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CD44:不同异构体的生理表达作为器官特异性转移形成的证据

CD44: physiological expression of distinct isoforms as evidence for organ-specific metastasis formation.

作者信息

Zöller M

机构信息

Department of Tumor Progression and Immune Defense, German Cancer Research Center, Heidelberg, Germany.

出版信息

J Mol Med (Berl). 1995 Sep;73(9):425-38. doi: 10.1007/BF00202261.

Abstract

Continuous progress has been achieved during recent decades in the therapy of metastasizing malignancies by improving chemotherapeutic strategies and new approaches in radiation therapy. Genetic manipulation of tumor cells and of the tumor fighting immune system is hoped to add significant contributions to curative interventions in disseminated tumors. That we are still far from eradicating death by malignant growth is due ultimately to our limited understanding of the cascade of events resulting in metastasis formation, which until recently was believed to rely on multiple rounds of mutation and selection processes. This implies an individually specific history of each metastatic tumor, which would rule out uniform diagnostic and therapeutic concepts. When it was noted in a rat tumor model that the transfer of cDNA of a single gene, a CD44 variant isoform (CD44v) covering the exons v4-v7, sufficed to initiate metastasis formation of a locally growing tumor, hope was created that a "metastogene" may have been identified. Although the idea of CD44v expression as a unifying concept for tumor progression was not sustained, the discovery of CD44v-initiated metastatic spread allowed a conceptually new hypothesis on tumor progression as a consequence of the reactivation of genetic programs of ontogeny, stem cell differentiation, and/or lymphocyte activation. Since distinct CD44 isoforms play an important role in these processes, unraveling the functions of this family of molecules can indeed provide a cornerstone in the understanding of tumor progression. This article summarizes briefly the present knowledge on known functions of CD44 isoforms with particular focus on parallels between physiological programs and tumor progression.

摘要

近几十年来,通过改进化疗策略和放射治疗的新方法,转移性恶性肿瘤的治疗取得了持续进展。人们希望对肿瘤细胞和抗肿瘤免疫系统进行基因操作,能为播散性肿瘤的治愈性干预做出重大贡献。我们仍远未消除恶性肿瘤导致的死亡,归根结底是因为我们对导致转移形成的一系列事件了解有限,直到最近,人们还认为转移依赖于多轮突变和选择过程。这意味着每个转移性肿瘤都有其独特的发展历程,这将排除统一的诊断和治疗理念。当在大鼠肿瘤模型中发现,单个基因的cDNA(一种覆盖外显子v4 - v7的CD44变异体同种型(CD44v))的转移足以引发局部生长肿瘤的转移形成时,人们产生了一种希望,即可能已经鉴定出一个“转移基因”。尽管将CD44v表达作为肿瘤进展的统一概念的想法并未得到证实,但CD44v引发的转移扩散的发现,使人们对肿瘤进展产生了一个概念上全新的假设,即肿瘤进展是个体发育、干细胞分化和/或淋巴细胞激活的基因程序重新激活的结果。由于不同的CD44同种型在这些过程中发挥着重要作用,阐明这一家族分子的功能确实可以为理解肿瘤进展提供一个基石。本文简要总结了目前关于CD44同种型已知功能的知识,特别关注生理程序与肿瘤进展之间的相似之处。

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