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核盘菌专化型 ssp1 和 ssp2 基因编码的凝集素具有不同但互补的调控作用。

The development-specific ssp1 and ssp2 genes of Sclerotinia sclerotiorum encode lectins with distinct yet compensatory regulation.

机构信息

Department of Plant Pathology, University of Florida, Gainesville, FL 32611-0680, USA.

出版信息

Fungal Genet Biol. 2010 Jun;47(6):531-8. doi: 10.1016/j.fgb.2010.03.008. Epub 2010 Mar 27.

Abstract

The Ssp1 development-specific protein is the most abundant soluble protein in sclerotia and apothecia of Sclerotinia sclerotiorum. Although closely associated with these developmental stages, the functions of the Ssp1 protein and its paralog, Ssp2, are not known. In this study, protein structure prediction analysis revealed that Ssp1 and Ssp2 are structurally similar to fucose-specific lectins. In an effort to understand the function of these abundant, development-specific proteins, a homokaryotic ssp1 deletion mutant was generated. The resulting mutant (Deltassp1) displays a wild-type growth and development phenotype in culture but produces approximately 50% fewer sclerotia in cultures supplemented with hygromycin. Genetic complementation with a wild-type copy of ssp1 restores normal sclerotium formation in the presence of hygromycin. This suggests that Ssp1 might play a role in resistance to glycoside-containing antibiotics encountered in the environment. Although a slight delay in carpogenic germination was observed, no additional effects of ssp1 loss-of-function were found in regards to apothecial morphology or fecundity. When the expression of ssp2 was examined in the Deltassp1 mutant, it was found to be expressed earlier in sclerotial development and its encoded protein accumulated to higher levels in both sclerotia and apothecia. These findings suggest regulatory compensation for loss of Ssp1 coupled with potential functional redundancy among lectins accumulating in sclerotia and apothecia.

摘要

Ssp1 发育特异性蛋白是核盘菌菌核和子囊壳中含量最丰富的可溶性蛋白。尽管 Ssp1 蛋白及其同源物 Ssp2 与这些发育阶段密切相关,但它们的功能尚不清楚。本研究通过蛋白质结构预测分析发现,Ssp1 和 Ssp2 与岩藻糖特异性凝集素在结构上具有相似性。为了研究这些丰富的、发育特异性蛋白的功能,我们构建了 Ssp1 同源缺失突变体。该突变体(Deltassp1)在培养过程中表现出与野生型相似的生长和发育表型,但在添加潮霉素的培养基中形成的菌核数量减少约 50%。用野生型 ssp1 基因进行遗传互补,可在潮霉素存在的情况下恢复正常菌核的形成。这表明 Ssp1 可能在抵抗环境中糖苷类抗生素方面发挥作用。尽管观察到其产子实体的能力略有延迟,但在子囊壳形态或产孢能力方面,ssp1 缺失功能没有发现其他影响。当在 Deltassp1 突变体中检测 ssp2 的表达时,发现其在菌核发育早期表达,并在菌核和子囊壳中积累到更高的水平。这些发现表明,Ssp1 缺失后可能会发生调控补偿,同时在菌核和子囊壳中积累的凝集素可能具有潜在的功能冗余。

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