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通过mRNA表达谱鉴定为肿瘤排斥表位的肿瘤相关抗原。

Tumor-associated antigens identified by mRNA expression profiling as tumor rejection epitopes.

作者信息

Andersen Marie Louise, Ruhwald Morten, Thorn Mette, Pedersen Anders Elm, Mathiassen Susanne, Buus Soren, Claesson Mogens H

机构信息

Department of Medical Anatomy, University of Copenhagen, Copenhagen, Denmark.

出版信息

J Immune Based Ther Vaccines. 2003 Jan 29;1(1):1. doi: 10.1186/1476-8518-1-1.

Abstract

Thirteen H-2b-binding peptides derived from six potentially overexpressed proteins in p53-/- thymoma (SM7) cells were studied for immunogenecity and vaccine-induced prevention of tumor growth in mice inoculated with SM7 tumor cells. Six of the peptides generated specific CTL responses after immunization, but only two of these peptides (RAD23-31 and RAD24-31) were capable of generating a weak vaccination-induced protection against adoptive tumor growth. SM7 inoculated mice treated with a blocking antibody against the inhibitory T cell signal transducing molecule CTLA4 appeared to delay tumor take, suggesting that SM7 thymoma cells are recognized by the adaptive immune system of the host. However, prophylactic vaccination with RAD23-31 and RAD24-31 peptides combined with anti-CTLA4 Ab treatment and did not improve tumor resistance. Our data would indicate that vaccination with immunogenic peptides derived from potentially overexpressed tumor proteins, as identified by mRNA expression profiling of p53-/- thymoma cells, at best results in a weak tumor protection thus questioning this way of detection of new tumor rejection epitopes.

摘要

研究了从p53基因敲除的胸腺瘤(SM7)细胞中6种可能过表达的蛋白衍生而来的13种H-2b结合肽的免疫原性,以及在接种SM7肿瘤细胞的小鼠中疫苗诱导预防肿瘤生长的情况。其中6种肽在免疫后产生了特异性CTL反应,但只有两种肽(RAD23-31和RAD24-31)能够产生较弱的疫苗诱导的针对过继性肿瘤生长的保护作用。用针对抑制性T细胞信号转导分子CTLA4的阻断抗体处理接种了SM7的小鼠,似乎能延迟肿瘤形成,这表明SM7胸腺瘤细胞能被宿主的适应性免疫系统识别。然而,用RAD23-31和RAD24-31肽进行预防性疫苗接种并联合抗CTLA4抗体治疗,并没有提高肿瘤抗性。我们的数据表明,用p53基因敲除的胸腺瘤细胞mRNA表达谱鉴定出的可能过表达的肿瘤蛋白衍生的免疫原性肽进行疫苗接种,充其量只能产生较弱的肿瘤保护作用,因此对这种检测新的肿瘤排斥表位的方法提出了质疑。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ecc9/153425/219aa242fea5/1476-8518-1-1-1.jpg

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