Your search keyword '"Schreiber, Katherine A."' showing total 2 results

1. Rapamycin-mediated mTORC2 inhibition is determined by the relative expression of FK506-binding proteins.

Author

Schreiber, Katherine H., Ortiz, Denise, Academia, Emmeline C., Anies, Arieanna C., Liao, Chen‐Yu, and Kennedy, Brian K.

Subjects

*TOR proteins, *CELLULAR aging, *GENE expression, *CARRIER proteins, *TACROLIMUS, *DRUG administration

Abstract

The mechanism by which the drug rapamycin inhibits the mechanistic target of rapamycin ( mTOR) is of intense interest because of its likely relevance in cancer biology, aging, and other age-related diseases. While rapamycin acutely and directly inhibits mTORC1, only chronic administration of rapamycin can inhibit mTORC2 in some, but not all, cell lines or tissues. The mechanism leading to cell specificity of mTORC2 inhibition by rapamycin is not understood and is especially important because many of the negative metabolic side effects of rapamycin, reported in mouse studies and human clinical trials, have been attributed recently to mTORC2 inhibition. Here, we identify the expression level of different FK506-binding proteins (FKBPs), primarily FKBP12 and FKBP51, as the key determinants for rapamycin-mediated inhibition of mTORC2. In support, enforced reduction of FKBP12 completely converts a cell line that is sensitive to mTORC2 inhibition to an insensitive cell line, and increased expression can enhance mTORC2 inhibition. Further reduction of FKBP12 in cell lines with already low FKBP12 levels completely blocks mTORC1 inhibition by rapamycin, indicating that relative FKBP12 levels are critical for both mTORC1 and mTORC2 inhibition, but at different levels. In contrast, reduction of FKBP51 renders cells more sensitive to mTORC2 inhibition. Our findings reveal that the expression of FKBP12 and FKBP51 is the rate limiting factor that determines the responsiveness of a cell line or tissue to rapamycin. These findings have implications for treating specific diseases, including neurodegeneration and cancer, as well as targeting aging in general. [ABSTRACT FROM AUTHOR]

Published

2015

2. The Ribosomal Protein Rpl22 Controls Ribosome Composition by Directly Repressing Expression of Its Own Paralog, Rpl22l1.

Author

O'Leary, Monique N., Schreiber, Katherine H., Zhang, Yong, Duc, Anne-Cécile E., Rao, Shuyun, Hale, J. Scott, Academia, Emmeline C., Shah, Shreya R., Morton, John F., Holstein, Carly A., Martin, Dan B., Kaeberlein, Matt, Ladiges, Warren C., Fink, Pamela J., MacKay, Vivian L., Wiest, David L., and Kennedy, Brian K.

Subjects

*RIBOSOMES, *PHENOTYPES, *PROTEIN research, *GENE expression, *PROTEIN binding

Abstract

Most yeast ribosomal protein genes are duplicated and their characterization has led to hypotheses regarding the existence of specialized ribosomes with different subunit composition or specifically-tailored functions. In yeast, ribosomal protein genes are generally duplicated and evidence has emerged that paralogs might have specific roles. Unlike yeast, most mammalian ribosomal proteins are thought to be encoded by a single gene copy, raising the possibility that heterogenous populations of ribosomes are unique to yeast. Here, we examine the roles of the mammalian Rpl22, finding that Rpl22−/− mice have only subtle phenotypes with no significant translation defects. We find that in the Rpl22−/− mouse there is a compensatory increase in Rpl22-like1 (Rpl22l1) expression and incorporation into ribosomes. Consistent with the hypothesis that either ribosomal protein can support translation, knockdown of Rpl22l1 impairs growth of cells lacking Rpl22. Mechanistically, Rpl22 regulates Rpl22l1 directly by binding to an internal hairpin structure and repressing its expression. We propose that ribosome specificity may exist in mammals, providing evidence that one ribosomal protein can influence composition of the ribosome by regulating its own paralog. [ABSTRACT FROM AUTHOR]

Published

2013