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在一个骨尺寸减小的ENU突变体中鉴定骨大小和机械敏感性的新基因位点。

Identification of novel genetic loci for bone size and mechanosensitivity in an ENU mutant exhibiting decreased bone size.

作者信息

Srivastava Apurva K, Kapur Sanjay, Mohan Suburaman, Yu Hongrun, Kapur Sonia, Wergedal Jon, Baylink David J

机构信息

Musculoskeletal Disease Center, Jerry L. Pettis Veterans Administration Medical Center, Loma Linda, California 92357, USA.

出版信息

J Bone Miner Res. 2005 Jun;20(6):1041-50. doi: 10.1359/JBMR.041239. Epub 2004 Dec 27.

Abstract

UNLABELLED

Using a dominant ENU mutagenesis screen in C57BL/6J (B6) mice to reveal gene function, we identified a mutant, 917M, with a reduced bone size phenotype, which is expressed only in males. We show that mutation results in osteoblasts with reduced proliferation, increased apoptosis, and an impaired response to in vitro mechanical load. The mutation is mapped to a novel locus (LOD score of 7.9 at 10.5 cM) on chromosome 4.

INTRODUCTION

Using a dominant ENU mutagenesis screen in C57BL/6J (B6) mice to reveal gene function, we identified a mutant, 917M, with a reduced bone size phenotype, which is expressed only in males. In this report, we show the chromosomal location of this mutation using linkage analysis and cellular characterization of the mutant phenotype.

MATERIALS AND METHODS

The mutant mouse was bred to wildtype B6 to produce progeny for characterization of the bone size phenotype. Periosteal osteoblasts isolated from the tibia and femur of mutant and wildtype mice were studied for proliferation, differentiation, and apoptosis potential. To determine the chromosomal location of the mutation, a low-resolution linkage map was established by completing a genome-wide scan in B6C3H F2 male mice generated from intercross breeding of mutant mice.

RESULTS AND CONCLUSIONS

Mutant progeny (16 weeks old) displayed a total body bone area that was 10-13% lower and a periosteal circumference that was 5-8% lower at the femur and tibia midshaft compared with wildtype B6 mice. Periosteal osteoblasts from mutant mice showed 17-27% reduced cell proliferation and 23% increased apoptosis compared with wildtype controls. In addition, osteoblasts from mutant mice showed an impaired response to shear stress-induced proliferation rate, an in vitro model for mechanical loading. Interval mapping in B6C3H F2 males (n = 69) indicated two major loci affecting bone size on chromosome 1 at 45 cM (LOD 4.9) and chromosome 4 at 10.5 cM (LOD 7.9, genome-wide p < 0.01). Interval mapping using body weight as covariate revealed only one significant interval at chromosome 4 (LOD 6.8). Alleles of the chromosome 4 interval inherited from the B6 mutant strain contributed to a significantly lower bone size than those inherited from C3H. A pairwise interaction analysis showed evidence for a significant interaction between loci on chromosome 1 with the chromosome 4 quantitative trait loci. The 917M locus on chromosome 4 seems to be novel because it does not correspond with those loci previously associated with bone size on chromosome 4 in B6 and C3H/HeJ mice or other crosses.

摘要

未标记

利用对C57BL/6J(B6)小鼠进行的显性ENU诱变筛选来揭示基因功能,我们鉴定出一个突变体917M,其具有骨尺寸减小的表型,且仅在雄性中表达。我们发现该突变导致成骨细胞增殖减少、凋亡增加以及对体外机械负荷的反应受损。该突变被定位到4号染色体上的一个新位点(在10.5 cM处的LOD分数为7.9)。

引言

利用对C57BL/6J(B6)小鼠进行的显性ENU诱变筛选来揭示基因功能,我们鉴定出一个突变体917M,其具有骨尺寸减小的表型,且仅在雄性中表达。在本报告中,我们使用连锁分析和突变体表型的细胞特征分析展示了该突变的染色体定位。

材料与方法

将突变小鼠与野生型B6杂交以产生后代,用于骨尺寸表型的特征分析。研究了从突变小鼠和野生型小鼠的胫骨和股骨中分离出的骨膜成骨细胞的增殖、分化和凋亡潜能。为了确定突变的染色体定位,通过对由突变小鼠杂交繁殖产生的B6C3H F2雄性小鼠进行全基因组扫描,建立了一个低分辨率连锁图谱。

结果与结论

与野生型B6小鼠相比,突变后代(16周龄)的全身骨面积低10 - 13%,股骨和胫骨中段的骨膜周长低5 - 8%。与野生型对照相比,突变小鼠的骨膜成骨细胞显示细胞增殖减少17 - 27%,凋亡增加23%。此外,突变小鼠的成骨细胞对剪切应力诱导的增殖率反应受损,这是一种机械负荷的体外模型。对B6C3H F2雄性小鼠(n = 69)进行区间定位表明,在1号染色体上45 cM处(LOD 4.9)和4号染色体上10.5 cM处(LOD 7.9,全基因组p < 0.01)有两个影响骨尺寸的主要位点。以体重作为协变量进行区间定位仅在4号染色体上发现一个显著区间(LOD 6.8)。从B6突变株遗传而来的4号染色体区间的等位基因导致的骨尺寸明显低于从C3H遗传而来的等位基因。成对相互作用分析显示1号染色体上的位点与4号染色体上的数量性状位点之间存在显著相互作用的证据。4号染色体上的917M位点似乎是新的,因为它与B6和C3H/HeJ小鼠或其他杂交组合中先前与4号染色体上骨尺寸相关的那些位点不对应。

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