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拟南芥中3-羟基-3-甲基戊二酰辅酶A还原酶1(HMG1)功能丧失会导致植株矮化、早衰和雄性不育,并降低甾醇水平。

Loss of function of 3-hydroxy-3-methylglutaryl coenzyme A reductase 1 (HMG1) in Arabidopsis leads to dwarfing, early senescence and male sterility, and reduced sterol levels.

作者信息

Suzuki Masashi, Kamide Yukiko, Nagata Noriko, Seki Hikaru, Ohyama Kiyoshi, Kato Hisashi, Masuda Kazuo, Sato Shusei, Kato Tomohiko, Tabata Satoshi, Yoshida Shigeo, Muranaka Toshiya

机构信息

Plant Science Center, RIKEN, Tsurumi-ku, Yokohama, Kanagawa 230-0045, Japan.

出版信息

Plant J. 2004 Mar;37(5):750-61. doi: 10.1111/j.1365-313x.2004.02003.x.

Abstract

3-Hydroxy-3-methylglutaryl-CoA reductase (HMGR) catalyzes the first committed step in the cytosolic isoprenoid biosynthesis pathway in higher plants. To understand the contribution of HMGR to plant development, we isolated T-DNA insertion mutants for HMG1 and HMG2. The hmg1 and hmg2 mutants were both more sensitive than the wild type (WT) to lovastatin, an inhibitor of HMGR. The hmg2 mutant showed no visible phenotype under normal growth conditions. In contrast, the hmg1 mutant exhibited dwarfing, early senescence, and sterility. Expression of senescence-associated genes 12 (SAG12), a marker gene for senescence, was induced in the hmg1 mutant at an earlier stage than in the WT. Levels of trans-cytokinins--hormones known to inhibit senescence--were not lower in hmg1. The mutant did not have the typical appearance of brassinosteroid (BR)-deficient mutants, except for a dwarf phenotype, because of the suppression of cell elongation. The expression of several genes involved in cell elongation was suppressed in hmg1. WT plants treated exogenously with inhibitors of sterol biosynthesis had similar gene expression and sterility characteristics as the hmg1 mutants. Pleiotropic phenotypes were rescued by feeding with squalene, the precursor of sterols and triterpenoids. The sterol levels in hmg1 mutants were lower than in the WT. These findings suggest that HMG1 plays a critical role in triterpene biosynthesis, and that sterols and/or triterpenoids contribute to cell elongation, senescence, and fertility.

摘要

3-羟基-3-甲基戊二酰辅酶A还原酶(HMGR)催化高等植物胞质类异戊二烯生物合成途径中的首个关键步骤。为了解HMGR对植物发育的贡献,我们分离了HMG1和HMG2的T-DNA插入突变体。hmg1和hmg2突变体对HMGR抑制剂洛伐他汀均比野生型(WT)更敏感。hmg2突变体在正常生长条件下未表现出可见表型。相比之下,hmg1突变体表现出矮化、早衰和不育。衰老相关基因12(SAG12)是衰老的标记基因,其在hmg1突变体中的表达比在WT中诱导得更早。反式细胞分裂素(已知可抑制衰老的激素)水平在hmg1中并不低。该突变体除了矮化表型外,没有油菜素内酯(BR)缺陷型突变体的典型外观,这是由于细胞伸长受到抑制。hmg1中几个参与细胞伸长的基因表达受到抑制。用甾醇生物合成抑制剂外源处理的WT植物具有与hmg1突变体相似的基因表达和不育特征。通过饲喂角鲨烯(甾醇和三萜类化合物的前体)可挽救多效性表型。hmg1突变体中的甾醇水平低于WT。这些发现表明HMG1在三萜生物合成中起关键作用,并且甾醇和/或三萜类化合物有助于细胞伸长、衰老和育性。

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