Purpose
To identify genetic alleles associated with differences in choroidal thickness (CT) in a population-based multiethnic Asian cohort.
Methods
A population-based multiethnic Asian cohort without retinal pathology was subjected to spectral-domain OCT (SD-OCT) and genotyping of risk alleles in
CFH
,
VIPR2
,
ARMS2
, and
CETP
. Subfoveal choroidal thickness (SFCT) values were assessed from SD-OCT, and associations with the risk alleles were determined for each cohort.
Results
A total of 1045 healthy Asian individuals (550 Chinese, 147 Indians, 348 Malays) were prospectively enrolled in the study. Several
CFH
alleles (rs800292, rs1061170, and rs1329428) were associated with increased SFCT in Indians (+18.7 to +31.7 µm;
P
= 0.001–0.038) and marginally associated with decreased SFCT in Malays (−12.7 to −20.6 µm;
P
= 0.014–0.022). Haplotype analysis of
CFH
revealed variable associations with SFCT among races, with the H6 haplotype being associated with a 29.08-µm reduction in SFCT in the Chinese cohort (
P
= 0.02) but a 35.2-µm increase in SFCT in the Indian cohort (
P
< 0.001). Finally, subfield analysis of the Chinese cohort identified associations between the
CFH
risk allele rs1061170 and reduced CT in the nasal and superior sectors (−20.2 to −25.8 µm;
P
= 0.003–0.027).
Conclusions
CFH
variants are variably associated with CT among Asian ethnic groups. This has broad implications for the pathogenesis of common diseases such as age-related macular degeneration and central serous choroidopathy, the pathogenesis of which is associated with CT.