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Retired self-proteins as vaccine targets for primary immunoprevention of adult-onset cancers

机译:退役自身蛋白作为成人成年癌症一级免疫预防的疫苗靶标

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We propose that optimized control of adult-onset cancers requires the incorporation of a defense-based strategy in the form of preemptive immunity induced in healthy cancer-free subjects prior to the appearance of tumors. However, development of such prophylactic immunity has traditionally targeted etiopathogenic agents. We propose that in the absence of available cancer-inducing pathogens, safe and effective protection against the emergence of tumors may be achieved by inducing targeted immunity against tissue-specific self-proteins that are ' retired' from expression at immunogenic levels in normal tissues due to the normal aging process, but are expressed in emerging tumors. Thus, ' retired' self-proteins may substitute for unavailable pathogens as targets for developing prophylactic immunity against tumors we confront with age like breast, ovarian and prostate cancer. Our current efforts involve testing this primary ' immunoprevention' strategy in clinical trials focused on prevention of the more aggressive and lethal forms of breast cancer.
机译:我们建议对成年癌症的最佳控制要求在肿瘤出现之前以健康无癌受试者中诱导的先发性免疫的形式结合基于防御的策略。然而,这种预防性免疫的发展传统上具有靶向的致病性试剂。我们建议,在没有可用的诱发癌症的病原体的情况下,可以通过诱导针对组织特异性自身蛋白的靶向免疫来针对肿瘤的出现提供安全有效的保护,所述组织特异性自身蛋白由于正常组织中免疫原水平的表达而被“淘汰”到正常衰老过程,但在新兴肿瘤中表达。因此,“退休的”自身蛋白可能替代不可用的病原体,成为针对我们面对年龄(例如乳腺癌,卵巢癌和前列腺癌)的肿瘤进行预防性免疫的靶标。我们目前的工作包括在临床试验中测试这种主要的“免疫预防”策略,该策略的重点是预防更具侵略性和致命性的乳腺癌。

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