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Published in:

01-08-2017

Metabolic Impact of Rapamycin (Sirolimus) and B-Estradiol Using Mouse Embryonic Fibroblasts as a Model for Lymphangioleiomyomatosis

Authors: Katherine M. Marsh, David Schipper, Alice S. Ferng, Kitsie Johnson, Julia Fisher, Shannon Knapp, Destiny Dicken, Zain Khalpey

Published in: Lung | Issue 4/2017

Abstract

Introduction

Lymphangioleiomyomatosis (LAM) is a rare, progressive cystic lung disease that predominantly affects women of childbearing age. Exogenous rapamycin (sirolimus) has been shown to improve clinical outcomes and was recently approved to treat LAM, whereas estrogen (E₂) is implicated in disease progression. No consistent metabolic model currently exists for LAM, therefore wild-type mouse embryonic fibroblasts (MEF +/+) and TSC2 knockout cells (MEF −/−) were used in this study as a model for LAM.

Methods

Oxygen consumption rates (OCR) and redox potential were measured to determine metabolic state across control cells, MEF +/+ and −/− cells treated with rapamycin (Rapa), and MEF +/+ and −/− cells treated with E₂. An XF96 extracellular flux analyzer from Seahorse Bioscience^® was used to measure OCR, and a RedoxSYS™ ORP was used to measure redox potential.

Results

OCR of MEF −/− cells treated with rapamycin (MEF −/− Rapa) versus MEF −/− control were significantly lower across all conditions. The static oxidation reduction potential of the MEF −/− Rapa group was also lower, approaching significance. The coupling efficiency and ratio of ATP-linked respiration to maximum respiration were statistically lower in MEF −/− Rapa compared to MEF +/+ Rapa. There were no significant metabolic findings across any of the MEF cells treated with E₂. MEF −/− control cells versus MEF +/+ control cells were not found to significantly differ.

Conclusion

MEF cells are thought to be a feasible metabolic model for LAM, which has implications for future pharmacologic and biologic testing.

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Title: Metabolic Impact of Rapamycin (Sirolimus) and B-Estradiol Using Mouse Embryonic Fibroblasts as a Model for Lymphangioleiomyomatosis
Authors: Katherine M. Marsh
David Schipper
Alice S. Ferng
Kitsie Johnson
Julia Fisher
Shannon Knapp
Destiny Dicken
Zain Khalpey
Publication date: 01-08-2017
Publisher: Springer US
Published in: Lung / Issue 4/2017
Print ISSN: 0341-2040
Electronic ISSN: 1432-1750
DOI: https://doi.org/10.1007/s00408-017-0016-3

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Abstract

Introduction

Methods

Results

Conclusion

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