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化疗诱导的骨骼肌分子变化。

Chemotherapy-Induced Molecular Changes in Skeletal Muscle.

作者信息

Pedrosa Mafalda Barbosa, Barbosa Samuel, Vitorino Rui, Ferreira Rita, Moreira-Gonçalves Daniel, Santos Lúcio Lara

机构信息

Associated Laboratory for Green Chemistry of the Network of Chemistry and Technology (LAQV-REQUIMTE), Department of Chemistry, University of Aveiro, 3810-193 Aveiro, Portugal.

Research Centre in Physical Activity, Health and Leisure (CIAFEL), Faculty of Sport, University of Porto, 4200-450 Porto, Portugal.

出版信息

Biomedicines. 2023 Mar 15;11(3):905. doi: 10.3390/biomedicines11030905.

Abstract

Paraneoplastic conditions such as cancer cachexia are often exacerbated by chemotherapy, which affects the patient's quality of life as well as the response to therapy. The aim of this narrative review was to overview the body-composition-related changes and molecular effects of different chemotherapy agents used in cancer treatment on skeletal-muscle remodeling. A literature search was performed using the Web of Science, Scopus, and Science Direct databases and a total of 77 papers was retrieved. In general, the literature survey showed that the molecular changes induced by chemotherapy in skeletal muscle have been studied mainly in animal models and mostly in non-tumor-bearing rodents, whereas clinical studies have essentially assessed changes in body composition by computerized tomography. Data from preclinical studies showed that chemotherapy modulates several molecular pathways in skeletal muscle, including the ubiquitin-proteasome pathway, autophagy, IGF-1/PI3K/Akt/mTOR, IL-6/JAK/STAT, and NF-κB pathway; however, the newest chemotherapy agents are underexplored. In conclusion, chemotherapy exacerbates skeletal-muscle wasting in cancer patients; however, the incomplete characterization of the chemotherapy-related molecular effects on skeletal muscle makes the development of new preventive anti-wasting strategies difficult. Therefore, further investigation on molecular mechanisms and clinical studies are necessary.

摘要

诸如癌症恶病质等副肿瘤性病症常常会因化疗而加剧,这会影响患者的生活质量以及对治疗的反应。本叙述性综述的目的是概述癌症治疗中使用的不同化疗药物对骨骼肌重塑的与身体组成相关的变化及分子效应。使用科学网、Scopus和科学Direct数据库进行了文献检索,共检索到77篇论文。总体而言,文献调查表明,化疗在骨骼肌中诱导的分子变化主要在动物模型中进行了研究,且大多是在无肿瘤的啮齿动物中,而临床研究主要通过计算机断层扫描评估身体组成的变化。临床前研究的数据表明,化疗可调节骨骼肌中的多种分子途径,包括泛素-蛋白酶体途径、自噬、IGF-1/PI3K/Akt/mTOR、IL-6/JAK/STAT和NF-κB途径;然而,最新的化疗药物尚未得到充分研究。总之,化疗会加剧癌症患者的骨骼肌消耗;然而,化疗对骨骼肌相关分子效应的不完全表征使得开发新的预防性抗消耗策略变得困难。因此,有必要对分子机制进行进一步研究并开展临床研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e161/10045751/fe7887b8cfa8/biomedicines-11-00905-g001.jpg

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