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001-es BibID:	BIBFORM058218
Első szerző:	Losonczy Gergely (szemész)
Cím:	A novel homozygous mutation (1619delC) in GPIIb gene associated with Glanzmann thrombasthenia, the decay of GPIIb-mRNA and the synthesis of a truncated GPIIb unable to form complex with GPIIIa / Gergely Losonczy, Nurit Rosenberg, Csongor Kiss, János Kappelmayer, György Vereb, Adrienne Kerényi, István Balogh, László Muszbek
Dátum:	2005
ISSN:	0340-6245
Megjegyzések:	The absence of agonist-induced platelet aggregation and the lack of fibrinogen receptor (GPIIb/IIIa) on the platelet surface demonstrated that the severe hemorrhagic complications of a child of Romany descent were caused by Glanzmann thrombasthenia. DNA sequencing revealed a novel homozygous deletion of a cytosine (1619delC) in the GPIIb gene causing a frameshift and predicting a novel stop codon at position 533 following 24 altered amino acids. Both parents possessed the same deletion in heterozygous form. The amount of GPIIb mRNA in the patient's platelets was 0.06% of the amount measured in control platelets. Neither GPIIb nor its truncated form could be detected in the platelets of the patient by Western blotting, while a small amount of GPIIIa was demonstrated. Quantitative flowcytometric analysis showed an elevated number of vitronectin receptors, a component of which is GPIIIa, on the patient's platelets. The surface expression of vitronectin receptor on thrombasthenic, but not on normal platelets was further increased by activation with thrombin receptor agonist peptide. BHK cells transfected with wild type GPIIIa andmutated GPIIb failed to express any mature GPIIb or pro-GPIIb. Immunoprecipitation with a polyclonal antibody recognizing both GPIIb and GPIIIa recovered a 60 kDa truncated form of GPIIb. This band was absent when immunoprecipitation was carried out with an antibody recognizing GPIIIa, suggesting that the truncated protein, lacking calf-1, calf-2 domains and major part of the thigh domain, is unable to form complex with GPIIIa.
Tárgyszavak:	Orvostudományok Elméleti orvostudományok idegen nyelvű folyóiratközlemény külföldi lapban Amino Acids analysis Animals Antibodies biosynthesis Blood Platelets Blotting, Western Case Report Cell Line Cells chemistry Child Cricetinae Cytosine Dna Electrophoresis, Polyacrylamide Gel Exons Family Health Female Flow Cytometry Gene Deletion genetics Homozygote Humans Hungary Immunoprecipitation Integrin alphaVbeta3 Integrin beta3 Male metabolism Mutagenesis, Site-Directed Mutation Platelet Aggregation Platelet Glycoprotein GPIIb-IIIa Complex Platelet Membrane Glycoprotein IIb Polymerase Chain Reaction Protein Binding Protein Structure, Tertiary Research RNA, Messenger Sequence Analysis, DNA Support Thrombasthenia Thrombin Transfection
Megjelenés:	Thrombosis and Haemostasis. - 93 : 5 (2005), p. 904-909. -
További szerzők:	Rosenberg, Nurit Kiss Csongor (1956-) (hematológus, onkológus) Kappelmayer János (1960-) (laboratóriumi szakorvos) Vereb György (1965-) (biofizikus, orvos) Kerényi Adrienne (1970-) (laboratóriumi szakorvos) Balogh István (1972-) (molekuláris biológus, genetikus) Muszbek László (1942-) (haematológus, kutató orvos)
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001-es BibID:	BIBFORM001214
Első szerző:	Takács Lili (szemész)
Cím:	TGFBI (BIGH3) gene mutations in Hungary-report of the novel F547S mutation associated with polymorphic corneal amyloidosis / Lili Takács, Gergely Losonczy, Klára Matesz, István Balogh, Zoltán Sohajda, Károly Tóth, Ferenc Fazakas, György Vereb, András Berta
Dátum:	2007
Megjegyzések:	To identify mutations in the Transforming Growth Factor Beta Induced (TGFBI) gene in Hungarian patients with corneal dystrophy and to characterize histological features of their corneal buttons excised during penetrating keratoplasty. METHODS: Exons of TGFBI were sequenced in 38 members of 15 unrelated families with corneal dystrophy and exon 12 was also sequenced in 100 healthy controls from the same population. Immunohistological analysis of available corneal buttons excised during penetrating keratoplasty was also performed. RESULTS: Molecular genetic analysis revealed a heterozygous R124C mutation in 18 patients with lattice type I dystrophy. A R555W heterozygous mutation was detected in five patients with granular Groenouw type I corneal dystrophy and a R555Q heterozygous mutation was found in four patients clinically diagnosed with Reis-Bucklers (one patient) and Thiel-Behnke (three patients) dystrophy. Three patients with "atypical granular" dystrophy later diagnosed as Avellino dystrophy were heterozygous for the R124H mutation. A novel heterozygous mutation (T1640C) causing a F547S amino acid exchange was detected in a patient with polymorphic corneal amyloidosis. Immunohistochemistry showed the presence of BIGH3 protein deposits in all examined corneal buttons. Electron microscopy confirmed the presence of amyloid fibrils in the case of the novel mutation. CONCLUSIONS: Our results indicate that molecular genetic analysis is required to confirm the diagnosis of corneal dystrophies. We report the first cases of Avellino dystrophy from Central-Eastern Europe. We conclude that the novel F547S mutation causes polymorphic corneal amyloidosis since no other mutations were detected in the TGFBI gene of this patient and the novel mutation could not be found in healthy controls.
Tárgyszavak:	Orvostudományok Természettudományok Klinikai orvostudományok Elméleti orvostudományok Biológiai tudományok idegen nyelvű folyóiratközlemény külföldi lapban TGFBI (BIGH3) gene mutation F547S polymorphic corneal amyloidosis
Megjelenés:	Molecular Vision. - 13 (2007), p. 1976-1983. -
További szerzők:	Losonczy Gergely (1977-) (szemész) Matesz Klára (1949-) (anatómus, neurobiológus) Balogh István (1972-) (molekuláris biológus, genetikus) Sohajda Zoltán (1969-) (szemész) Tóth Károly (orvos) Fazakas Ferenc (1969-) (molekuláris biológus) Vereb György (1965-) (biofizikus, orvos) Berta András (1955-) (szemész, gyermekszemész)
Internet cím:	elektronikus változat elektronikus változat
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