erythrocytes. The idiotypic of CH12 IgM is similar to that expressed by Ly-1+ normal splenic B cells of the same specificity. The significance of these data in relation to other commonly studied autoantigens, and to the restricted specificity of normal Ly-1+ B cells is discussed.
机译:14种不同的Ly-1 +鼠B细胞淋巴瘤中有6种的细胞与包裹荧光素的合成脂质体结合。脂质体由二硬脂酰磷脂酰胆碱(DSPC),二硬脂酰磷脂酰甘油(DSPG)和胆固醇制成。在所有情况下,脂质体结合都是由于肿瘤细胞表面IgM对磷脂酰胆碱的识别。脂质体结合可以被DSPC抑制,但不能被DSPG抑制,每个细胞结合的脂质体数量与细胞表面IgM浓度直接相关。由一种淋巴瘤CH12衍生的杂交瘤分泌的IgM被证明可凝集脂质体,并用于固相免疫测定中以研究纯磷脂对脂质体结合的抑制作用。 DSPC和鞘磷脂都抑制,而DSPG则不。六种结合磷脂酰胆碱的淋巴瘤携带的Ig也与SRBC和经菠萝蛋白酶处理的小鼠红细胞结合。 CH12 IgM的独特型与相同特异性的Ly-1 +正常脾脏B细胞表达的相似。讨论了这些数据与其他通常研究的自身抗原以及正常Ly-1 + B细胞的限制性特异性相关的意义。

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