CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease

BACKGROUND: Cholinergic neuronal loss is one of the hallmarks of AD related neurodegeneration; however, preclinical promise of α7 nAChR drugs failed to translate into humans. CHRFAM7A, a uniquely human fusion gene, is a negative regulator of α7 nAChR and was unaccounted for in preclinical models. ME...

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Autores principales: Szigeti, Kinga, Ihnatovych, Ivanna, Birkaya, Barbara, Chen, Ziqiang, Ouf, Aya, Indurthi, Dinesh C., Bard, Jonathan E., Kann, Julien, Adams, Alexandrea, Chaves, Lee, Sule, Norbert, Reisch, Joan S., Pavlik, Valory, Benedict, Ralph H.B., Auerbach, Anthony, Wilding, Gregory
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Research paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7452451/
https://www.ncbi.nlm.nih.gov/pubmed/32818803
http://dx.doi.org/10.1016/j.ebiom.2020.102892
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author Szigeti, Kinga
Ihnatovych, Ivanna
Birkaya, Barbara
Chen, Ziqiang
Ouf, Aya
Indurthi, Dinesh C.
Bard, Jonathan E.
Kann, Julien
Adams, Alexandrea
Chaves, Lee
Sule, Norbert
Reisch, Joan S.
Pavlik, Valory
Benedict, Ralph H.B.
Auerbach, Anthony
Wilding, Gregory
author_facet Szigeti, Kinga
Ihnatovych, Ivanna
Birkaya, Barbara
Chen, Ziqiang
Ouf, Aya
Indurthi, Dinesh C.
Bard, Jonathan E.
Kann, Julien
Adams, Alexandrea
Chaves, Lee
Sule, Norbert
Reisch, Joan S.
Pavlik, Valory
Benedict, Ralph H.B.
Auerbach, Anthony
Wilding, Gregory
author_sort Szigeti, Kinga
collection PubMed
description BACKGROUND: Cholinergic neuronal loss is one of the hallmarks of AD related neurodegeneration; however, preclinical promise of α7 nAChR drugs failed to translate into humans. CHRFAM7A, a uniquely human fusion gene, is a negative regulator of α7 nAChR and was unaccounted for in preclinical models. METHODS: Molecular methods: Function of CHRFAM7A alleles was studied in vitro in two disease relevant phenotypic readouts: electrophysiology and Aβ uptake. Genome edited human induced pluripotent stem cells (iPSC) were used as a model system with the human context. Double blind pharmacogenetic study: We performed double-blind pharmacogenetic analysis on the effect of AChEI therapy based on CHRFAM7A carrier status in two paradigms: response to drug initiation and DMT effect. Mini Mental Status Examination (MMSE) was used as outcome measure. Change in MMSE score from baseline was compared by 2-tailed T-test. Longitudinal analysis of clinical outcome (MMSE) was performed using a fitted general linear model, based on an assumed autoregressive covariance structure. Model independent variables included age, sex, and medication regimen at the time of the first utilized outcome measure (AChEI alone or AChEI plus memantine), APOE4 carrier status (0, 1 or 2 alleles as categorical variables) and CHRFAM7A genotype. FINDINGS: The direct and inverted alleles have distinct phenotypes. Functional CHRFAM7A allele classifies the population as 25% non-carriers and 75% carriers. Induced pluripotent stem cell (iPSC) models α7 nAChR mediated Aβ neurotoxicity. Pharmacological readout translates into both first exposure (p = 0.037) and disease modifying effect (p = 0.0048) in two double blind pharmacogenetic studies. INTERPRETATION: CHRFAM7A accounts for the translational gap in cholinergic strategies in AD. Clinical trials not accounting for this uniquely human genetic factor may have rejected drug candidates that would benefit 25% of AD. Reanalyses of the completed trials using this pharmacogenetic paradigm may identify effective therapy. Funding:
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spelling pubmed-74524512020-09-03 CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease Szigeti, Kinga Ihnatovych, Ivanna Birkaya, Barbara Chen, Ziqiang Ouf, Aya Indurthi, Dinesh C. Bard, Jonathan E. Kann, Julien Adams, Alexandrea Chaves, Lee Sule, Norbert Reisch, Joan S. Pavlik, Valory Benedict, Ralph H.B. Auerbach, Anthony Wilding, Gregory EBioMedicine Research paper BACKGROUND: Cholinergic neuronal loss is one of the hallmarks of AD related neurodegeneration; however, preclinical promise of α7 nAChR drugs failed to translate into humans. CHRFAM7A, a uniquely human fusion gene, is a negative regulator of α7 nAChR and was unaccounted for in preclinical models. METHODS: Molecular methods: Function of CHRFAM7A alleles was studied in vitro in two disease relevant phenotypic readouts: electrophysiology and Aβ uptake. Genome edited human induced pluripotent stem cells (iPSC) were used as a model system with the human context. Double blind pharmacogenetic study: We performed double-blind pharmacogenetic analysis on the effect of AChEI therapy based on CHRFAM7A carrier status in two paradigms: response to drug initiation and DMT effect. Mini Mental Status Examination (MMSE) was used as outcome measure. Change in MMSE score from baseline was compared by 2-tailed T-test. Longitudinal analysis of clinical outcome (MMSE) was performed using a fitted general linear model, based on an assumed autoregressive covariance structure. Model independent variables included age, sex, and medication regimen at the time of the first utilized outcome measure (AChEI alone or AChEI plus memantine), APOE4 carrier status (0, 1 or 2 alleles as categorical variables) and CHRFAM7A genotype. FINDINGS: The direct and inverted alleles have distinct phenotypes. Functional CHRFAM7A allele classifies the population as 25% non-carriers and 75% carriers. Induced pluripotent stem cell (iPSC) models α7 nAChR mediated Aβ neurotoxicity. Pharmacological readout translates into both first exposure (p = 0.037) and disease modifying effect (p = 0.0048) in two double blind pharmacogenetic studies. INTERPRETATION: CHRFAM7A accounts for the translational gap in cholinergic strategies in AD. Clinical trials not accounting for this uniquely human genetic factor may have rejected drug candidates that would benefit 25% of AD. Reanalyses of the completed trials using this pharmacogenetic paradigm may identify effective therapy. Funding: Elsevier 2020-08-17 /pmc/articles/PMC7452451/ /pubmed/32818803 http://dx.doi.org/10.1016/j.ebiom.2020.102892 Text en © 2020 The Author(s) http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research paper
Szigeti, Kinga
Ihnatovych, Ivanna
Birkaya, Barbara
Chen, Ziqiang
Ouf, Aya
Indurthi, Dinesh C.
Bard, Jonathan E.
Kann, Julien
Adams, Alexandrea
Chaves, Lee
Sule, Norbert
Reisch, Joan S.
Pavlik, Valory
Benedict, Ralph H.B.
Auerbach, Anthony
Wilding, Gregory
CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title_full CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title_fullStr CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title_full_unstemmed CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title_short CHRFAM7A: A human specific fusion gene, accounts for the translational gap for cholinergic strategies in Alzheimer's disease
title_sort chrfam7a: a human specific fusion gene, accounts for the translational gap for cholinergic strategies in alzheimer's disease
topic Research paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7452451/
https://www.ncbi.nlm.nih.gov/pubmed/32818803
http://dx.doi.org/10.1016/j.ebiom.2020.102892
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