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肿瘤免疫学回顾

[A retrospective view of tumor immunology].

作者信息

Dosne Pasqualini C

机构信息

Instituto de Investigaciones Hematológicas, Academia Nacional de Medicina, Buenos Aires, Argentina.

出版信息

Medicina (B Aires). 1996;56 Suppl 1:3-12.

PMID:9224970
Abstract

The story of tumor immunology includes periods of hope followed by ones of disenchantment as far as clinical applications are concerned. In antiquity, cancer was considered "contrary to Nature", a concept which was confirmed by Ehrlich at the beginning of our century when the layed down the foundations of immunology. The latter was defined as the defence against all "non-self" intruders, including cancer, as opposed to the protection of "self". This concept was further accentuated by the theory immune surveillance proposed by Burnet in 1969 which implicated a destruction of nascent neoplastic cells by T lymphocytes. To increase host defence was the basis of tumor immunotherapy with BCG, levamisol and other adjuvants. The appearance of the nude mouse, athymic, and yet free of spontaneous tumors, led to a new paradigm, the network theory proposed by Jerne. This was based on immunological homeostasis implicating that both "self" and "non-self" can be rejected and tolerated. Cancer gradually ceased to be considered as "contrary to Nature". As for the proposed viral etiology of cancer which was the basis of the National Cancer Act signed by Nixon in 1971, this led to various breakthroughs and Nobel Prizes (Table 1), to discoveries such as reverse transcriptase, cellular oncogenes, tumor suppressor genes, which gave a new explanation for neoplastic transformation. The latter can now be considered as the consequence of a cascade of molecular events which include oncogene expression, anti-oncogene deletion, etc... converting, step by step, for instance, a polyp into a colon cancer and its metastases. The availability of monoclonal antibodies capable of attacking tumor cells did not lead to the expected success because of the complexity of the immune system. Attempts at a better understanding of the latter have led to a subdivision of the T lymphocyte CD4 population into Th1 and Th2. Th1 favor rejection (tumoral, fetal or of transplants) through the elaboration of IL-2, IFN and TNF while Th2 led to tolerance or acceptation through the production of IL-4, IL-5 and IL-10: both functions neutralize each other establishing a "normal" equilibrium Th1 vs Th2. This could explain the state of "tumor dormancy" or tumors in situ which are apparently quite frequent. That any immunological stimulation would cause these dormant tumors to proliferate is the basis of the immunostimulation theory proposed by Prehn and supported by the clinical observations of Stewart. This new concept has led some authors to propose that instead of destroying the tumor cells an attempt be made to maintain them in a state of dormancy in congenial company with normal cells.

摘要

就临床应用而言,肿瘤免疫学的发展历程可谓是充满希望,而后又陷入失望。在古代,癌症被认为是“违背自然规律的”,这一概念在本世纪初被埃利希所证实,当时他奠定了免疫学的基础。免疫学最初被定义为对所有“非自身”入侵者的防御,其中包括癌症,与对“自身”的保护相对。1969年伯内特提出的免疫监视理论进一步强化了这一概念,该理论认为新生的肿瘤细胞会被T淋巴细胞破坏。增强宿主防御能力是使用卡介苗、左旋咪唑和其他佐剂进行肿瘤免疫治疗的基础。裸鼠(无胸腺且无自发肿瘤)的出现引发了一种新的范式,即杰尔内提出的网络理论。该理论基于免疫稳态,意味着“自身”和“非自身”都可能被排斥或耐受。癌症逐渐不再被视为“违背自然规律的”。至于1971年尼克松签署的《国家癌症法案》所基于的癌症病毒病因假说,它带来了各种突破并催生了多项诺贝尔奖(表1),还促成了逆转录酶、细胞癌基因、肿瘤抑制基因等的发现,这些发现为肿瘤转化提供了新的解释。肿瘤转化现在可被视为一系列分子事件的结果,这些事件包括癌基因表达、抗癌基因缺失等,例如,一步步地将息肉转变为结肠癌及其转移灶。能够攻击肿瘤细胞的单克隆抗体的出现并未带来预期的成功,原因在于免疫系统的复杂性。为了更好地理解免疫系统,人们将T淋巴细胞CD4群体细分为Th1和Th2。Th1通过分泌白细胞介素 - 2、干扰素和肿瘤坏死因子促进排斥反应(针对肿瘤、胎儿或移植组织),而Th2则通过产生白细胞介素 - 4、白细胞介素 - 5和白细胞介素 - 10导致耐受或接受:这两种功能相互抵消,建立了Th1与Th2之间的“正常”平衡。这可以解释“肿瘤休眠”状态或原位肿瘤的情况,而原位肿瘤显然相当常见。任何免疫刺激都会导致这些休眠肿瘤增殖,这是普雷恩提出的免疫刺激理论的基础,并得到了斯图尔特临床观察结果的支持。这一新概念使得一些作者提议,与其破坏肿瘤细胞,不如尝试使它们与正常细胞和谐共处,保持在休眠状态。

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