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Structural modules for receptor dimerization in the S-locus receptor kinase extracellular domain

机译:S-基因座受体激酶胞外域中受体二聚化的结构模块

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The highly polymorphic S-locus receptor kinase (SRK) is the stigma determinant of specificity in the self-incompatibility response of the Brassicaceae. SRK spans the plasma membrane of stigma epidermal cells, and it is activated in an allele-specific manner on binding of its extracellular region (eSRK) to its cognate pollen coat-localized S-locus cysteine-rich (SCR) ligand. SRK, like several other receptor kinases, forms dimers in the absence of ligand. To identify domains in SRK that mediate ligand-independent dimerization, we assayed eSRK for self-interaction in yeast. We show that SRK dimerization is mediated by two regions in eSRK, primarily by a C-terminal region inferred by homology modeling/fold recognition techniques to assume a PAN_APPLE-like structure, and secondarily by a region containing a signature sequence of the S-domain gene family, which might assume an EGF-like structure. We also show that eSRK exhibits a marked preference for homodimerization rnover heterodimerization with other eSRK variants and that this preference is mediated by a small, highly variable region within the PAN_APPLE domain. Thus, the extensive polymorphism exhibited by the eSRK not only determines differential affinity toward the SCR ligand, as has been assumed thus far, but also underlies a previously unrecognized allelic specificity in SRK dimerization. We propose that preference for SRK homodimerization rnexplains the codominance exhibited by a majority of SRKs in the typically heterozygous stigmas of self-incompatible plants, whereas an increased propensity for heterodimerization combined with reduced affinity of heterodimers for cognate SCRs might underlie the dominant-recessive or mutual weakening relationships exhibited by some SRK allelic pairs.
机译:高度多态的S位基因受体激酶(SRK)是十字花科自交不亲和反应的特异性的柱头决定因素。 SRK跨过柱头表皮细胞的质膜,并在其胞外区(eSRK)与同源花粉被膜定位的富含S-基因座半胱氨酸(SCR)配体结合后以等位基因特异性方式被激活。 SRK与其他几种受体激酶一样,在不存在配体的情况下会形成二聚体。为了鉴定SRK中介导不依赖配体的二聚化的结构域,我们在酵母中检测了eSRK的自我相互作用。我们显示SRK二聚化是由eSRK中的两个区域介导的,主要是由通过同源建模/折叠识别技术推断为PAN_APPLE样结构的C端区域介导的,其次是由包含S结构域签名序列的区域介导的基因家族,可能具有类似EGF的结构。我们还显示,eSRK对同二聚体与其他eSRK变体的异二聚化表现出显着的偏爱,并且该偏爱由PAN_APPLE域内的一个很小的,高度可变的区域介导。因此,eSRK表现出的广泛多态性不仅决定了迄今为止对SCR配体的不同亲和力,而且还奠定了SRK二聚体中先前无法识别的等位基因特异性的基础。我们建议偏爱SRK同源二聚体rn解释大多数SRK在自交不亲和植物的典型杂合柱头上表现出的共性,而异源二聚化倾向的增加以及异源二聚体对同源SCR亲和力的降低可能是显性-隐性或互作的基础一些SRK等位基因对表现出的弱化关系。

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