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A translational kidney organoid system bolsters human relevance of clinical development candidate

Amy Westerling-Bui, Thomas W. Soare, Srinivasan Venkatachalan, Michael DeRan, Eva Maria Fast, Alyssa B. Fanelli, Sergii Kyrychenko, Hien Hoang, Grinal M. Corriea, Wei Zhang, Maolin Yu, Matthew Daniels, Goran Malojcic, Xin-Ru Pan-Zhou, Mark W. Ledeboer, Jean-Christophe Harmange, Maheswarareddy Emani, Thomas T. Tibbitts, John F. Reilly, Peter Mundel
doi: https://doi.org/10.1101/2019.12.30.891440
Amy Westerling-Bui
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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  • For correspondence: abui@goldfinchbio.com jreilly@goldfinchbio.com pmundel@goldfinchbio.com
Thomas W. Soare
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Srinivasan Venkatachalan
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Michael DeRan
2Diamond Age Data Science, Somerville, MA 02143, USA
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Eva Maria Fast
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Alyssa B. Fanelli
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Sergii Kyrychenko
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Hien Hoang
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Grinal M. Corriea
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Wei Zhang
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Maolin Yu
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Matthew Daniels
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Goran Malojcic
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Xin-Ru Pan-Zhou
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Mark W. Ledeboer
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Jean-Christophe Harmange
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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Maheswarareddy Emani
3Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA
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Thomas T. Tibbitts
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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John F. Reilly
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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  • For correspondence: abui@goldfinchbio.com jreilly@goldfinchbio.com pmundel@goldfinchbio.com
Peter Mundel
1Goldfinch Bio, Inc., Cambridge, MA, 02142, USA
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  • For correspondence: abui@goldfinchbio.com jreilly@goldfinchbio.com pmundel@goldfinchbio.com
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Abstract

A major challenge in drug discovery is gaining confidence in the human relevance of pre-clinical animal studies. While human iPSC-derived organoids offer exciting opportunities to address this, concerns about applicability and scalability remain. Here, we report a high-throughput organoid platform for assessment of kidney disease targeting compounds in a human system. We confirmed platform reproducibility by single cell RNA-Seq (scRNA-Seq) and derived a NanoString panel for efficient quality control (QC). Organoid transplantation in rats for 2 to 4 weeks promoted organoid maturation and vascularization. In functional studies, cyclosporine A (CsA) and GFB-887, a novel TRPC5 channel blocker, protected kidney organoids from injury. Pharmacodynamic studies with GFB-887 delivered orally to rats were also successfully performed in human transplanted organoids. These data show how human organoids can deliver confidence in taking development candidate compounds to the clinic, fulfilling their promise to revolutionize drug discovery.

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Posted December 31, 2019.
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A translational kidney organoid system bolsters human relevance of clinical development candidate
Amy Westerling-Bui, Thomas W. Soare, Srinivasan Venkatachalan, Michael DeRan, Eva Maria Fast, Alyssa B. Fanelli, Sergii Kyrychenko, Hien Hoang, Grinal M. Corriea, Wei Zhang, Maolin Yu, Matthew Daniels, Goran Malojcic, Xin-Ru Pan-Zhou, Mark W. Ledeboer, Jean-Christophe Harmange, Maheswarareddy Emani, Thomas T. Tibbitts, John F. Reilly, Peter Mundel
bioRxiv 2019.12.30.891440; doi: https://doi.org/10.1101/2019.12.30.891440
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A translational kidney organoid system bolsters human relevance of clinical development candidate
Amy Westerling-Bui, Thomas W. Soare, Srinivasan Venkatachalan, Michael DeRan, Eva Maria Fast, Alyssa B. Fanelli, Sergii Kyrychenko, Hien Hoang, Grinal M. Corriea, Wei Zhang, Maolin Yu, Matthew Daniels, Goran Malojcic, Xin-Ru Pan-Zhou, Mark W. Ledeboer, Jean-Christophe Harmange, Maheswarareddy Emani, Thomas T. Tibbitts, John F. Reilly, Peter Mundel
bioRxiv 2019.12.30.891440; doi: https://doi.org/10.1101/2019.12.30.891440

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