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Single-cell transcriptomic analysis of adult mouse pituitary reveals sexual dimorphism and physiologic demand-induced cellular plasticity
Yugong Ho, Peng Hu, Michael T. Peel, Sixing Chen, Pablo G. Camara, Douglas J. Epstein, Hao Wu, Stephen A. Liebhaber
Protein Cell. 2020, 11 (8): 565-583.
https://doi.org/10.1007/s13238-020-00705-x
The anterior pituitary gland drives highly conserved physiologic processes in mammalian species. These hormonally controlled processes are central to somatic growth, pubertal transformation, fertility, lactation, and metabolism. Current cellular models of mammalian anteiror pituitary, largely built on candidate gene based immuno-histochemical and mRNA analyses, suggest that each of the seven hormones synthesized by the pituitary is produced by a specific and exclusive cell lineage. However, emerging evidence suggests more complex relationship between hormone specificity and cell plasticity. Here we have applied massively parallel single-cell RNA sequencing (scRNA-seq), in conjunction with complementary imaging-based single-cell analyses of mRNAs and proteins, to systematically map both cell-type diversity and functional state heterogeneity in adult male and female mouse pituitaries at single-cell resolution and in the context of major physiologic demands. These quantitative single-cell analyses reveal sex-specific cell-type composition under normal pituitary homeostasis, identify an array of cells associated with complex complements of hormone-enrichment, and undercover non-hormone producing interstitial and supporting cell-types. Interestingly, we also identified a Pou1f1-expressing cell population that is characterized by a unique multi-hormone gene expression profile. In response to two well-defined physiologic stresses, dynamic shifts in cellular diversity and transcriptome profiles were observed for major hormone producing and the putative multi-hormone cells. These studies reveal unanticipated cellular complexity and plasticity in adult pituitary, and provide a rich resource for further validating and expanding our molecular understanding of pituitary gene expression programs and hormone production.
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Crystal structure of the African swine fever virus structural protein p35 reveals its role for core shell assembly
Guobang Li, Dan Fu, Guangshun Zhang, Dongming Zhao, Mingyu Li, Xue Geng, Dongdong Sun, Yuhui Wang, Cheng Chen, Peng Jiao, Lin Cao, Yu Guo, Zihe Rao
Protein Cell. 2020, 11 (8): 600-605.
https://doi.org/10.1007/s13238-020-00730-w
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Structure of African swine fever virus p15 reveals its dual role for membrane-association and DNA binding
Dan Fu, Dongming Zhao, Wei Zhang, Guangshun Zhang, Mingyu Li, Zheng Zhang, Yuhui Wang, Dongdong Sun, Peng Jiao, Cheng Chen, Yu Guo, Zihe Rao
Protein Cell. 2020, 11 (8): 606-612.
https://doi.org/10.1007/s13238-020-00731-9
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Broad spectrum antibiotic-degrading metallo-β-lactamases are phylogenetically diverse
Marcelo Monteiro Pedroso, David W. Waite, Okke Melse, Liam Wilson, Nataša Mitić, Ross P. McGeary, Iris Antes, Luke W. Guddat, Philip Hugenholtz, Gerhard Schenk
Protein Cell. 2020, 11 (8): 613-617.
https://doi.org/10.1007/s13238-020-00736-4
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Correction to: EGFR signaling augments TLR4 cell surface expression and function in macrophages via regulation of Rab5a activation
Jing Tang, Bowei Zhou, Melanie J. Scott, Linsong Chen, Dengming Lai, Erica K. Fan, Yuehua Li, Qiang Wu, Timothy R. Billiar, Mark A. Wilson, Ping Wang, Jie Fan
Protein Cell. 2020, 11 (8): 618-619.
https://doi.org/10.1007/s13238-019-00679-5
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8 articles
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