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辅酶Q合成基因Smed-dlp1的敲低影响涡虫再生和组织稳态。

Knockdown of the coenzyme Q synthesis gene Smed-dlp1 affects planarian regeneration and tissue homeostasis.

作者信息

Shiobara Yumiko, Harada Chiaki, Shiota Takeshi, Sakamoto Kimitoshi, Kita Kiyoshi, Tanaka Saeko, Tabata Kenta, Sekie Kiyoteru, Yamamoto Yorihiro, Sugiyama Tomoyasu

机构信息

Graduate School of Bionics, Tokyo University of Technology, Hachioji-shi, Tokyo 192-0982, Japan.

Department of Biochemistry and Molecular Biology, Faculty of Agriculture and Life Science, Hirosaki University, Aomori 036-8561, Japan.

出版信息

Redox Biol. 2015 Dec;6:599-606. doi: 10.1016/j.redox.2015.10.004. Epub 2015 Oct 21.

Abstract

The freshwater planarian is a model organism used to study tissue regeneration that occupies an important position among multicellular organisms. Planarian genomic databases have led to the identification of genes that are required for regeneration, with implications for their roles in its underlying mechanism. Coenzyme Q (CoQ) is a fundamental lipophilic molecule that is synthesized and expressed in every cell of every organism. Furthermore, CoQ levels affect development, life span, disease and aging in nematodes and mice. Because CoQ can be ingested in food, it has been used in preventive nutrition. In this study, we investigated the role of CoQ in planarian regeneration. Planarians synthesize both CoQ9 and rhodoquinone 9 (RQ9). Knockdown of Smed-dlp1, a trans-prenyltransferase gene that encodes an enzyme that synthesizes the CoQ side chain, led to a decrease in CoQ9 and RQ9 levels. However, ATP levels did not consistently decrease in these animals. Knockdown animals exhibited tissue regression and curling. The number of mitotic cells decreased in Smed-dlp1 (RNAi) animals. These results suggested a failure in physiological cell turnover and stem cell function. Accordingly, regenerating planarians died from lysis or exhibited delayed regeneration. Interestingly, the observed phenotypes were partially rescued by ingesting food supplemented with α-tocopherol. Taken together, our results suggest that oxidative stress induced by reduced CoQ9 levels affects planarian regeneration and tissue homeostasis.

摘要

淡水涡虫是一种用于研究组织再生的模式生物,在多细胞生物中占据重要地位。涡虫基因组数据库已导致了对再生所需基因的鉴定,这对它们在其潜在机制中的作用具有启示意义。辅酶Q(CoQ)是一种基本的亲脂性分子,在每个生物体的每个细胞中合成并表达。此外,CoQ水平影响线虫和小鼠的发育、寿命、疾病和衰老。由于CoQ可以在食物中摄取,它已被用于预防性营养。在本研究中,我们研究了CoQ在涡虫再生中的作用。涡虫能合成CoQ9和玫红醌9(RQ9)。敲低Smed-dlp1,一个编码合成CoQ侧链的酶的反式异戊二烯基转移酶基因,导致CoQ9和RQ9水平降低。然而,这些动物的ATP水平并没有持续下降。敲低的动物表现出组织退化和卷曲。Smed-dlp1(RNA干扰)动物中有丝分裂细胞的数量减少。这些结果表明生理细胞更新和干细胞功能出现故障。因此,正在再生的涡虫死于裂解或表现出再生延迟。有趣的是,通过摄取补充有α-生育酚的食物,观察到的表型部分得到挽救。综上所述,我们的结果表明CoQ9水平降低诱导的氧化应激影响涡虫再生和组织稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/80c4/4635435/74969a8488f5/fx1.jpg

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