Molecular Mechanisms of ARID5B-Mediated Genetic Susceptibility to Acute Lymphoblastic Leukemia.

Xujie Zhao Maoxiang Qian Charnise Goodings Yang Zhang Wenjian Yang Ping Wang Beisi Xu Cheng Tian Ching-Hon Pui Stephen P Hunger Elizabeth A Raetz Meenakshi Devidas Mary V Relling Mignon L Loh Daniel Savic Chunliang Li Jun J Yang

J Natl Cancer Inst

Department of Pharmaceutical Sciences, St. Jude Children's Research Hospital, Memphis, TN, USA.

Published: September 2022

There is a genetic link to childhood acute lymphoblastic leukemia (ALL), particularly involving non-coding variants at the ARID5B gene locus, which are linked to leukemia risk but have unclear functional effects.
Researchers analyzed the ARID5B gene in over 5,000 children with ALL and identified variants that could impact the gene's expression and susceptibility to leukemia, confirming their findings using advanced genomic techniques.
A highly significant risk variant (rs7090445) was found within an enhancer region that affects the binding of the transcription factor MEF2C, suggesting a crucial role for this mechanism in the development of ALL.

Background: There is growing evidence for the inherited basis of susceptibility to childhood acute lymphoblastic leukemia (ALL). Genome-wide association studies have identified non-coding ALL risk variants at the ARID5B gene locus, but their exact functional effects and the molecular mechanism linking ARID5B to B-cell ALL leukemogenesis remain largely unknown.

Methods: We performed targeted sequencing of ARID5B in germline DNA of 5008 children with ALL. Variants were evaluated for association with ALL susceptibility using 3644 patients from the UK10K cohort as non-ALL controls, under an additive model. Cis-regulatory elements in ARID5B were systematically identified using dCas9-KRAB-mediated enhancer interference system enhancer screen in ALL cells. Disruption of transcription factor binding by ARID5B variant was predicted informatically and then confirmed using chromatin immunoprecipitation and coimmunoprecipitation. ARID5B variant association with hematological traits was examined using UK Biobank dataset. All statistical tests were 2-sided.

Results: We identified 54 common variants in ARID5B statistically significantly associated with leukemia risk, all of which were noncoding. Six cis-regulatory elements at the ARID5B locus were discovered using CRISPR-based high-throughput enhancer screening. Strikingly, the top ALL risk variant (rs7090445, P = 5.57 × 10-45) is located precisely within the strongest enhancer element, which is also distally tethered to the ARID5B promoter. The variant allele disrupts the MEF2C binding motif sequence, resulting in reduced MEF2C affinity and decreased local chromosome accessibility. MEF2C influences ARID5B expression in ALL, likely via a transcription factor complex with RUNX1. Using the UK Biobank dataset (n = 349 861), we showed that rs7090445 was also associated with lymphocyte percentage and count in the general population (P = 8.6 × 10-22 and 2.1 × 10-18, respectively).

Conclusions: Our results indicate that ALL risk variants in ARID5B function by modulating cis-regulatory elements at this locus.

Download full-text PDF	Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9468286	PMC
http://dx.doi.org/10.1093/jnci/djac101	DOI Listing

Publication Analysis

Top Keywords

variants arid5b

cis-regulatory elements

arid5b

acute lymphoblastic

lymphoblastic leukemia

risk variants

elements arid5b

transcription factor

arid5b variant

biobank dataset

Similar Publications

Want AI Summaries of new PubMed Abstracts delivered to your In-box?

Enter search terms and have AI summaries delivered each week - change queries or unsubscribe any time!