Comparative analysis of two independent Myh6-Cre transgenic mouse lines

Amanda Davenport; Chase W. Kessinger; Ryan D. Pfeiffer; Nikita Shah; Richard Xu; E. Dale Abel; Nathan R. Tucker; Zhiqiang Lin

Journal of Molecular and Cellular Cardiology Plus (Sep 2024)

Comparative analysis of two independent Myh6-Cre transgenic mouse lines

Amanda Davenport,
Chase W. Kessinger,
Ryan D. Pfeiffer,
Nikita Shah,
Richard Xu,
E. Dale Abel,
Nathan R. Tucker,
Zhiqiang Lin

Affiliations

Amanda Davenport: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America
Chase W. Kessinger: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America
Ryan D. Pfeiffer: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America
Nikita Shah: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America; College of Arts and Sciences, SUNY Polytechnic Institute, Utica, NY 13502, United States of America
Richard Xu: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America
E. Dale Abel: Department of Medicine David Geffen School of Medicine and UCLA Health, United States of America
Nathan R. Tucker: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America
Zhiqiang Lin: Department of Biomedical Research and Translational Medicine, Masonic Medical Research Institute, 2150 Bleecker Street, Utica, NY 13501, United States of America; Corresponding author.

Journal volume & issue: Vol. 9
p. 100081

Abstract

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We have previously shown that the Myh6 promoter drives Cre expression in a subset of male germ line cells in three independent Myh6-Cre mouse lines, including two transgenic lines and one knock-in allele. In this study, we further compared the tissue-specificity of the two Myh6-Cre transgenic mouse lines, MDS Myh6-Cre and AUTR Myh6-Cre, through examining the expression of tdTomato (tdTom) red fluorescence protein in multiple internal organs, including the heart, brain, liver, lung, pancreas and brown adipose tissue. Our results show that MDS Myh6-Cre mainly activates tdTom reporter in the heart, whereas AUTR Myh6-Cre activates tdTom expression significantly in the heart, and in the cells of liver, pancreas and brain. In the heart, similar to MDS Myh6-Cre, AUTR Myh6-Cre activates tdTom in most cardiomyocytes. In the other organs, AUTR Myh6-Cre not only mosaically activates tdTom in some parenchymal cells, such as hepatocytes in the liver and neurons in the brain, but also turns on tdTom in some interstitial cells of unknown identity.

Published in Journal of Molecular and Cellular Cardiology Plus

ISSN: 2772-9761 (Online)
Publisher: Elsevier
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the circulatory (Cardiovascular) system
Website: https://www.sciencedirect.com/journal/journal-of-molecular-and-cellular-cardiology-plus

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