Caspase-3 mediated release of SAC domain containing fragment from Par-4 is necessary for the sphingosine-induced apoptosis in Jurkat cells.

Q2 Biochemistry, Genetics and Molecular Biology Journal of Molecular Signaling Pub Date : 2013-02-27 DOI:10.1186/1750-2187-8-2
Faisal Thayyullathil, Siraj Pallichankandy, Anees Rahman, Jaleel Kizhakkayil, Shahanas Chathoth, Mahendra Patel, Sehamuddin Galadari
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引用次数: 29

Abstract

Background: Prostate apoptosis response-4 (Par-4) is a tumor-suppressor protein that selectively activates and induces apoptosis in cancer cells, but not in normal cells. The cancer specific pro-apoptotic function of Par-4 is encoded in its centrally located SAC (Selective for Apoptosis induction in Cancer cells) domain (amino acids 137-195). The SAC domain itself is capable of nuclear entry, caspase activation, inhibition of NF-κB activity, and induction of apoptosis in cancer cells. However, the precise mechanism(s) of how the SAC domain is released from Par-4, in response to apoptotic stimulation, is not well explored.

Results: In this study, we demonstrate for the first time that sphingosine (SPH), a member of the sphingolipid family, induces caspase-dependant cleavage of Par-4, leading to the release of SAC domain containing fragment from it. Par-4 is cleaved at the EEPD131G site on incubation with caspase-3 in vitro, and by treating cells with several anti-cancer agents. The caspase-3 mediated cleavage of Par-4 is blocked by addition of the pan-caspase inhibitor z-VAD-fmk, caspase-3 specific inhibitor Ac-DEVD-CHO, and by introduction of alanine substitution for D131 residue. Moreover, suppression of SPH-induced Akt dephosphorylation also abrogated the caspase dependant cleavage of Par-4.

Conclusion: Evidence provided here shows that Par-4 is cleaved by caspase-3 during SPH-induced apoptosis. Cleavage of Par-4 leads to the generation of SAC domain containing fragment which may possibly be essential and sufficient to induce or augment apoptosis in cancer cells.

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Caspase-3介导的Par-4中含有SAC结构域片段的释放是鞘氨醇诱导Jurkat细胞凋亡的必要条件。
背景:前列腺凋亡反应-4 (Par-4)是一种肿瘤抑制蛋白,在癌细胞中选择性激活和诱导细胞凋亡,而在正常细胞中不具有选择性。par4的癌症特异性促凋亡功能编码于其位于中心位置的SAC (Selective for Apoptosis induction in cancer cells)结构域(氨基酸137-195)。SAC结构域本身能够在癌细胞中进入核、激活caspase、抑制NF-κB活性和诱导凋亡。然而,在凋亡刺激下SAC结构域如何从Par-4释放的确切机制尚未得到很好的探讨。结果:在本研究中,我们首次证明鞘脂家族成员sphingosin (SPH)诱导par4的caspase依赖性切割,导致其释放含有SAC结构域的片段。在体外与caspase-3孵育以及用几种抗癌药物治疗细胞时,Par-4在EEPD131G位点被切割。通过添加泛caspase抑制剂z-VAD-fmk、caspase-3特异性抑制剂Ac-DEVD-CHO以及引入丙氨酸取代D131残基,caspase-3介导的Par-4裂解被阻断。此外,抑制sph诱导的Akt去磷酸化也消除了caspase依赖性的Par-4切割。结论:在sph诱导的细胞凋亡过程中,par4被caspase-3切割。par4的切割导致含有SAC结构域的片段的产生,这可能是诱导或增强癌细胞凋亡所必需和充分的。
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Journal of Molecular Signaling
Journal of Molecular Signaling Biochemistry, Genetics and Molecular Biology-Biochemistry
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期刊介绍: Journal of Molecular Signaling is an open access, peer-reviewed online journal that encompasses all aspects of molecular signaling. Molecular signaling is an exponentially growing field that encompasses different molecular aspects of cell signaling underlying normal and pathological conditions. Specifically, the research area of the journal is on the normal or aberrant molecular mechanisms involving receptors, G-proteins, kinases, phosphatases, and transcription factors in regulating cell proliferation, differentiation, apoptosis, and oncogenesis in mammalian cells. This area also covers the genetic and epigenetic changes that modulate the signaling properties of cells and the resultant physiological conditions.
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