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CRISPR–Cas9 mediated repression of BACE1 for amyloid-beta reduction in early-stage Alzheimer’s disease: A meta-analysis


Article Information

Title: CRISPR–Cas9 mediated repression of BACE1 for amyloid-beta reduction in early-stage Alzheimer’s disease: A meta-analysis

Authors: Atta Ur Rehman Khan, Safdar Manzoor, Muhammad Sarmad, Muhammad Rizwan Anwar

Journal: Pakistan Journal of Pathology

HEC Recognition History
Category From To
Y 2023-07-01 2024-09-30
Y 2022-07-01 2023-06-30
Y 2021-07-01 2022-06-30
Y 2020-07-01 2021-06-30
Y 1900-01-01 2005-06-30

Publisher: Pakistan Association of Pathologists

Country: Pakistan

Year: 2025

Volume: 36

Issue: 3

Language: en

DOI: 10.55629/pakjpathol.v36i3.942

Categories

Abstract

Objective: To assess the efficacy of CRISPR–Cas9-mediated repression of β-site amyloid precursor protein cleaving enzyme 1 (BACE1) in reducing amyloid-beta (Aβ) accumulation, neuropathological changes, and cognitive deficits in preclinical Alzheimer’s disease (AD) models.
Data Sources: A systematic search (2017–2024) was conducted in PubMed, Scopus, Web of Science, and Google Scholar, following PRISMA 2020 guidelines.
Study Selection: Ten preclinical studies using rodent or neuronal AD models with CRISPR–Cas9 or CRISPR interference targeting BACE1 were included.
Data Extraction: Extracted data included Aβ₄₀/₄₂ levels, BACE1 expression, plaque burden, neuronal integrity, neuroinflammation, and cognitive performance.
Data Synthesis: Meta-analysis (RevMan 5.4, STATA 17) showed significant reductions in Aβ₄₀/₄₂ (SMD = –1.45), BACE1 expression (SMD = –1.73), and plaque burden (SMD = –1.38). Qualitative findings indicated improved neuronal survival, reduced inflammation, and cognitive benefits.
Conclusions: CRISPR–Cas9 repression of BACE1 effectively attenuates amyloid pathology and supports cognitive improvements in preclinical AD models, underscoring its promise for translational CRISPR-based therapies.
Keywords: Alzheimer’s Disease, CRISPR, BACE1, Amyloid-beta, Meta-analysis, Gene editing.


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