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Lin28a transgenic mice manifest size and puberty phenotypes identified in human genetic association studies.

Nature genetics (2010-06-01)
Hao Zhu, Samar Shah, Ng Shyh-Chang, Gen Shinoda, William S Einhorn, Srinivas R Viswanathan, Ayumu Takeuchi, Corinna Grasemann, John L Rinn, Mary F Lopez, Joel N Hirschhorn, Mark R Palmert, George Q Daley
RESUMEN

Recently, genome-wide association studies have implicated the human LIN28B locus in regulating height and the timing of menarche. LIN28B and its homolog LIN28A are functionally redundant RNA-binding proteins that block biogenesis of let-7 microRNAs. lin-28 and let-7 were discovered in Caenorhabditis elegans as heterochronic regulators of larval and vulval development but have recently been implicated in cancer, stem cell aging and pluripotency. The let-7 targets Myc, Kras, Igf2bp1 and Hmga2 are known regulators of mammalian body size and metabolism. To explore the function of the Lin28-Let-7 pathway in vivo, we engineered transgenic mice to express Lin28a and observed in them increased body size, crown-rump length and delayed onset of puberty. Investigation of metabolic and endocrine mechanisms of overgrowth in these transgenic mice revealed increased glucose metabolism and insulin sensitivity. Here we report a mouse that models the human phenotypes associated with genetic variation in the Lin28-Let-7 pathway.

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MISSION® esiRNA, targeting mouse Lin28a