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同一健康:针对人类和犬类组织细胞肉瘤及树突状细胞肉瘤中基因变异的疗法

One Health: Therapies Targeting Genetic Variants in Human and Canine Histiocytic and Dendritic Cell Sarcomas.

作者信息

Erich Suzanne Agnes, Teske Erik

机构信息

Department of Clinical Sciences of Companion Animals, Faculty of Veterinary Medicine, Utrecht University, Utrecht, The Netherlands.

出版信息

Vet Comp Oncol. 2024 Sep;22(3):322-339. doi: 10.1111/vco.12988. Epub 2024 Jun 12.

DOI:10.1111/vco.12988
PMID:38867335
Abstract

The precise cause of HS/DCS is still unknown. The relatively low incidence in humans urges for an animal model with a high incidence to accelerate knowledge about genetics and optimal treatment of HS/DCS. Namely, until now, the therapies targeting genetic variants are still more experimental and sparsely used, while consensus is missing. In addition, the literature about variants and possible mutation-targeted therapies in humans and dogs consists mainly of case reports scattered throughout the literature. Therefore, an overview is provided of all currently known genetic variants in humans and dogs with HS/DCS and its subtypes, their possible mutation-targeted therapies, their efficacy, and a contemplation about the future. Several genetic variants have already been discovered in HS/DCS, of which many are shared between canine and human HS/DCS, but unique variants exist as well. Unfortunately, none of these already found variants seem to be specifically causal for HS/DCS, and the puzzle of its landscape of genetic variation is far from complete. The use of mutation-targeted therapies, including MAPK-/MEK-inhibitors and the future use of PTPN11-, CDK4/6- and PD-1-inhibitors, seems to be promising for these specific variants, but clearly, clinical trials are needed to determine optimal inhibitors and standardised protocols for all variants. It can be concluded that molecular analysis for variants and subsequent mutation-targeted therapy are an essential addition to cancer diagnostics and therapy. A joint effort of humans and dogs in research is urgently needed and will undoubtedly increase knowledge and survival of this devastating disease in dogs and humans.

摘要

化脓性汗腺炎/顶泌汗腺炎(HS/DCS)的确切病因仍然未知。人类中相对较低的发病率促使人们建立一种高发病率的动物模型,以加速对HS/DCS遗传学和最佳治疗方法的了解。也就是说,到目前为止,针对基因变异的疗法仍更多处于实验阶段且使用较少,同时也缺乏共识。此外,关于人类和犬类中基因变异以及可能的针对突变的疗法的文献主要由分散在各处的病例报告组成。因此,本文提供了关于人类和患有HS/DCS及其亚型的犬类中所有目前已知的基因变异、其可能的针对突变的疗法、疗效以及对未来的思考的概述。在HS/DCS中已经发现了几种基因变异,其中许多在犬类和人类HS/DCS中是共有的,但也存在独特的变异。不幸的是,这些已发现的变异似乎都不是HS/DCS的特异性病因,其基因变异情况的谜题远未完整。使用针对突变的疗法,包括丝裂原活化蛋白激酶/MEK抑制剂以及未来使用蛋白酪氨酸磷酸酶非受体型11(PTPN11)、细胞周期蛋白依赖性激酶4/6(CDK4/6)和程序性死亡受体1(PD-1)抑制剂,对于这些特定变异似乎很有前景,但显然需要进行临床试验来确定所有变异的最佳抑制剂和标准化方案。可以得出结论,对变异进行分子分析以及随后的针对突变的疗法是癌症诊断和治疗的重要补充。迫切需要人类和犬类在研究中的共同努力,这无疑将增加对这种毁灭性疾病在犬类和人类中的了解并提高生存率。

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