Table 4.
Candidate genetic variants identified in the Siberian HSP family based on analysis of whole exome sequencing data
| Gene symbol | Encoded protein | Amino acid change | Pathogenic prediction/score | Encoded protein expression | Encoded protein function and known disease associations | ||
|---|---|---|---|---|---|---|---|
| Pphen/SIFT | CADD | Grant-ham | |||||
| DLGAP2 | Disk large associated protein 2 | p.D758N | Damaging/deleterious | 24.2 | 23 | Brain | Involved in synaptic function and neuronal cell signaling |
| DSCAML1 | Down syndrome cell adhesion molecule like 1 | p.I1742N | Damaging/deleterious | 31 | 149 | Brain, heart, liver, pancreas, skeletal muscle | Involved in neuronal and axonal migration, cell adhesion, neuronal self-avoidance |
| DNAH10 | Dynein, axonemal, heavy chain 10 | p.V3539M | Damaging/deleterious | 17.13 | 21 | Brain, testis, trachea | Involved in axonal transport – moving vesicles, organelles, and signaling molecules along the axon |
| DNM2 | Dynamin 2 | p.R719W | Damaging/deleterious | 14.7 | 101 | Ubiquitously expressed | Clathrin mediated endocytosis and intracellular membrane trafficking. Linked to Centronuclear myopathy and Charcot-Marie-Tooth neuropathy |