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[人胰岛素及其衍生物作为具有潜在抗凋亡和已证实神经保护活性的肽]

[Humanin and its derivatives as peptides with potential antiapoptotic and confirmed neuroprotective activities].

作者信息

Zapała Barbara, Staszel Teresa, Kieć-Wilk Beata, Polus Anna, Knapp Anna, Wybrańska Iwona, Kaczyński Łukasz, Dembińska-Kieć Aldona

机构信息

Katedra i Zakład Biochemii Klinicznej, Uniwersytet Jagielloński, Collegium Medicum, Kraków.

出版信息

Przegl Lek. 2011;68(7):372-7.

PMID:22010475
Abstract

Humanin (HN) is a newly discovered 24-amino acid peptide, which may suppress neuronal cell death. HN cDNA includes the open reading frame (HN-ORF) of 75 bases, located 950 bases downstream of the 5' end of the HN cDNA. It was demonstrated that HN cDNA is 99% identical with mitochondrial DNA (mtDNA) sequence. HN homologues have been identified as expressed sequence tags (ESTs) in rat and nematode. Certain regions homologous to the HN cDNA exist on human chromosomes. HN forms homodimers and multimers and this seems to be essential for the peptide functions. HN acts as a ligand for formyl peptide receptor-like 1 (FPRL1) and 2 (FPRL2). It was demonstrated that HN plays a protective role by an antiapoptotic activity interfering with Bax activation, and suppressing Bax-dependent apoptosis. HN is also shown to suppress the c-Jun N-terminal kinase (JNK) and ASK/JNK-mediated neuronal cell death. Several studies also confirm that HN could be important in prevention of angiopathy-associated Alzheimer's disease dementia, diseases related to mitochondrial dysfunction (MELAS), and other types of beta-amyloid accumulation associated neurodegeneration. A very recent study demonstrated a pluripotent cytoprotective effect and mechanisms of HNs in cells other than from the CNS, such as germ cells, or panreatic b-cells, and potent physiological consequences that result from HN interaction with IGFBP3 and STAT3. The in vivo studies suggest that humanin may protect against cognitive impairment, also due to ischemia/reperfusion injury.

摘要

人胰岛素(HN)是一种新发现的由24个氨基酸组成的肽,它可能抑制神经元细胞死亡。HN cDNA包含一个75个碱基的开放阅读框(HN-ORF),位于HN cDNA 5'端下游950个碱基处。已证明HN cDNA与线粒体DNA(mtDNA)序列有99%的同一性。在大鼠和线虫中,HN同源物已被鉴定为表达序列标签(ESTs)。人类染色体上存在与HN cDNA同源的某些区域。HN形成同型二聚体和多聚体,这似乎对该肽的功能至关重要。HN作为甲酰肽受体样1(FPRL1)和2(FPRL2)的配体发挥作用。已证明HN通过干扰Bax激活的抗凋亡活性和抑制Bax依赖性凋亡发挥保护作用。HN还被证明可抑制c-Jun N端激酶(JNK)和ASK/JNK介导的神经元细胞死亡。多项研究还证实,HN在预防血管病相关的阿尔茨海默病痴呆、与线粒体功能障碍相关的疾病(MELAS)以及其他类型的β-淀粉样蛋白积累相关的神经退行性变中可能很重要。最近的一项研究证明了HN在中枢神经系统以外的细胞(如生殖细胞或胰腺β细胞)中的多能细胞保护作用及其机制,以及HN与IGFBP3和STAT3相互作用产生的强大生理后果。体内研究表明,人胰岛素也可能预防由缺血/再灌注损伤引起的认知障碍。

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Przegl Lek. 2011;68(7):372-7.
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