DNA, DNA

  • 文章类型: Journal Article
    各种心肌病的主要病因现在被认为是遗传的,在潜在分子原因的基础上创造一种新的靶向治疗模式。这篇综述为心肌病的传统临床分类提供了遗传和病因学背景,包括可能对现有或新兴治疗表现出不同反应的分子亚型。作者描述了几种新兴的心肌病治疗方法,包括基因疗法,直接靶向肌丝功能,蛋白质质量控制,新陈代谢,和其他人。作者讨论了这些方法的优缺点,并指出了短期和长期疗效的高潜力领域。
    The primary etiology of a diverse range of cardiomyopathies is now understood to be genetic, creating a new paradigm for targeting treatments on the basis of the underlying molecular cause. This review provides a genetic and etiologic context for the traditional clinical classifications of cardiomyopathy, including molecular subtypes that may exhibit differential responses to existing or emerging treatments. The authors describe several emerging cardiomyopathy treatments, including gene therapy, direct targeting of myofilament function, protein quality control, metabolism, and others. The authors discuss advantages and disadvantages of these approaches and indicate areas of high potential for short- and longer term efficacy.
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  • 文章类型: Journal Article
    溶瘤病毒是一类相对较新的抗癌免疫治疗剂。在过去的几十年中,几种病毒在临床试验中进行了评估,第一种药物即将被批准用作一种新的癌症治疗方式。在当前的审查中,概述了溶瘤病毒领域的近期(临床前)进展,这些进展以前或目前正在临床试验中进行评估。特别注意可能的安全问题,如毒性,环境脱落,突变和回复为野生型病毒。
    Oncolytic viruses are a relatively new class of anti-cancer immunotherapy agents. Several viruses have undergone evaluation in clinical trials in the last decades, and the first agent is about to be approved to be used as a novel cancer therapy modality. In the current review, an overview is presented on recent (pre)clinical developments in the field of oncolytic viruses that have previously been or currently are being evaluated in clinical trials. Special attention is given to possible safety issues like toxicity, environmental shedding, mutation and reversion to wildtype virus.
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  • 文章类型: Journal Article
    凋亡是肝脏疾病发病机制的主要特征。肝细胞凋亡受自噬活性调节。然而,中介它们相互作用的机制还有待确定。自噬的基础水平确保了旧的和受损的细胞器的生理更新。自噬也是压力条件下的适应性反应。自噬可以通过不同的串扰信号控制细胞命运。肝自噬和凋亡之间的复杂相互作用决定了临床前模型和临床试验所证明的肝细胞凋亡的程度和肝病的进展。本文就自噬在肝脏病理生理中的作用进行综述。自噬途径可以成为肝病治疗的新靶点。
    Apoptosis is a primary characteristic in the pathogenesis of liver disease. Hepatic apoptosis is regulated by autophagic activity. However, mechanisms mediating their interaction remain to be determined. Basal level of autophagy ensures the physiological turnover of old and damaged organelles. Autophagy also is an adaptive response under stressful conditions. Autophagy can control cell fate through different cross-talk signals. A complex interplay between hepatic autophagy and apoptosis determines the degree of hepatic apoptosis and the progression of liver disease as demonstrated by pre-clinical models and clinical trials. This review summarizes recent advances on roles of autophagy that plays in pathophysiology of liver. The autophagic pathway can be a novel therapeutic target for liver disease.
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