12个近交系小鼠品系的骨微结构及其相关遗传变异性:显微CT研究与计算机基因组扫描
Bone microstructure and its associated genetic variability in 12 inbred mouse strains: microCT study and in silico genome scan.
作者信息
Sabsovich Ilya, Clark J David, Liao Guochun, Peltz Gary, Lindsey Derek P, Jacobs Christopher R, Yao Wei, Guo Tian-Zhi, Kingery Wade S
机构信息
Physical Medicine and Rehabilitation Service, Veterans Affairs Palo Alto Health Care System, Palo Alto, California 94304, USA.
出版信息
Bone. 2008 Feb;42(2):439-51. doi: 10.1016/j.bone.2007.09.041. Epub 2007 Sep 22.
UNLABELLED
MicroCT analysis of 12 inbred strains of mice identified 5 novel chromosomal regions influencing skeletal phenotype. Bone morphology varied in a compartment- and site-specific fashion across strains and genetic influences contributed to the morphometric similarities observed in femoral and vertebral bone within the trabecular bone compartment.
INTRODUCTION
Skeletal development is known to be regulated by both heritable and environmental factors, but whether genetic influence on peak bone mass is site- or compartment-specific is unknown. This study examined the genetic variation of cortical and trabecular bone microarchitecture across 12 strains of mice.
MATERIALS AND METHODS
MicroCT scanning was used to measure trabecular and cortical bone morphometry in the femur and vertebra of 12 strains of 4-month-old inbred male mice. A computational genome mapping technique was used to identify chromosomal intervals associated with skeletal traits.
RESULTS
Skeletal microarchitecture varied in a compartment- and site-specific fashion across strains. Genome mapping identified 13 chromosomal intervals associated with skeletal traits and 5 of these intervals were novel. Trabecular microarchitecture in different bone sites correlated across strains and most of the chromosomal intervals associated with these trabecular traits were shared between skeletal sites. Conversely, no chromosomal intervals were shared between the trabecular and cortical bone compartments in the femur, even though there was a strong correlation for these different bone compartments across strains, suggesting site-specific regulation by environmental or intrinsic factors.
CONCLUSION
In summary, these data confirm that there are distinct genetic determinants that define the skeletal phenotype at the time when peak bone mass is being acquired, and that genomic regulation of bone morphology is specific for skeletal compartment.
未标记
对12个近交系小鼠进行的显微CT分析确定了5个影响骨骼表型的新染色体区域。不同品系间骨形态在不同骨区和特定部位存在差异,遗传因素导致了小梁骨区股骨和椎骨形态测量上的相似性。
引言
已知骨骼发育受遗传和环境因素调控,但遗传因素对骨峰值的影响是否具有部位或骨区特异性尚不清楚。本研究检测了12个品系小鼠皮质骨和小梁骨微结构的遗传变异。
材料与方法
采用显微CT扫描测量12个品系4月龄近交雄性小鼠股骨和椎骨的小梁骨和皮质骨形态。运用计算基因组图谱技术鉴定与骨骼性状相关的染色体区间。
结果
不同品系间骨骼微结构在骨区和特定部位存在差异。基因组图谱鉴定出13个与骨骼性状相关的染色体区间,其中5个为新发现的区间。不同骨部位的小梁微结构在品系间具有相关性,且与这些小梁性状相关的大多数染色体区间在不同骨骼部位间共享。相反,股骨中小梁骨和皮质骨区之间没有共享染色体区间,尽管不同骨区在品系间有很强的相关性,这表明存在环境或内在因素的部位特异性调控。
结论
总之,这些数据证实,在获得骨峰值时存在明确的遗传决定因素来定义骨骼表型,并且骨形态的基因组调控对骨骼区域具有特异性。
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