Your search keyword '"Kivanç Birsoy"' showing total 3 results

1. Limitation of adipose tissue by the number of embryonic progenitor cells

Author

Kristina Hedbacker, Yi-Hsueh Lu, Olof Dallner, Zhiying Li, Gulya Fayzikhodjaeva, Kıvanç Birsoy, Chiayun Han, Chingwen Yang, and Jeffrey M Friedman

Subjects

adipose tissue, obesity, metabolic syndrome, metabolism, lipodystrophy, leptin, Medicine, Science, Biology (General), QH301-705.5

Abstract

Adipogenesis in adulthood replaces fat cells that turn over and can contribute to the development of obesity. However, the proliferative potential of adipocyte progenitors in vivo is unknown (Faust et al., 1976; Faust et al., 1977; Hirsch and Han, 1969; Johnson and Hirsch, 1972). We addressed this by injecting labeled wild-type embryonic stem cells into blastocysts derived from lipodystrophic A-ZIP transgenic mice, which have a genetic block in adipogenesis. In the resulting chimeric animals, wild-type ES cells are the only source of mature adipocytes. We found that when chimeric animals were fed a high-fat-diet, animals with low levels of chimerism showed a significantly lower adipose tissue mass than animals with high levels of chimerism. The difference in adipose tissue mass was attributed to variability in the amount of subcutaneous adipose tissue as the amount of visceral fat was independent of the level of chimerism. Our findings thus suggest that proliferative potential of adipocyte precursors is limited and can restrain the development of obesity.

Published

2020

2. The anticancer natural product ophiobolin A induces cytotoxicity by covalent modification of phosphatidylethanolamine

Author

Christopher Chidley, Sunia A Trauger, Kıvanç Birsoy, and Erin K O'Shea

Subjects

chemical biology, mechanism of action, cytotoxicity, covalent modification, drug development, genetic screen, Medicine, Science, Biology (General), QH301-705.5

Abstract

Phenotypic screens allow the identification of small molecules with promising anticancer activity, but the difficulty in characterizing the mechanism of action of these compounds in human cells often undermines their value as drug leads. Here, we used a loss-of-function genetic screen in human haploid KBM7 cells to discover the mechanism of action of the anticancer natural product ophiobolin A (OPA). We found that genetic inactivation of de novo synthesis of phosphatidylethanolamine (PE) mitigates OPA cytotoxicity by reducing cellular PE levels. OPA reacts with the ethanolamine head group of PE in human cells to form pyrrole-containing covalent cytotoxic adducts and these adducts lead to lipid bilayer destabilization. Our characterization of this unusual cytotoxicity mechanism, made possible by unbiased genetic screening in human cells, suggests that the selective antitumor activity displayed by OPA may be due to altered membrane PE levels in cancer cells.

Published

2016

3. A critical role for mTORC1 in erythropoiesis and anemia

Author

Zachary A Knight, Sarah F Schmidt, Kivanc Birsoy, Keith Tan, and Jeffrey M Friedman

Subjects

mTOR, mTORC1, anemia, erythropoiesis, RBC, Medicine, Science, Biology (General), QH301-705.5

Abstract

Red blood cells (RBC) must coordinate their rate of growth and proliferation with the availability of nutrients, such as iron, but the signaling mechanisms that link the nutritional state to RBC growth are incompletely understood. We performed a screen for cell types that have high levels of signaling through mTORC1, a protein kinase that couples nutrient availability to cell growth. This screen revealed that reticulocytes show high levels of phosphorylated ribosomal protein S6, a downstream target of mTORC1. We found that mTORC1 activity in RBCs is regulated by dietary iron and that genetic activation or inhibition of mTORC1 results in macrocytic or microcytic anemia, respectively. Finally, ATP competitive mTOR inhibitors reduced RBC proliferation and were lethal after treatment with phenylhydrazine, an inducer of hemolysis. These results identify the mTORC1 pathway as a critical regulator of RBC growth and proliferation and establish that perturbations in this pathway result in anemia.

Published

2014