Skip to main content
. 2024 Jan 11;14:1299232. doi: 10.3389/fendo.2023.1299232

Table 5.

Inheritance and genetic characteristics.

All patients (n = 568) Patients with pathogenic variants (n = 437)
n % n %
Inheritance No 97 17.1% 72 16.5%
Yes 204 35.9% 122 27.9%
Unknown 267 47.0% 243 55.6%
Mutation No 131 23.1%
Yes 437 76.9% 437 100.0%
Mutational status No mutation 131 23.1%
Homozygosis/compound heterozygosis 9 1.6% 9 2.1%
Heterozygosis 428 75.4% 428 97.9%
Mutated gene COL1A1 313 55.1% 313 71.6%
COL1A2 112 19.7% 112 25.6%
CRTAP 1 0.2% 1 0.2%
FKBP10 1 0.2% 1 0.2%
IFITM5 3 0.5% 3 0.7%
LEPRE1 3 0.5% 3 0.7%
PLS3 1 0.2% 1 0.2%
SERPINF1 3 0.5% 3 0.7%
Negative for COL1 109 19.2%
Negative for COL1− and other genes 22 3.9%
Dominant mutation No mutation 131 23.1%
No 9 1.6% 9 2.1%
Yes 428 75.4% 428 97.9%
Effect of mutation No mutation or non-COL1 mutation 143 25.2% 12 2.7%
Quantitative/haploinsufficiency 202 35.6% 202 46.2%
Qualitative/structural 223 39.3% 223 51.0%
Mutation type No mutation 131 23.1%
Splice site 76 13.4% 76 17.4%
Deletion/insertion/duplication/frameshift/big rearrangements 136 23.9% 136 31.1%
Glycine substitution 129 22.7% 129 29.5%
Other missense 20 3.5% 20 4.6%
Nonsense 72 12.7% 72 16.5%
Initiating methionine 4 0.7% 4 0.9%