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雷帕霉素与静脉畸形的治疗。

Rapamycin and treatment of venous malformations.

机构信息

Institut Roi Albert II, Department of Medical Oncology.

Center for Vascular Anomalies, Division of Plastic Surgery.

出版信息

Curr Opin Hematol. 2019 May;26(3):185-192. doi: 10.1097/MOH.0000000000000498.

Abstract

PURPOSE OF REVIEW

The field of vascular anomalies has seen a fundamental change during the past 10 years. The identification of somatic genetic mutations as the explanation of sporadic vascular anomalies opened the doors to study prospectively and a posteriori the causes of various vascular malformations. This was helped by the rapidly evolving genetic techniques including the highly sensitive next generation sequencing. In parallel, knowledge on signaling alterations occurring in vascular endothelial cells because of the various mutations, development of in-vitro and especially the first in-vivo models, gave the possibility to test preclinically molecular therapies for vascular malformations.

RECENT FINDINGS

One of the first molecules, rapamycin, showed clear evidence of interrupting lesion growth. As its safety profile had been established in other conditions, it was quickly accepted for clinical trials on vascular anomalies. Now, with a few trials published and others ongoing, it is establishing itself as a gold standard for molecular therapy for recalcitrant lesions.

SUMMARY

Targeted molecular therapies are becoming interesting new additions to the management of vascular anomalies, and rapamycin is establishing itself as a gold standard for venous malformations.

摘要

目的综述

在过去的 10 年中,血管异常领域发生了根本性的变化。体细胞基因突变的鉴定为研究各种血管畸形的病因提供了线索,这使得前瞻性研究成为可能。这得益于包括高度敏感的下一代测序在内的快速发展的遗传技术。与此同时,由于各种突变导致血管内皮细胞中信号转导的改变,体外培养特别是体内模型的发展,为血管畸形的临床前分子治疗提供了可能。

最近的发现

最早的分子之一雷帕霉素(rapamycin),已经明确显示出中断病变生长的作用。由于其在其他疾病中的安全性已经得到证实,它很快被接受用于血管异常的临床试验。现在,随着一些试验的发表和其他试验的进行,它正在确立自己作为治疗难治性病变的分子治疗的金标准。

总结

靶向分子治疗正在成为血管异常治疗的新方法,雷帕霉素正在确立自己作为静脉畸形治疗的金标准。

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