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灰色区域 - ALT
蓝线 - 乙肝表面抗原
X axis - 日
the data demonstrate that intravenous administration of two doses (2 mg/kg, 3 mg/kg) of ARC-520 in a chimpanzee chronically infected with HBV, resulted in substantial and sustained reductions in HBV DNA, HBeAg, and HBsAg, which did not return to baseline until study day 43, 43, and 71 respectively. In addition, an increase in serum alanine transaminase (ALT) occurred 4 weeks after the last dose, coincident with the nadir of circulating HBsAg. This is suggestive of a therapeutic immunological flare, which is thought to be part of a cascade that under chronic therapy may lead to HBsAg seroconversion and functional cure. Robert E. Lanford, Ph.D., of the Texas Biomedical Research Institute where the study was conducted, presented these data and the poster was selected as a Presidential Poster of Distinction indicating that it was in the top 10% of all abstracts selected for poster presentation.
“This study would have been important if ARC-520 just demonstrated safe and effective HBsAg reduction because this is thought to be a necessary step in achieving a functional cure,” said Dr. Lanford. “What is really exciting about these data, however, is that we appear to have seen immune de-repression, the next step toward HBsAg seroconversion and functional cure. The timing of the ALT rise and associated increases in key chemokine/cytokine mRNAs suggest that they were related to the therapy-induced reduction in circulating HBsAg and represented an immunological event.”
该数据表明的ARC- 520两种剂量( 2毫克/公斤, 3毫克/公斤)的黑猩猩慢性HBV感染的静脉给药,导致大量和持续降低HBV DNA和HBeAg ,与HBsAg ,哪些没有回到基线,直到分别研究一天43 , 43 ,和71 。此外,增加血清丙氨酸转氨酶( ALT )发生后4周的最后一剂,暗合循环HBsAg的最低点。这是暗示治疗免疫耀斑,这被认为是,在长期治疗可能导致HBsAg血清学转换和功能治愈级联的一部分。罗伯特·E·兰福德德州生物医学研究所在那里进行的研究,博士,发表上述研究资料和海报被选为优异的总统海报,表明它是在选定的所有论文摘要的前10%海报介绍。
“这项研究将是重要的,如果ARC- 520只是证明安全有效的乙肝表面抗原减少,因为这被认为是在实现一个功能治愈的必要步骤, ”兰福德博士说。 “什么是真正令人兴奋的关于这些数据,但是,我们似乎已经看到免疫力去压制,对HBsAg血清学转换和功能治愈下一步。的ALT升高和时间的关键趋化因子/细胞因子mRNA的增加相关联表明,它们均与循环中的乙肝表面抗原治疗引起的减少和代表的免疫活动。 “
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