TY - JOUR
T1 - ALK germline mutations in patients with neuroblastoma
T2 - A rare and weakly penetrant syndrome
AU - Bourdeaut, Franck
AU - Ferrand, Sandrine
AU - Brugières, Laurence
AU - Hilbert, Marjorie
AU - Ribeiro, Agnès
AU - Lacroix, Ludovic
AU - Bénard, Jean
AU - Combaret, Valérie
AU - Michon, Jean
AU - Valteau-Couanet, Dominique
AU - Isidor, Bertrand
AU - Rialland, Xavier
AU - Poirée, Maryline
AU - Defachelles, Anne Sophie
AU - Peuchmaur, Michel
AU - Schleiermacher, Gudrun
AU - Pierron, Gaëlle
AU - Gauthier-Villars, Marion
AU - Janoueix-Lerosey, Isabelle
AU - Delattre, Olivier
N1 - Funding Information:
This work was supported by grants from the Institut National du Cancer (INCa) and Direction de l¢Hospitalisation et de l¢Organisation des Soins (DHOS), the Ligue Nationale contre le Cancer (Equipe labellise’e and CIT project), the APAESIC (Association des Parents et des Amis des Enfants Soignés à l’Institut Curie), the Association Hubert Gouin, les amis de Claire, Les Bagouz à Manon, la Hulotte and Enfance et Sante. We thank all the clinicians and pathologists from the French Society of Cancer in children (SFCE) who refer their tumours and clinical data. We thank Dr Virginie Verkarre for the picture of the myenteric plexus hyperplasia.
PY - 2012/3/1
Y1 - 2012/3/1
N2 - Neuroblastic tumours may occur in a predisposition context. Two main genes are involved: PHOX2B, observed in familial cases and frequently associated with other neurocristopathies (Ondine's and Hirschsprung's disease); and ALK, mostly in familial tumours. We have assessed the frequency of mutations of these two genes in patients with a presumable higher risk of predisposition. We sequenced both genes in 26 perinatal cases (prebirth and <1 month of age, among which 10 were multifocal), 16 multifocal postnatal (>1 month) cases, 3 pairs of affected relatives and 8 patients with multiple malignancies. The whole coding sequences of the two genes were analysed in tumour and/or constitutional DNAs. We found three ALK germline mutations, all in a context of multifocal tumours. Two mutations (T1151R and R1192P) were inherited and shared by several unaffected patients, thus illustrating an incomplete penetrance. Younger age at tumour onset did not seem to offer a relevant selection criterion for ALK analyses. Conversely, multifocal tumours might be the most to benefit from the genetic screening. Finally, no PHOX2B germline mutation was found in this series. In conclusion, ALK deleterious mutations are rare events in patients with a high probability of predisposition. Other predisposing genes remain to be discovered.
AB - Neuroblastic tumours may occur in a predisposition context. Two main genes are involved: PHOX2B, observed in familial cases and frequently associated with other neurocristopathies (Ondine's and Hirschsprung's disease); and ALK, mostly in familial tumours. We have assessed the frequency of mutations of these two genes in patients with a presumable higher risk of predisposition. We sequenced both genes in 26 perinatal cases (prebirth and <1 month of age, among which 10 were multifocal), 16 multifocal postnatal (>1 month) cases, 3 pairs of affected relatives and 8 patients with multiple malignancies. The whole coding sequences of the two genes were analysed in tumour and/or constitutional DNAs. We found three ALK germline mutations, all in a context of multifocal tumours. Two mutations (T1151R and R1192P) were inherited and shared by several unaffected patients, thus illustrating an incomplete penetrance. Younger age at tumour onset did not seem to offer a relevant selection criterion for ALK analyses. Conversely, multifocal tumours might be the most to benefit from the genetic screening. Finally, no PHOX2B germline mutation was found in this series. In conclusion, ALK deleterious mutations are rare events in patients with a high probability of predisposition. Other predisposing genes remain to be discovered.
KW - ALK
KW - neuroblastoma
KW - predisposition
UR - http://www.scopus.com/inward/record.url?scp=84857190916&partnerID=8YFLogxK
U2 - 10.1038/ejhg.2011.195
DO - 10.1038/ejhg.2011.195
M3 - Article
C2 - 22071890
AN - SCOPUS:84857190916
SN - 1018-4813
VL - 20
SP - 291
EP - 297
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 3
ER -