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肝胆相照论坛 论坛 学术讨论& HBV English AASLD2018[418]CRV431,亲环蛋白抑制剂,减少 小鼠纤维 ...
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AASLD2018[418]CRV431,亲环蛋白抑制剂,减少 小鼠纤维化和肿瘤 [复制链接]

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发表于 2018-10-18 13:56 |只看该作者 |倒序浏览 |打印
418
CRV431, a Cyclophilin Inhibitor, Reduces
Fibrosis and Tumor Burden in Mice with
Hepatocellular Carcinoma
Joseph Kuo1, Michael Bobardt1, Udayan Chatterji1, Daniel
Trepanier2, Daren Ure2, Philippe Gallay1 and Robert Foster2,
(1)Immunology & Microbiology, The Scripps Research
Institute, (2)Contravir Pharmaceuticals Inc.
Background: An important objective in the treatment of
hepatitis B is the reduction of liver disease, including fibrosis,
cirrhosis, and hepatocellular carcinoma (HCC), arising from
chronic hepatitis B virus (HBV) infection. Previous studies
have shown that cyclophilin isomerases, in addition to their
beneficial role in protein folding, also paradoxically contribute
to a variety of injury and disease processes. The aim of
this study was to examine whether the cyclophilin inhibitor,
CRV431, in addition to its antiviral activities, also reduces
characteristics of liver disease in a mouse model. The nonalcoholic
steatohepatitis (NASH) mouse model was used to
assess liver-protective effects of CRV431, since this model
exhibits many pathogenic outcomes in similarity to chronic
HBV infection, including inflammation, fibrosis, and HCC.
Methods: Mice were administered streptozotocin, followed
by a high-fat diet for either 11 or 27 weeks, for assessment of
fibrosis and HCC development, respectively. CRV431 50 mg/
kg or vehicle control were administered orally each day for the
final 6 or 10 weeks of the two studies, respectively. In the HCC
study, CRV431 dosing was initiated once the presence of
nodules was confirmed. Livers were examined morphologically
and histologically for assessment of steatosis, inflammation,
fibrosis, and HCC tumor burden. HCC was scored according
to a developed system incorporating number and size of
nodules. Systemic cytokine levels in serum were detected by
multiplex assays. Results: CRV431 showed beneficial effects
by reducing liver fibrosis and HCC development. Liver fibrosis,
measured morphometrically following Sirius Red staining,
was reduced by 46% with CRV431 administration compared
with vehicle control (p=0.03). CRV431 reduced the number
of tumor nodules by 44% and reduced total tumor burden
by 52% compared to vehicle (p=0.02). Significantly, 25% of
CRV431-treated mice had no liver tumors at the end of the
study, whereas all vehicle-treated mice had at least 5 tumors
per liver. The reduction in tumor burden was associated with
reductions in body and liver weights. No effects of CRV431
were observed on steatosis, inflammation, systemic cytokine
levels, or blood glucose levels. Conclusion: CRV431
represents a well-tolerated and potent candidate treatment for
chronic HBV. The present study demonstrates that CRV431
may potentially benefit patients not only through its anti-HBV
activities but also by reducing development of fibrosis and
HCC.
Disclosures:
Robert Foster – ContraVir Pharmaceuticals Inc.: Employment
The following people have nothing to disclose: Joseph Kuo, Udayan Chatterji
Disclosure information not available at the time of publication: Michael Bobardt,
Daniel Trepanier, Daren Ure, Philippe Gallay

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发表于 2018-10-18 13:57 |只看该作者
418
CRV431,亲环蛋白抑制剂,减少
小鼠纤维化和肿瘤负荷
肝细胞癌
Joseph Kuo1,Michael Bobardt1,Udayan Chatterji1,Daniel
Trepanier2,Daren Ure2,Philippe Gallay1和Robert Foster2,
(1)免疫学和微生物学,斯克里普斯研究
研究所,(2)Contravir Pharmaceuticals Inc.
背景:治疗的重要目标
乙型肝炎是肝病的减少,包括纤维化,
肝硬化和肝细胞癌(HCC),由
慢性乙型肝炎病毒(HBV)感染。之前的学习
已经证明了亲环素异构酶,除了它们之外
蛋白质折叠中的有益作用,也是矛盾的贡献
对各种伤害和疾病过程。目标是
这项研究是为了检验亲环蛋白抑制剂,
除了抗病毒活性外,CRV431也减少了
小鼠模型中肝脏疾病的特征。非酒精的
使用脂肪性肝炎(NASH)小鼠模型
评估CRV431的肝脏保护作用,因为这个模型
表现出与慢性病相似的许多致病结果
HBV感染,包括炎症,纤维化和HCC。
方法:小鼠给予链脲佐菌素,随后
通过高脂肪饮食11或27周,评估
纤维化和HCC发展分别。 CRV431 50毫克/
每天口服给予kg或载体对照以用于治疗
两项研究的最后6或10周分别进行。在HCC
研究中,CRV431一旦存在就开始给药
结节得到确认。从形态上检查肝脏
和组织学上评估脂肪变性,炎症,
纤维化和HCC肿瘤负担。 HCC得分
一个包含数量和大小的开发系统
结节。检测血清中全身细胞因子水平
多重分析。结果:CRV431显示出有益效果
通过减少肝纤维化和HCC发展。肝纤维化,
天狼星红染色后形态测量,
与CRV431给药相比,减少了46%
车辆控制(p = 0.03)。 CRV431减少了数量
肿瘤结节减少44%,肿瘤总负荷减少
与载体相比为52%(p = 0.02)。显着,25%
CRV431治疗的小鼠在结束时没有肝脏肿瘤
研究,而所有载体处理的小鼠至少有5个肿瘤
每肝。肿瘤负荷的减少与
减少体重和肝脏重量。没有CRV431的影响
观察到脂肪变性,炎症,全身细胞因子
水平或血糖水平。结论:CRV431
代表了一种耐受性良好且有效的候选治疗方法
慢性HBV。本研究表明CRV431
不仅可以通过其抗HBV使患者受益
活动还要通过减少纤维化的发展和
HCC。
披露:
Robert Foster - ContraVir Pharmaceuticals Inc。:就业
以下人士没有透露任何内容:Joseph Kuo,Udayan Chatterji
披露信息在发布时不可用:Michael Bobardt,
Daniel Trepanier,Daren Ure,Philippe Gallay

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发表于 2018-10-18 15:11 |只看该作者
回复 StephenW 的帖子

CRV431还处于临床前,不过还是期待着
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