IRIS

Autosomal recessive spastic paraplegia with thinning of corpus callosum (ARHSP-TCC) is a complex form of HSP initially described in Japan but subsequently reported to have a worldwide distribution with a particular high frequency in multiple families from the Mediterranean basin. We recently showed that ARHSP-TCC is commonly associated with mutations in SPG11/KIAA1840 on chromosome 15q. We have now screened a collection of new patients mainly originating from Italy and Brazil, in order to further ascertain the spectrum of mutations in SPG11, enlarge the ethnic origin of SPG11 patients, determine the relative frequency at the level of single Countries (i.e., Italy), and establish whether there is one or more common mutation. In 25 index cases we identified 32 mutations; 22 are novel, including 9 nonsense, 3 small deletions, 4 insertions, 1 in/del, 1 small duplication, 1 missense, 2 splice-site, and for the first time a large genomic rearrangement. This brings the total number of SPG11 mutated patients in the SPATAX collection to 111 cases in 44 families and in 17 isolated cases, from 16 Countries, all assessed using homogeneous clinical criteria. While expanding the spectrum of mutations in SPG11, this larger series also corroborated the notion that even within apparently homogeneous population a molecular diagnosis cannot be achieved without full gene sequencing.

Screening of ARHSP-TCC patients expands the spectrum of SPG11 mutations and includes a large scale gene deletion / Denora, Ps; Schlesinger, D; Casali, C; Kok, F; Tessa, A; Boukhris, A; Azzedine, H; Dotti, Mt; Bruno, C; Truchetto, J; Biancheri, R; Fedirko, E; Di Rocco, M; Bueno, C; Malandrini, A; Battini, R; Sickl, E; de Leva, Mf; Boespflug Tanguy, O; Silvestri, G; Simonati, A; Said, E; Ferbert, A; Criscuolo, C; Heinimann, K; Modoni, A; Weber, P; Palmeri, S; Plasilova, M; Pauri, F; Cassandrini, D; Battisti, C; Pini, A; Tosetti, M; Hauser, E; Masciullo, M; Fabio, Rd; Piccolo, F; Denis, E; Cioni, G; Massa, R; Giustina, Ed; Calabrese, O; Melone, Ma; DE MICHELE, Giuseppe; Federico, A; Bertini, E; Durr, A; Brockmann, K; van der Knaap, Ms; Zatz, M; Filla, Alessandro; Brice, A; Stevanin, G; Santorelli, F. M.. - In: HUMAN MUTATION. - ISSN 1059-7794. - 1050:30(2009), pp. 500-519. [10.1002/humu.20945]

Screening of ARHSP-TCC patients expands the spectrum of SPG11 mutations and includes a large scale gene deletion.

DE MICHELE, GIUSEPPE;FILLA, ALESSANDRO;
2009

Abstract

Autosomal recessive spastic paraplegia with thinning of corpus callosum (ARHSP-TCC) is a complex form of HSP initially described in Japan but subsequently reported to have a worldwide distribution with a particular high frequency in multiple families from the Mediterranean basin. We recently showed that ARHSP-TCC is commonly associated with mutations in SPG11/KIAA1840 on chromosome 15q. We have now screened a collection of new patients mainly originating from Italy and Brazil, in order to further ascertain the spectrum of mutations in SPG11, enlarge the ethnic origin of SPG11 patients, determine the relative frequency at the level of single Countries (i.e., Italy), and establish whether there is one or more common mutation. In 25 index cases we identified 32 mutations; 22 are novel, including 9 nonsense, 3 small deletions, 4 insertions, 1 in/del, 1 small duplication, 1 missense, 2 splice-site, and for the first time a large genomic rearrangement. This brings the total number of SPG11 mutated patients in the SPATAX collection to 111 cases in 44 families and in 17 isolated cases, from 16 Countries, all assessed using homogeneous clinical criteria. While expanding the spectrum of mutations in SPG11, this larger series also corroborated the notion that even within apparently homogeneous population a molecular diagnosis cannot be achieved without full gene sequencing.
2009
HUMAN MUTATION
Screening of ARHSP-TCC patients expands the spectrum of SPG11 mutations and includes a large scale gene deletion / Denora, Ps; Schlesinger, D; Casali, C; Kok, F; Tessa, A; Boukhris, A; Azzedine, H; Dotti, Mt; Bruno, C; Truchetto, J; Biancheri, R; Fedirko, E; Di Rocco, M; Bueno, C; Malandrini, A; Battini, R; Sickl, E; de Leva, Mf; Boespflug Tanguy, O; Silvestri, G; Simonati, A; Said, E; Ferbert, A; Criscuolo, C; Heinimann, K; Modoni, A; Weber, P; Palmeri, S; Plasilova, M; Pauri, F; Cassandrini, D; Battisti, C; Pini, A; Tosetti, M; Hauser, E; Masciullo, M; Fabio, Rd; Piccolo, F; Denis, E; Cioni, G; Massa, R; Giustina, Ed; Calabrese, O; Melone, Ma; DE MICHELE, Giuseppe; Federico, A; Bertini, E; Durr, A; Brockmann, K; van der Knaap, Ms; Zatz, M; Filla, Alessandro; Brice, A; Stevanin, G; Santorelli, F. M.. - In: HUMAN MUTATION. - ISSN 1059-7794. - 1050:30(2009), pp. 500-519. [10.1002/humu.20945]
1.1 Articolo in rivista
File in questo prodotto:
File Dimensione Formato  
Screening.pdf

accesso aperto

Tipologia: Documento in Post-print
Licenza: Dominio pubblico
Dimensione 842.3 kB
Formato Adobe PDF
Visualizza/Apri
842.3 kB Adobe PDF Visualizza/Apri

I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.

Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/342172
Citazioni
  • ???jsp.display-item.citation.pmc??? ND
  • Scopus 57
  • ???jsp.display-item.citation.isi??? 57
social impact