Table 1.
Germline mutations in familial neuroblastoma predisposition genes. ALK, anaplastic lymphoma kinase; PHOX2B, paired-like homeobox 2B; HPCAL1, Hippocalcin-like protein 1.
| Gene | Mutation | Clinical Characteristics | Functional Consequence | Reference |
|---|---|---|---|---|
| PHOX2B | R100L | Found in families with Hirschsprung disease and neuroblastic tumors | Missense mutation in DNA binding domain Not dominant negative |
(Trochet et al. 2004) (Bourdeaut et al. 2005) (Pei et al. 2013) |
| R141G | Neuroblastoma patient inherited from mother, who was not affected | Missense mutation in homeodomain | (Trochet et al. 2004) | |
| G197D | Present in a family with multiple individuals with NB but no evidence of autonomic dysfunction or neurocristopathy | (McConville et al. 2006) | ||
| 676delG | Found in families with Hirschsprung disease and neuroblastoma | Overexpression causes decrease in terminal differentiation markers in sympathetic ganglion cells Dominant negative Unable to bind HPCAL1 |
(Mosse et al. 2004) (Pei et al. 2013) (Wang et al. 2014) |
|
| Polyalanine Repeat Mutations | Associated with congenital central hypoventilation syndrome (CCHS) | Genotype 20/33 identified in a neuroblastoma/CCHS/Hirschsprung disease patient | (Armstrong et al. 2015) | |
| ALK | R1060H | Unlikely to be clinically significant Believed to be a silent/passenger mutation | Not predicted to be damaging by algorithms Between kinase and transmembrane domains |
(Bresler et al. 2014) |
| G1128A | P-loop of kinase domain Transforms NIH-3T3 cells |
(Mosse et al. 2008) | ||
| T1151M T1151R | T1151R found in patient with multifocal tumors | Promotes modest constitutive ALK activation Does not transform NIH-3T3 cells β3 Strand of kinase domain |
(Bourdeaut et al. 2012) (Bresler et al. 2014) |
|
| I1183T | Unlikely to be clinically significant Believed to be a silent/passenger mutation |
N-lobe of kinase domain | (Bresler et al. 2014) | |
| R1192P | Found in patient with multifocal tumors | β4 Strand of kinase domain Increases kcat of non-phosphorylated ALK tyrosine kinase domain by 15x Transforms NIH-3T3 cells |
(Mosse et al. 2008) (Bourdeaut et al. 2012) (Bresler et al. 2014) |
|
| L1204F | Unlikely to be clinically significant Believed to be a silent/passenger mutation |
C-lobe of kinase domain | (Bresler et al. 2014) | |
| R1231Q | Unlikely to be clinically significant Believed to be a silent/passenger mutation |
Not predicted to be damaging by algorithms αE helix of kinase domain |
(Bresler et al. 2014) | |
| I1250T | Unlikely to be clinically significant Believed to be a silent/passenger mutation |
“Kinase dead” mutation that results in reduced activity via protein instability/misfolding Phe core domain |
(Schonherr, Ruuth, Eriksson, et al. 2011) (Bresler et al. 2014) |
|
| R1275Q | Crizotinib-sensitive Found in patient with multifocal tumors | R1275 residue accounts for ~45% of overall neuroblastoma ALK mutations (sporadic and germline) Activation loop of kinase domain |
(Mosse et al. 2008) (Bresler et al. 2011) (Bourdeaut et al. 2012) |