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. 2015 Mar 30;35(6):1483–1492. doi: 10.3892/ijmm.2015.2158

Table I.

Human genetic skeletal diseases result from qualitative (anti-morphic) defects in cartilage structural proteins.

Gene Protein Disease(s) Genetic loci Domain Refs.
COMP COMP Pseudoachondroplasia (AD)
Multiple epiphyseal dysplasia (AD)		 PSACH
EDM1		 T3-7 repeats
C-terminal domain		 (4,45)
MATN3 Matrilin-3 Multiple epiphyseal dysplasia (AD) EDM5 vWFA (18)
COL9A1
COL9A2
COL9A3 		Type IX collagen Multiple epiphyseal dysplasia (AD) EDM6
EDM2
EDM3		 COL3 domain (4648)
COL2A1 Type II collagen Diverse range of AD and AR phenotypes collectively known as type II collagenopathies Various Triple helical region and C-propeptide (49)
COL11A1
COL11A2 		Type XI collagen Diverse range of AD and AR phenotypes collectively known as type XI collagenopathies Various (50)
COL10A1 Type X collagen Metaphyseal chondrodysplasia, type Schmid (AD) MCDS Carboxyl-terminal non-collagenous domain (NC1) (51)
ACAN Aggrecan Spondyloepimetaphyseal dyslasia (AR)
Osteochondritis dissecans (AD)
Short stature, accelerated bonematuration (AD)		 SEMD
OCD		 G3 C-type lectin domain (5254)

COMP, cartilage oligomeric matrix protein; PSACH, pseudoachondroplasia; AD, autosomal dominant; AR, autosomal recessive.