公开(公告)号：WO2020264339A1

公开(公告)日：2020-12-30

申请号：PCT/US2020/039877

申请日：2020-06-26

Applicant: REGENERON PHARMACEUTICALS, INC.

Inventor： SHARMA-KANNING, Aarti ,  FRENDEWEY, David ,  ZAMBROWICZ, Brian

IPC: C07K14/47 ,  C12N15/113 ,  C12N15/85 ,  A01K2217/075 ,  A01K2217/077 ,  A01K2227/105 ,  A01K2267/0318 ,  A01K67/0276 ,  A61K49/0008 ,  C07K14/4703 ,  C12N15/11 ,  C12N15/8509 ,  C12N2015/8536 ,  C12N2310/11 ,  C12N2310/14 ,  C12N2310/141 ,  C12N2310/20 ,  C12N2310/341 ,  C12N2506/02 ,  C12N2510/00 ,  C12N5/0606 ,  C12N5/0619 ,  C12N9/22 ,  G01N2800/2835 ,  G01N33/5088 ,  G01N33/6896

Abstract: Described herein is the discovery that neither the nuclear localization signal (NLS) nor the prion-like domain (PLD) of TDP-43 is necessary for embryonic stem cell culture and differentiation into motor neurons in vitro. The ability of ES cells to express these TDP-43 mutants and differentiate into motor neurons that exhibit an ALS-like phenotype whereby the TDP-43 mutants redistribute to and aggregate in the cytoplasm and fail to regulate cryptic exon splicing allows these cells to act as a model of TDP-43 proteinopathy for the testing of candidate therapeutic agents that may resolve such proteinopathy. Additionally, these ES cells may be used to successfully generate non-human animals, e.g., mice, that also exhibit hallmark symptoms of ALS and that may be used in testing candidate agents useful in treating TDP-43 proteinopathies.

公开(公告)号：WO2022256290A2

公开(公告)日：2022-12-08

申请号：PCT/US2022/031519

申请日：2022-05-31

Applicant: ALNYLAM PHARMACEUTICALS, INC. ,  REGENERON PHARMACEUTICALS, INC. ,  DANG, Lan, Thi Hoang ,  MCININCH, James, D. ,  NGUYEN, Tuyen, M. ,  DUBOSE, Brittany

Inventor： FRENDEWEY, David ,  SHARMA-KANNING, Aarti

IPC: C12N15/113 ,  A61K31/713 ,  A61P25/28 ,  C12N2310/14 ,  C12N2310/3183 ,  C12N2310/321 ,  C12N2310/322 ,  C12N2310/351 ,  C12N2310/3515

Abstract: The disclosure relates to double stranded ribonucleic acid (dsRNAi) agents and compositions targeting a human chromosome 9 open reading frame 72 (C9orf72) gene, as well as methods of inhibiting expression of a C9orf72 gene and methods of treating subjects having a C9orf72-associated disease or disorder, e.g., C9orf72 amyotrophic lateral sclerosis, frontotemporal dementia or Huntington-Like Syndrome Due To C9orf72 Expansions, using such dsRNAi agents and compositions.

公开(公告)号：WO2021119226A1

公开(公告)日：2021-06-17

申请号：PCT/US2020/064159

申请日：2020-12-10

Applicant: ALNYLAM PHARMACEUTICALS, INC. ,  REGENERON PHARMACEUTICALS, INC.

Inventor： FISHILEVICH, Elane ,  MILSTEIN, Stuart ,  BROWN, Kirk ,  ZIMMERMANN, Tracy ,  MCININCH, James, D. ,  FRENDEWEY, David ,  CHIAO, Eric ,  SHARMA-KANNING, Aarti ,  GAGLIARDI, Anthony ,  DROGUETT, Gustavo ,  DUBOSE, Brittany ,  ZAMBROWICZ, Brian

IPC: C12N15/113 ,  A61K31/713 ,  A61P25/28

Abstract: The disclosure relates to double stranded ribonucleic acid (dsRNAi) agents and compositions targeting a human chromosome 9 open reading frame 72 (C9orf72) gene, as well as methods of inhibiting expression of a C9orf72 gene and methods of treating subjects having a C9orf72-associated disease or disorder, e.g., C9orf72 amyotrophic lateral sclerosis/frontotemporal dementia or Huntington-Like Syndrome Due To C9orf72 Expansions, using such dsRNAi agents and compositions.

公开(公告)号：WO2020264339A9

公开(公告)日：2020-12-30

申请号：PCT/US2020/039877

申请日：2020-06-26

Applicant: REGENERON PHARMACEUTICALS, INC.

Inventor： SHARMA-KANNING, Aarti ,  FRENDEWEY, David ,  ZAMBROWICZ, Brian

IPC: C07K14/47 ,  C12N15/113 ,  C12N15/85

Abstract: Described herein is the discovery that neither the nuclear localization signal (NLS) nor the prion-like domain (PLD) of TDP-43 is necessary for embryonic stem cell culture and differentiation into motor neurons in vitro . The ability of ES cells to express these TDP-43 mutants and differentiate into motor neurons that exhibit an ALS-like phenotype whereby the TDP-43 mutants redistribute to and aggregate in the cytoplasm and fail to regulate cryptic exon splicing allows these cells to act as a model of TDP-43 proteinopathy for the testing of candidate therapeutic agents that may resolve such proteinopathy. Additionally, these ES cells may be used to successfully generate non-human animals, e.g., mice, that also exhibit hallmark symptoms of ALS and that may be used in testing candidate agents useful in treating TDP-43 proteinopathies.

公开(公告)号：WO2020131632A1

公开(公告)日：2020-06-25

申请号：PCT/US2019/066317

申请日：2019-12-13

Applicant: REGENERON PHARMACEUTICALS, INC.

Inventor： KAJIMURA, Daisuke ,  SHARMA-KANNING, Aarti ,  DUBOSE, Brittany ,  DROGUETT, Gustavo ,  SIAO, Chia-Jen ,  KUNO, Junko ,  FRENDEWEY, David ,  ZAMBROWICZ, Brian

IPC: C12N15/10 ,  A01K67/027 ,  C12N15/11

Abstract: Nuclease-mediated methods for expanding repeats already present at a genomic locus are provided. Non-human animal genomes, non-human animal cells, and non-human animals comprising a heterologous hexanucleotide repeat expansion sequence inserted at an endogenous C9orf72 locus and methods of making such non-human animal cells and non-human animals through nuclease-mediated repeat expansion are also provided. Methods of using the non-human animal cells or non-human animals to identify therapeutic candidates that may be used to prevent, delay or treat one or more neurodegenerative disorders associated with repeat expansion at the C9orf72 locus are also provided.