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参与兰姆达霉素生产的 LanK 蛋白配体的生物学特性及作用位点分析。

Insights into the Biological Properties of Ligands and Identity of Operator Site for LanK Protein Involved in Landomycin Production.

机构信息

Department of Genetics and Biotechnology, Ivan Franko National University of Lviv, 4 Hrushevskoho St, Lviv, 79005, Ukraine.

Department of Chemistry, Tufts University, 62 Talbot Ave, Medford, MA, 02155, USA.

出版信息

Curr Microbiol. 2023 Nov 10;81(1):5. doi: 10.1007/s00284-023-03528-1.

Abstract

LanK is a TetR type regulatory protein that coordinates the late steps of the biosynthesis of the landomycin family of antitumor angucyclic polyketides and their export from the cells of Streptomyces cyanogenus S136. We recently described the structure of LanK and showed that it is the carbohydrate portion of the landomycins that is responsible for abrogating the repressing effect of LanK on landomycin production and export. The effect has been established in a series of in vitro tests using synthetic analogs of the landomycin carbohydrate chains. Whether such synthetic compounds would function as effector molecules for LanK under in vivo conditions remained unknown. Furthermore, the location and identity of LanK operator sites within the lanK-lanJ intergenic region (lanKJp) was unknown. Here we report that methoxyphenyl analogs of tri- and hexasaccharide chains of landomycins cannot function as LanK ligands when applied externally to the reporter strain. The lability of these compounds to cellular media and/or their poor penetration into the cells could explain our observations. The LanK operator site has been mapped to a 14-bp region of lanKJp that includes a plausible -35 site upstream of the lanK start codon in a series of electrophoretic DNA mobility shift assays. This opens the door to studies of the DNA-LanK interaction at a single nucleotide resolution level.

摘要

兰克是 TetR 型调节蛋白,它协调放线紫红素族抗肿瘤角环多酮生物合成的后期步骤及其从链霉菌 S136 细胞中的输出。我们最近描述了兰克的结构,并表明是放线紫霉素糖部分负责消除兰克对放线紫霉素产生和输出的抑制作用。这种效应已在一系列使用放线紫霉素糖链的合成类似物的体外试验中得到证实。在体内条件下,这些合成化合物是否能作为兰克的效应分子仍然未知。此外,兰克-兰 J 基因间区(lanKJp)内兰克操纵子位点的位置和身份尚不清楚。在这里,我们报告说,当应用于报告菌株时,兰克的三糖和六糖链的甲氧基苯类似物不能作为兰克配体发挥作用。这些化合物对细胞介质的不稳定性和/或它们进入细胞的能力较差可能解释了我们的观察结果。兰克操纵子位点已被定位到 lanKJp 的一个 14 碱基对区域,该区域包括一个在一系列电泳 DNA 迁移率变动分析中在兰克起始密码子上游的合理 -35 位点。这为在单个核苷酸分辨率水平上研究 DNA-LanK 相互作用打开了大门。

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