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New pharmacological strategies against metastatic spread.

机译:对抗转移扩散的新药理策略。

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Although metastatic spread is the most frequent cause of death in cancer patients, there are very few drugs specifically targeting this process. Bases for a new antimetastatic drug discovery strategy are weak because a great number of unknowns characterize the complete understanding of the metastatic cascade mechanisms. Moreover, the current experimental models are too simplistic and do not account for the complexity of the phenomenon. Some targets have been identified but too few are validated. Among them, the metastasis suppressor genes seem to be the most promising. In spite of this, during recent years, a dozen of molecules, which fulfil the definition of a specific metastatic drug that inhibits the metastases without altering the growth of the primary tumour (which can be eradicated by surgery), have been identified and assessed for the proof of the concept. The continuation of this effort would benefit in terms of efficiency, if the objectives were defined more precisely. It is particularly important to distinguish molecules that prevent spread of the metastatic cells of the early-stage primary tumour from the ones which induce a regression of the established metastases or to inhibit the transition from disseminated occult tumour cells to dormant micrometastasis. This second goal is a priori more relevant in the current clinical setting where the detection of early metastatic spread is very difficult, and therefore would call for greater effort on the part of the scientific community.
机译:尽管转移扩散是癌症患者最常见的死亡原因,但针对这种过程的药物很少。一种新的抗转移药物发现策略的基础薄弱,因为大量的未知数表征了对转移级联机制的完全理解。此外,当前的实验模型过于简单,无法说明现象的复杂性。已经确定了一些目标,但验证的目标太少。其中,转移抑制基因似乎是最有前途的。尽管如此,近年来,已经鉴定并评估了十几种分子,这些分子符合特定转移药物的定义,该药物在不改变原发性肿瘤生长的情况下可抑制转移而可通过手术根除。概念的证明。如果目标得到更精确的定义,那么继续努力将在效率方面受益。将阻止早期原发性肿瘤转移细胞扩散的分子与诱导已确定的转移灶消退的分子或抑制从弥散性隐匿性肿瘤细胞向休眠的微转移的过渡相区分的分子尤其重要。在当前临床环境中,这第二个目标是先验的,在当前环境中,早期转移扩散的检测非常困难,因此需要科学界作出更大的努力。

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