We have previously mapped the interval on Chromosome 4 for a major polycystic kidney disease modifier (Mpkd) of the B6(Cg)-Cys1cpk/J mouse model of recessive polycystic kidney disease (PKD). Informatic analyses predicted that this interval contains at least three individual renal cystic disease severity-modulating loci (Mpkd1-3). In the current study, we provide further validation of these predicted effects using a congenic mouse line carrying the entire CAST/EiJ (CAST)-derived Mpkd1-3 interval on the C57BL/6J background. We have also generated a derivative congenic line with a refined CAST-derived Mpkd1-2 interval and demonstrated its dominantly-acting disease-modulating effects (e.g., 4.2-fold increase in total cyst area; p<0.001). The relative strength of these effects allowed the use of recombinants from these crosses to fine map the Mpkd2 effects to a <14 Mbp interval that contains 92 RefSeq sequences. One of them corresponds to the previously described positional Mpkd2 candidate gene, Kif12. Among the positional Mpkd2 candidates, only expression of Kif12 correlates strongly with the expression pattern of Cys1 across multiple anatomical nephron structures and developmental time points. Also, we demonstrate that Kif12 encodes a primary cilium-associated protein. Together, these data provide genetic and informatic validation of the predicted renal cystic disease-modulating effects of Mpkd1-3 loci and implicate Kif12 as the candidate locus for Mpkd2.
Genetic and Informatic Analyses Implicate Kif12 as a Candidate Gene within the Mpkd2 Locus That Modulates Renal Cystic Disease Severity in the Cys1cpk Mouse.
遗传和信息学分析表明,Kif12 是 Mpkd2 位点内的候选基因,可以调节 Cys1cpk 小鼠肾囊性疾病的严重程度
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作者:Mrug Michal, Zhou Juling, Yang Chaozhe, Aronow Bruce J, Cui Xiangqin, Schoeb Trenton R, Siegal Gene P, Yoder Bradley K, Guay-Woodford Lisa M
| 期刊: | PLoS One | 影响因子: | 2.600 |
| 时间: | 2015 | 起止号: | 2015 Aug 21; 10(8):e0135678 |
| doi: | 10.1371/journal.pone.0135678 | 种属: | Mouse |
| 研究方向: | 其它 | ||
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