Rough endoplasmic reticulum trafficking errors by different classes of mutant dentin sialophosphoprotein (DSPP) cause dominant negative effects in both dentinogenesis imperfecta and dentin dysplasia by entrapping normal DSPP.

[dentinogenesis imperfecta]

Families with nonsyndromic dentinogenesis imperfecta (DGI ) and the milder , dentin dysplasia (DD ), have mutations in one allele of the dentin sialophosphoprotein (DSPP ) gene . Because loss of a single Dspp allele in mice (and likely , humans ) causes no dental phenotype , the mechanism (s ) underling the dominant negative effects were investigated . DSPP mutations occur in three classes . (The first class , the mid-leader missense mutation , Y 6 D , was not investigated in this report .) All other 5 ′ mutations of DSPP result in changes /loss in the first three amino acids (isoleucine-proline-valine [IPV ]) of mature DSPP or , for the A 15 V missense mutation , some retention of the hydrophobic leader sequence . All of this second class of mutations caused mutant DSPP to be retained in the rough endoplasmic reticulum (rER ) of transfected HEK 293 cells . Trafficking out of the rER by coexpressed normal DSPP was reduced in a dose-responsive manner , probably due to formation of Ca 2 +-dependent complexes with the retained mutant DSPP . IPV-like sequences begin many secreted Ca 2 +-binding proteins , and changing the third amino acid to the charged aspartate (D ) in three other acidic proteins also caused increased rER accumulation . Both the leader -retaining A 15 V and the long string of hydrophobic amino acids resulting from all known frameshift mutations within the 3 ′-encoded Ca 2 +-binding repeat domain (third class of mutations ) caused retention by association of the mutant proteins with rER membranes . More 5 ′ frameshift mutations result in longer mutant hydrophobic domains , but the milder phenotype , DD , probably due to lower effectiveness of the remaining , shorter Ca 2 +-binding domain in capturing normal DSPP protein within the rER . This study presents evidence of a shared underlying mechanism of capturing of normal DSPP by two different classes of DSPP mutations and offers an explanation for the mild (DD-II ) versus severe (DGI -II and III ) nonsyndromic dentin phenotypes . Evidence is also presented that many acidic , Ca 2 +-binding proteins may use the same IPV-like receptor /pathway for exiting the rER .