Adenine base editing and prime editing of chemically derived hepatic progenitors rescue genetic liver disease

Yohan Kim; Sung Ah Hong; Jihyeon Yu; Jeongyun Eom; Kiseok Jang; Sangtae Yoon; Da Hee Hong; Daekwan Seo; Seu Na Lee; Jae Sung Woo; Jaemin Jeong; Sangsu Bae; Dongho Choi

doi:10.1016/j.stem.2021.04.010

Adenine base editing and prime editing of chemically derived hepatic progenitors rescue genetic liver disease

Yohan Kim
, Sung Ah Hong
, Jihyeon Yu
, Jeongyun Eom
, Kiseok Jang
, Sangtae Yoon
, Da Hee Hong
, Daekwan Seo
, Seu Na Lee
, Jae Sung Woo
, Jaemin Jeong
, Sangsu Bae
, Dongho Choi

Research output: Contribution to journal › Article › peer-review

57 Scopus citations

Abstract

DNA base editors and prime editing technology enable therapeutic in situ correction of disease-causing alleles. These techniques could have broad applications for ex vivo editing of cells prior to transplantation in a range of diseases, but it is critical that the target population is efficiently modified and engrafts into the host. Chemically derived hepatic progenitors (CdHs) are a multipotent population capable of robust engraftment and hepatocyte differentiation. Here we reprogrammed hepatocytes from a mouse model of hereditary tyrosinemia type 1 (HT1) into expandable CdHs and successfully corrected the disease-causing mutation using both adenine base editors (ABEs) and prime editors (PEs). ABE- and PE-corrected CdHs repopulated the liver with fumarylacetoacetate hydrolase-positive cells and dramatically increased survival of mutant HT1 mice. These results demonstrate the feasibility of precise gene editing in transplantable cell populations for potential treatment of genetic liver disease.

Original language	English
Pages (from-to)	1614-1624.e5
Journal	Cell Stem Cell
Volume	28
Issue number	9
DOIs	https://doi.org/10.1016/j.stem.2021.04.010
State	Published - 2 Sep 2021
Externally published	Yes

Keywords

adenine base editor
chemically derived hepatic progenitor
ex vivo gene editing therapy
genetic disorder
prime editing
regenerative medicine
reprogramming
tyrosinemia type 1

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10.1016/j.stem.2021.04.010

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title = "Adenine base editing and prime editing of chemically derived hepatic progenitors rescue genetic liver disease",

abstract = "DNA base editors and prime editing technology enable therapeutic in situ correction of disease-causing alleles. These techniques could have broad applications for ex vivo editing of cells prior to transplantation in a range of diseases, but it is critical that the target population is efficiently modified and engrafts into the host. Chemically derived hepatic progenitors (CdHs) are a multipotent population capable of robust engraftment and hepatocyte differentiation. Here we reprogrammed hepatocytes from a mouse model of hereditary tyrosinemia type 1 (HT1) into expandable CdHs and successfully corrected the disease-causing mutation using both adenine base editors (ABEs) and prime editors (PEs). ABE- and PE-corrected CdHs repopulated the liver with fumarylacetoacetate hydrolase-positive cells and dramatically increased survival of mutant HT1 mice. These results demonstrate the feasibility of precise gene editing in transplantable cell populations for potential treatment of genetic liver disease.",

keywords = "adenine base editor, chemically derived hepatic progenitor, ex vivo gene editing therapy, genetic disorder, prime editing, regenerative medicine, reprogramming, tyrosinemia type 1",

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doi = "10.1016/j.stem.2021.04.010",

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T1 - Adenine base editing and prime editing of chemically derived hepatic progenitors rescue genetic liver disease

AU - Kim, Yohan

AU - Hong, Sung Ah

AU - Yu, Jihyeon

AU - Eom, Jeongyun

AU - Jang, Kiseok

AU - Yoon, Sangtae

AU - Hong, Da Hee

AU - Seo, Daekwan

AU - Lee, Seu Na

AU - Woo, Jae Sung

AU - Jeong, Jaemin

AU - Bae, Sangsu

AU - Choi, Dongho

PY - 2021/9/2

Y1 - 2021/9/2

N2 - DNA base editors and prime editing technology enable therapeutic in situ correction of disease-causing alleles. These techniques could have broad applications for ex vivo editing of cells prior to transplantation in a range of diseases, but it is critical that the target population is efficiently modified and engrafts into the host. Chemically derived hepatic progenitors (CdHs) are a multipotent population capable of robust engraftment and hepatocyte differentiation. Here we reprogrammed hepatocytes from a mouse model of hereditary tyrosinemia type 1 (HT1) into expandable CdHs and successfully corrected the disease-causing mutation using both adenine base editors (ABEs) and prime editors (PEs). ABE- and PE-corrected CdHs repopulated the liver with fumarylacetoacetate hydrolase-positive cells and dramatically increased survival of mutant HT1 mice. These results demonstrate the feasibility of precise gene editing in transplantable cell populations for potential treatment of genetic liver disease.

AB - DNA base editors and prime editing technology enable therapeutic in situ correction of disease-causing alleles. These techniques could have broad applications for ex vivo editing of cells prior to transplantation in a range of diseases, but it is critical that the target population is efficiently modified and engrafts into the host. Chemically derived hepatic progenitors (CdHs) are a multipotent population capable of robust engraftment and hepatocyte differentiation. Here we reprogrammed hepatocytes from a mouse model of hereditary tyrosinemia type 1 (HT1) into expandable CdHs and successfully corrected the disease-causing mutation using both adenine base editors (ABEs) and prime editors (PEs). ABE- and PE-corrected CdHs repopulated the liver with fumarylacetoacetate hydrolase-positive cells and dramatically increased survival of mutant HT1 mice. These results demonstrate the feasibility of precise gene editing in transplantable cell populations for potential treatment of genetic liver disease.

KW - adenine base editor

KW - chemically derived hepatic progenitor

KW - ex vivo gene editing therapy

KW - genetic disorder

KW - prime editing

KW - regenerative medicine

KW - reprogramming

KW - tyrosinemia type 1

UR - https://www.scopus.com/pages/publications/85113727567

U2 - 10.1016/j.stem.2021.04.010

DO - 10.1016/j.stem.2021.04.010

M3 - Article

C2 - 33951479

AN - SCOPUS:85113727567

SN - 1934-5909

VL - 28

SP - 1614-1624.e5

JO - Cell Stem Cell

JF - Cell Stem Cell

IS - 9

ER -

Adenine base editing and prime editing of chemically derived hepatic progenitors rescue genetic liver disease

Abstract

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