Jake M. Bieber
University of California, San Francisco
4 Papers
Jake M. Bieber is an academic researcher from University of California, San Francisco. The author has contributed to research in topics: Progenitor cell & LGR5. The author has an hindex of 2, co-authored 4 publications. Previous affiliations of Jake M. Bieber include University of California, Berkeley.
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Papers
Transit-Amplifying Cells Coordinate Changes in Intestinal Epithelial Cell-Type Composition.
Laura E. Sanman,Ina W. Chen,Jake M. Bieber,Veronica Steri,Coralie Trentesaux,Byron Hann,Ophir D. Klein,Lani F. Wu,Steven J. Altschuler +8 more
TL;DR: The authors investigated the responses of intestinal epithelium to individual and paired perturbations across eight epithelial signaling pathways and found that modulation of transit-amplifying cell proliferation changes the ratio of differentiated secretory to absorptive cell types.
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Transit-amplifying cells coordinate changes in intestinal epithelial cell-type composition
Laura E. Sanman,Ina W. Chen,Jake M. Bieber,Veronica Steri,Byron Hann,Lani F. Wu,Steven J. Altschuler +6 more
TL;DR: An underappreciated role for transit-amplifying cells is highlighted in which proliferation of these short-lived progenitors provides a lineage-based mechanism for tuning differentiated cell-type composition.
Generation and Quantitative Imaging of Enteroid Monolayers.
Laura E. Sanman,Ina W. Chen,Jake M. Bieber,Jake M. Bieber,Curtis A. Thorne,Lani F. Wu,Steven J. Altschuler +6 more
TL;DR: An enteroid monolayer (2D) culture system that recapitulates important features of 3D organoids and the in vivo intestinal epithelium such as tissue renewal, representation of diverse epithelial cell types, self-organization, and apical-basolateral polarization is developed.
Non-stem progenitors enable coordinated changes in gut epithelial cell-type composition
Laura E. Sanman,Ina W. Chen,Jake M. Bieber,Jake M. Bieber,Veronica Steri,Byron Hann,Lani F. Wu,Steven J. Altschuler +7 more
TL;DR: It is found that changes in proliferation of transit-amplifying (TA) cells, but not Lgr5+ stem cells, alters the composition of mature secretory and absorptive cell-types in organoids and in vivo.