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Radiation-Induced Liver Toxicity

机译:辐射诱导的肝脏毒性

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The advent of highly conformal radiation therapy (RT) has defined a new role for RT in the treatment of both primary and metastatic liver cancer. Despite major advances in how RT is delivered, radiation-induced liver disease (RILD) remains a concern. Classic RILD, characterized by anicteric ascites and hepatomegaly, is unlikely to occur if treating to doses of <= 30 Gy in 2 Gy per fraction in patients with baseline Child-Pugh A liver function. On the other hand, nonclassic RILD is a spectrum of liver toxicity, including a general decline in liver function and elevation of liver enzymes. It is less well defined and less predictable, especially in patients with underlying liver disease. Scoring and quantifying RILD remains a challenge. The Child-Pugh score has been the most consistently used parameter. Other scoring systems such as the albumin-bilirubin score provide further discrimination in patients with hepatocellular carcinoma, although their value in patients treated with RT remains to be established. Many serum and imaging biomarkers of liver function are currently being investigated, and they will provide further useful information in the future for local and global liver function assessment, for planning optimization, and for treatment adaptation. To date, no pharmacological therapies have provided consistent results in mitigating RILD once it has manifested clinically. Numerous promising treatment strategies including TGF beta inhibition, Hedgehog inhibition, CXCR4 inhibition, hepatocyte transplantation, and bone marrow-derived stromal cell therapy, have potential to be helpful in the treatment of RILD in the future. (C) 2017 Elsevier Inc. All rights reserved.
机译:高度保形放射治疗(RT)的出现在治疗原发性和转移性肝癌中,对RT确定了新作用。尽管rt是如何交付Rt的主要进步,但辐射诱导的肝病(RILD)仍然是一个问题。经典RIRD,其特征在于基线儿童-PUGH A肝功能的患者每分数在每小材2 GY中对2 GY的剂量<= 30GY的剂量,不太可能发生。另一方面,非计算力是一种肝脏毒性的光谱,包括肝功能的一般性下降和肝酶的升高。它缺乏定义且更少可预测,特别是肝脏疾病的患者。评分和量化RILD仍然是一项挑战。 Child-Pugh评分是最常用的使用参数。诸如白蛋白 - 胆红素评分的其他评分系统提供了肝细胞癌患者的进一步辨别,尽管它们在用室温的患者中的价值仍有待建立。目前正在调查许多血清和成像生物标志物,并将在未来为当地和全球肝功能评估提供进一步的有用信息,用于规划优化,以及治疗适应。迄今为止,一旦临床表现,就没有药理学疗法提供了一致的降低的结果。许多有前途的治疗策略,包括TGFβ抑制,刺猬抑制,CXCR4抑制,肝细胞移植和骨髓衍生的基质细胞疗法,有助于在未来治疗RILD。 (c)2017年Elsevier Inc.保留所有权利。

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