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天然内皮细胞中磷酸肌醇特异性磷脂酶C同工型的表达

Expression of phosphoinositide-specific phospholipase C isoforms in native endothelial cells.

作者信息

Béziau Delphine M, Toussaint Fanny, Blanchette Alexandre, Dayeh Nour R, Charbel Chimène, Tardif Jean-Claude, Dupuis Jocelyn, Ledoux Jonathan

机构信息

Research Center, Montreal Heart Institute, Montreal, Qc, Canada; Department of Molecular and Integrative Physiology, Université de Montréal, Montreal, Qc, Canada.

Research Center, Montreal Heart Institute, Montreal, Qc, Canada.

出版信息

PLoS One. 2015 Apr 13;10(4):e0123769. doi: 10.1371/journal.pone.0123769. eCollection 2015.

Abstract

Phospholipase C (PLC) comprises a superfamily of enzymes that play a key role in a wide array of intracellular signalling pathways, including protein kinase C and intracellular calcium. Thirteen different mammalian PLC isoforms have been identified and classified into 6 families (PLC-β, γ, δ, ε, ζ and η) based on their biochemical properties. Although the expression of PLC isoforms is tissue-specific, concomitant expression of different PLC has been reported, suggesting that PLC family is involved in multiple cellular functions. Despite their critical role, the PLC isoforms expressed in native endothelial cells (ECs) remains undetermined. A conventional PCR approach was initially used to elucidate the mRNA expression pattern of PLC isoforms in 3 distinct murine vascular beds: mesenteric (MA), pulmonary (PA) and middle cerebral arteries (MCA). mRNA encoding for most PLC isoforms was detected in MA, MCA and PA with the exception of η2 and β2 (only expressed in PA), δ4 (only expressed in MCA), η1 (expressed in all but MA) and ζ (not detected in any vascular beds tested). The endothelial-specific PLC expression was then sought in freshly isolated ECs. Interestingly, the PLC expression profile appears to differ across the investigated arterial beds. While mRNA for 8 of the 13 PLC isoforms was detected in ECs from MA, two additional PLC isoforms were detected in ECs from PA and MCA. Co-expression of multiple PLC isoforms in ECs suggests an elaborate network of signalling pathways: PLC isoforms may contribute to the complexity or diversity of signalling by their selective localization in cellular microdomains. However in situ immunofluorescence revealed a homogeneous distribution for all PLC isoforms probed (β3, γ2 and δ1) in intact endothelium. Although PLC isoforms play a crucial role in endothelial signal transduction, subcellular localization alone does not appear to be sufficient to determine the role of PLC in the signalling microdomains found in the native endothelium.

摘要

磷脂酶C(PLC)是一类酶的超家族,在包括蛋白激酶C和细胞内钙在内的多种细胞内信号通路中起关键作用。已鉴定出13种不同的哺乳动物PLC亚型,并根据其生化特性分为6个家族(PLC-β、γ、δ、ε、ζ和η)。尽管PLC亚型的表达具有组织特异性,但已有报道不同PLC亚型可同时表达,这表明PLC家族参与多种细胞功能。尽管其作用至关重要,但在天然内皮细胞(ECs)中表达的PLC亚型仍未确定。最初采用常规PCR方法来阐明PLC亚型在3种不同的小鼠血管床中的mRNA表达模式:肠系膜动脉(MA)、肺动脉(PA)和大脑中动脉(MCA)。在MA、MCA和PA中检测到了大多数PLC亚型的编码mRNA,但η2和β2(仅在PA中表达)、δ4(仅在MCA中表达)、η1(除MA外均有表达)和ζ(在所检测的任何血管床中均未检测到)除外。随后在新鲜分离的ECs中寻找内皮特异性的PLC表达。有趣的是,PLC的表达谱在不同的动脉床中似乎有所不同。在MA的ECs中检测到了13种PLC亚型中的8种的mRNA,而在PA和MCA的ECs中又检测到了另外两种PLC亚型。ECs中多种PLC亚型的共表达提示了一个复杂的信号通路网络:PLC亚型可能通过其在细胞微区中的选择性定位,对信号传导的复杂性或多样性有贡献。然而,原位免疫荧光显示,在所检测的完整内皮中,所有被检测的PLC亚型(β3、γ2和δ1)均呈均匀分布。尽管PLC亚型在内皮信号转导中起关键作用,但仅亚细胞定位似乎不足以确定PLC在天然内皮中发现的信号微区中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f80/4395365/a9b49649469b/pone.0123769.g001.jpg

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