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Functional Polymorphisms of the Lss and Fdft1 Genes in Laboratory Rats

机译:Lss和Fdft1基因在实验大鼠中的功能多态性

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We previously identified mutant alleles of the lanosterol synthase (Lss) and farnesyl diphosphate farnesyl transferase 1 (Fdft1) genes, which function in the cholesterol biosynthesis pathway, as determinants for hereditary cataracts in the SCR rat strain. Lss~S and Fdft1~S were established as hypomorphic alleles with missense nucleotide substitutions, while Lss~l is a null allele with nucleotide deletion/insertion mutations. Here we report a more detailed characterization of the rat Lss and Fdft1 genes. Screening of various laboratory rat strains revealed that the hypomorphic Lss~S and Fdft1~S alleles are not specific to the SCR strain, but are widely prevalent in other laboratory rat strains. Meanwhile, Lss~l was not found in any rat strains examined. It was also found that functional inter-strain polymorphisms are present in the Lss upstream regulatory region. The BN strain had a higher potential for expression of Lss transcripts than ACI and SCR under conditions where cholesterol synthesis is necessary. SCR was less efficient than BN and ACI in suppressing Lss transcription in circumstances when cholesterol synthesis should be halted. These findings not only imply that there is a genetic polymorphism for cholesterol homeostasis in laboratory rats, but also point to the possibility that rat strains with different Lss alleles exhibit different responses to measures intervening in cholesterol metabolism.
机译:我们先前确定了羊毛甾醇合酶(Lss)和法呢基二磷酸法呢基转移酶1(Fdft1)基因的突变等位基因,其在胆固醇生物合成途径中起作用,作为SCR大鼠株中遗传性白内障的决定因素。 Lss〜S和Fdft1〜S被确定为具有错义核苷酸取代的亚同等位基因,而Lss_1则是具有核苷酸缺失/插入突变的无效等位基因。在这里,我们报告大鼠Lss和Fdft1基因的更详细的表征。对各种实验室大鼠品系的筛选显示,亚型的Lss〜S和Fdft1〜S等位基因不是SCR菌株特异的,但在其他实验室大鼠品系中普遍存在。同时,在所检查的任何大鼠品系中均未发现Lss-1。还发现功能性菌株间多态性存在于Lss上游调节区中。在需要胆固醇合成的条件下,BN菌株比ACI和SCR具有更高的表达Lss转录物的潜力。在胆固醇合成应停止的情况下,SCR在抑制Lss转录方面不如BN和ACI有效。这些发现不仅暗示实验室大鼠胆固醇稳态存在遗传多态性,而且还指出具有不同Lss等位基因的大鼠品系对干预胆固醇代谢的措施表现出不同反应的可能性。

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