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使用可注射微球/水凝胶组合系统控制热休克蛋白的递送用于治疗心肌梗死。

Controlled delivery of heat shock protein using an injectable microsphere/hydrogel combination system for the treatment of myocardial infarction.

作者信息

Lee Jangwook, Tan Cheau Yih, Lee Sang-Kyung, Kim Yong-Hee, Lee Kuen Yong

机构信息

Department of Bioengineering, Hanyang University, Seoul 133-791, Republic of Korea.

出版信息

J Control Release. 2009 Aug 4;137(3):196-202. doi: 10.1016/j.jconrel.2009.04.008. Epub 2009 Apr 14.

Abstract

Myocardial infarction causes a high rate of morbidity and mortality worldwide, and heat shock proteins as molecular chaperones have been attractive targets for protecting cardiomyoblasts under environmental stimuli. In this study, in order to enhance the penetration of heat shock protein 27 (HSP27) across cell membranes, we fused HSP27 with transcriptional activator (TAT) derived from human immunodeficiency virus (HIV) as a protein transduction domain (PTD). We loaded the fusion protein (TAT-HSP27) into microsphere/hydrogel combination delivery systems to control the release behavior for prolonged time periods. We found that the release behavior of TAT-HSP27 was able to be controlled by varying the ratio of PLGA microspheres and alginate hydrogels. Indeed, the released fusion protein maintained its bioactivity and could recover the proliferation of cardiomyoblasts cultured under hypoxic conditions. This approach to controlling the release behavior of TAT-HSP27 using microsphere/hydrogel combination delivery systems may be useful for treating myocardial infarction in a minimally invasive manner.

摘要

心肌梗死在全球范围内导致了很高的发病率和死亡率,而热休克蛋白作为分子伴侣,在环境刺激下一直是保护心肌细胞的有吸引力的靶点。在本研究中,为了增强热休克蛋白27(HSP27)穿过细胞膜的能力,我们将HSP27与人免疫缺陷病毒(HIV)来源的转录激活因子(TAT)融合,作为蛋白转导结构域(PTD)。我们将融合蛋白(TAT-HSP27)加载到微球/水凝胶组合递送系统中,以控制其长时间的释放行为。我们发现,通过改变聚乳酸-羟基乙酸共聚物(PLGA)微球和海藻酸钠水凝胶的比例,可以控制TAT-HSP27的释放行为。事实上,释放的融合蛋白保持了其生物活性,并且可以恢复在缺氧条件下培养的心肌细胞的增殖。这种使用微球/水凝胶组合递送系统控制TAT-HSP27释放行为的方法,可能有助于以微创方式治疗心肌梗死。

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