TY - JOUR
T1 - MYH9 Spectrum of Autosomal-Dominant Giant Platelet Syndromes
T2 - Unexpected Association with Fibulin-1 Variant-D Inactivation
AU - Toren, Amos
AU - Rozenfeld-Granot, Galit
AU - Heath, Karen E.
AU - Amariglio, Ninette
AU - Rocca, Bianca
AU - Crosson, John
AU - Epstein, Charles J.
AU - Laghi, Ferdinando
AU - Landolfi, Raffaele
AU - Carlsson, Lena E.
AU - Argraves, Scott
AU - Bizzaro, Nicola
AU - Moxey-Mims, Marva
AU - Brok-Simoni, Frida
AU - Martignetti, John A.
AU - Greinacher, Andreas
AU - Rechavi, Gideon
PY - 2003/12
Y1 - 2003/12
N2 - The autosomal-dominant giant platelet syndromes (Fechtner, Epstein, and Sebastian platelet syndromes and May-Hegglin anomaly) represent a group of disorders characterized by variable degrees of macrothrombocytopenia with further combinations of neutrophil inclusion bodies and Alport-like syndrome manifestations, namely, deafness, renal disease, and eye abnormalities. The disease-causing gene of these giant platelet syndromes was previously mapped by us to chromosome 22. Following their successful mapping, these syndromes were shown to represent a broad phenotypic spectrum of disorders caused by different mutations in the nonmuscle myosin heavy chain 9 gene (MYH9). In this study, we examined the potential role of another gene, fibulin-1, encoding an extracellular matrix protein as a disease modifier. Eight unrelated families with autosomal-dominant giant platelet syndromes were studied for DNA sequence mutations and expression of the four fibulin-1 splice variants (A-D). A mutation in the splice acceptor site of fibulin-1 exon 19 was found in affected individuals of the Israeli Fechtner family, whereas no MYH9 mutations were identified. Unexpectedly, fibulin-1 variant D expression was absent in affected individuals from all eight families and coupled with expression of a putative antisense RNA. Transfection of the putative antisense RNA into H1299 cells abolished variant D expression. Based on the observation that only affected individuals lack variant D expression and demonstrate antisense RNA overexpression, we suggest that these autosomal-dominant giant platelet syndromes are associated, and may be modified, by aberrant antisense gene regulation of the fibulin-1 gene.
AB - The autosomal-dominant giant platelet syndromes (Fechtner, Epstein, and Sebastian platelet syndromes and May-Hegglin anomaly) represent a group of disorders characterized by variable degrees of macrothrombocytopenia with further combinations of neutrophil inclusion bodies and Alport-like syndrome manifestations, namely, deafness, renal disease, and eye abnormalities. The disease-causing gene of these giant platelet syndromes was previously mapped by us to chromosome 22. Following their successful mapping, these syndromes were shown to represent a broad phenotypic spectrum of disorders caused by different mutations in the nonmuscle myosin heavy chain 9 gene (MYH9). In this study, we examined the potential role of another gene, fibulin-1, encoding an extracellular matrix protein as a disease modifier. Eight unrelated families with autosomal-dominant giant platelet syndromes were studied for DNA sequence mutations and expression of the four fibulin-1 splice variants (A-D). A mutation in the splice acceptor site of fibulin-1 exon 19 was found in affected individuals of the Israeli Fechtner family, whereas no MYH9 mutations were identified. Unexpectedly, fibulin-1 variant D expression was absent in affected individuals from all eight families and coupled with expression of a putative antisense RNA. Transfection of the putative antisense RNA into H1299 cells abolished variant D expression. Based on the observation that only affected individuals lack variant D expression and demonstrate antisense RNA overexpression, we suggest that these autosomal-dominant giant platelet syndromes are associated, and may be modified, by aberrant antisense gene regulation of the fibulin-1 gene.
KW - Antisense
KW - Fibulin
KW - Giant platelet syndrome
KW - Myosin heavy chain 9
UR - http://www.scopus.com/inward/record.url?scp=10744226183&partnerID=8YFLogxK
U2 - 10.1002/ajh.10425
DO - 10.1002/ajh.10425
M3 - Article
C2 - 14635206
AN - SCOPUS:10744226183
SN - 0361-8609
VL - 74
SP - 254
EP - 262
JO - American Journal of Hematology
JF - American Journal of Hematology
IS - 4
ER -