TY - JOUR
T1 - Best Disease
T2 - Global Mutations Review, Genotype–Phenotype Correlation, and Prevalence Analysis in the Israeli Population
AU - Beryozkin, Avigail
AU - Sher, Ifat
AU - Ehrenberg, Miriam
AU - Zur, Dinah
AU - Newman, Hadas
AU - Gradstein, Libe
AU - Simaan, Francis
AU - Rotenstreich, Ygal
AU - Goldenberg-Cohen, Nitza
AU - Bahar, Irit
AU - Blumenfeld, Anat
AU - Rivera, Antonio
AU - Rosin, Boris
AU - Deitch-Harel, Iris
AU - Perlman, Ido
AU - Mechoulam, Hadas
AU - Chowers, Itay
AU - Leibu, Rina
AU - Ben-Yosef, Tamar
AU - Pras, Eran
AU - Banin, Eyal
AU - Sharon, Dror
AU - Khateb, Samer
N1 - Publisher Copyright:
© 2024 The Authors.
PY - 2024/2
Y1 - 2024/2
N2 - PURPOSE. To review all reported disease-causing mutations in BEST1, perform genotype–phenotype correlation, and estimate disease prevalence in the Israeli population. METHODS. Medical records of patients diagnosed with Best disease and allied diseases from nine Israeli medical centers over the past 20 years were collected, as were clinical data including ocular findings, electrophysiology results, and retina imaging. Mutation detection involved mainly whole exome sequencing and candidate gene analysis. Demographic data were obtained from the Israeli Bureau of Statistics (January 2023). A bibliometric study was also conducted to gather mutation data from online sources. RESULTS. A total of 134 patients were clinically diagnosed with Best disease and related conditions. The estimated prevalence of Best disease was calculated to be 1 in 127,000, with higher rates among Arab Muslims (1 in 76,000) than Jews (1 in 145,000). Genetic causes were identified in 76 individuals (57%), primarily showing autosomal-dominant inheritance due to BEST1 mutations (58 patients). Critical conserved domains were identified consisting of a high percentage of dominant missense mutations, primarily in transmembrane domains and the intracellular region (Ca2+ binding domain) of the BEST1 protein. CONCLUSIONS. This study represents the largest cohort of patients with Best disease reported in Israel and globally. The prevalence in Israel is akin to that in Denmark but is lower than that in the United States. Critical conserved domains within the BEST1 protein are pivotal for normal functioning, and even minor missense alterations in these areas lead to a dominant disease manifestation. Genetic testing is indispensable as the gold standard for Best disease diagnosis due to the variable clinical presentation of the disease.
AB - PURPOSE. To review all reported disease-causing mutations in BEST1, perform genotype–phenotype correlation, and estimate disease prevalence in the Israeli population. METHODS. Medical records of patients diagnosed with Best disease and allied diseases from nine Israeli medical centers over the past 20 years were collected, as were clinical data including ocular findings, electrophysiology results, and retina imaging. Mutation detection involved mainly whole exome sequencing and candidate gene analysis. Demographic data were obtained from the Israeli Bureau of Statistics (January 2023). A bibliometric study was also conducted to gather mutation data from online sources. RESULTS. A total of 134 patients were clinically diagnosed with Best disease and related conditions. The estimated prevalence of Best disease was calculated to be 1 in 127,000, with higher rates among Arab Muslims (1 in 76,000) than Jews (1 in 145,000). Genetic causes were identified in 76 individuals (57%), primarily showing autosomal-dominant inheritance due to BEST1 mutations (58 patients). Critical conserved domains were identified consisting of a high percentage of dominant missense mutations, primarily in transmembrane domains and the intracellular region (Ca2+ binding domain) of the BEST1 protein. CONCLUSIONS. This study represents the largest cohort of patients with Best disease reported in Israel and globally. The prevalence in Israel is akin to that in Denmark but is lower than that in the United States. Critical conserved domains within the BEST1 protein are pivotal for normal functioning, and even minor missense alterations in these areas lead to a dominant disease manifestation. Genetic testing is indispensable as the gold standard for Best disease diagnosis due to the variable clinical presentation of the disease.
KW - BEST1
KW - genotype-phenotype correlation
KW - macular degeneration
KW - mutations review
KW - prevalence
UR - http://www.scopus.com/inward/record.url?scp=85186750319&partnerID=8YFLogxK
U2 - 10.1167/iovs.65.2.39
DO - 10.1167/iovs.65.2.39
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C2 - 38411968
AN - SCOPUS:85186750319
SN - 0146-0404
VL - 65
JO - Investigative Ophthalmology and Visual Science
JF - Investigative Ophthalmology and Visual Science
IS - 2
M1 - 39
ER -