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1. High mutation detection rates in cerebral cavernous malformation upon stringent inclusion criteria: one‐third of probands are minors

Author

Spiegler, Stefanie, Najm, Juliane, Liu, Jian, Gkalympoudis, Stephanie, Schröder, Winnie, Borck, Guntram, Brockmann, Knut, Elbracht, Miriam, Fauth, Christine, Ferbert, Andreas, Freudenberg, Leonie, Grasshoff, Ute, Hellenbroich, Yorck, Henn, Wolfram, Hoffjan, Sabine, Hüning, Irina, Korenke, G Christoph, Kroisel, Peter M, Kunstmann, Erdmute, Mair, Martina, Munk-Schulenburg, Susanne, Nikoubashman, Omid, Pauli, Silke, Rudnik-Schöneborn, Sabine, Sudholt, Irene, Sure, Ulrich, Tinschert, Sigrid, Wiednig, Michaela, Zoll, Barbara, Ginsberg, Mark H, and Felbor, Ute

Subjects
Stroke, Genetic Testing, Neurosciences, Rare Diseases, Brain Disorders, Clinical Research, Genetics, 2.1 Biological and endogenous factors, Aetiology, Age at disease onset, CCM1, CCM2, CCM3, cerebral cavernous malformation, HEG1, mutation detection rate, predictive testing, Medicinal and Biomolecular Chemistry, Clinical Sciences
Abstract

Cerebral cavernous malformations (CCM) are prevalent vascular malformations occurring in familial autosomal dominantly inherited or isolated forms. Once CCM are diagnosed by magnetic resonance imaging, the indication for genetic testing requires either a positive family history of cavernous lesions or clinical symptoms such as chronic headaches, epilepsy, neurological deficits, and hemorrhagic stroke or the occurrence of multiple lesions in an isolated case. Following these inclusion criteria, the mutation detection rates in a consecutive series of 105 probands were 87% for familial and 57% for isolated cases. Thirty-one novel mutations were identified with a slight shift towards proportionally more CCM3 mutations carriers than previously published (CCM1: 60%, CCM2: 18%, CCM3: 22%). In-frame deletions and exonic missense variants requiring functional analyses to establish their pathogenicity were rare: An in-frame deletion within the C-terminal FERM domain of CCM1 resulted in decreased protein expression and impaired binding to the transmembrane protein heart of glass (HEG1). Notably, 20% of index cases carrying a CCM mutation were below age 10 and 33% below age 18 when referred for genetic testing. Since fulminant disease courses during the first years of life were observed in CCM1 and CCM3 mutation carriers, predictive testing of minor siblings became an issue.

Published
2014

13. Cytology-based treatment decision in primary lung cancer: Is it accurate enough?

Author

Roll, Patrice, Roca, Elisa, Lacroix, Romaric, Judicone, Coralie, Laroumagne, Sophie, Robert, Stéphane, Cointe, Sylvie, Muller, Alexandre, Kaspi, Elise, Brisson, Alain, Tantucci, Claudio, Astoul, Philippe, Dignat-George, Françoise, Barthélémy, Florian, Navarro, Claire, Fayek, Racha, Da Silva, Nathalie, Sigaudy, Sabine, Oshima, Junko, Bonne, Gisèle, Papadopoulou-Legbelou, Kyriaki, Evangeliou, Athanasios, Spilioti, Martha, LeMerrer, Martine, Wevers, Ron, Morava, Eva, Robaglia-Schlupp, Andrée, Lévy, Nicolas, Bartoli, Marc, De Sandre-Giovannoli, Annachiara, Hadj-Rabia, Smail, Mashiah, Jacob, Boyer, Amandine, Bourgeois, Patrice, Van Kien, Philippe Khau, Bodemer, Christine, Navarro, Claire Laure, Esteves-Vieira, Vera, Courrier, Sébastien, Duong Nguyen, Thuy, Huong, Le Thi Thanh, Meinke, Peter, Schröder, Winnie, Cormier-Daire, Valérie, Sznajer, Yves, Amor, David, Lagerstedt, Kristina, Biervliet, Martine, van den Akker, Peter, Cau, Pierre, BADENS, Catherine, Wehnert, Manfred, Sakr, Lama, Payan, Marie-José, Liprandi, Agnès, Dutau, Hervé, Loundou, Anderson, Barlesi, Fabrice, Aix Marseille Université (AMU), Assistance Publique - Hôpitaux de Marseille (APHM), Laboratoire de Biologie Cellulaire [Hôpital de la Timone - APHM], Assistance Publique - Hôpitaux de Marseille (APHM)- Hôpital de la Timone [CHU - APHM] (TIMONE), Marseille medical genetics - Centre de génétique médicale de Marseille (MMG), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), and Institut National de la Santé et de la Recherche Médicale (INSERM)-Aix Marseille Université (AMU)

Subjects
Adult, Male, Pulmonary and Respiratory Medicine, Cancer Research, medicine.medical_specialty, Pathology, Lung Neoplasms, Cytodiagnosis, [SDV]Life Sciences [q-bio], Cytological Techniques, Adenocarcinoma of Lung, Adenocarcinoma, Malignancy, 03 medical and health sciences, 0302 clinical medicine, Bronchoscopy, Carcinoma, Non-Small-Cell Lung, Biopsy, medicine, Carcinoma, Humans, Neoplasms, Squamous Cell, Lung cancer, ComputingMilieux_MISCELLANEOUS, Aged, Retrospective Studies, 030304 developmental biology, Aged, 80 and over, 0303 health sciences, medicine.diagnostic_test, business.industry, Biopsy, Needle, Not Otherwise Specified, Middle Aged, medicine.disease, Small Cell Lung Carcinoma, respiratory tract diseases, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Female, Radiology, business
Abstract

Accurate distinction of lung cancer types has become increasingly important as recent trials have shown differential response to chemotherapy among non-small cell lung carcinoma (NSCLC) subtypes. Cytological procedures are frequently used but their diagnostic accuracy has been previously questioned. However, new endoscopic and cytological techniques might have improved cytological accuracy in comparison with prior findings. The aim of this study was to reassess cytological accuracy for diagnosis of lung cancer subtypes. A retrospective chart review of subjects who underwent fiberoptic bronchoscopy (FOB) for suspicion of lung cancer in 2007–2008, was undertaken. Reports of bronchoscopically derived cytological specimens were compared to those of histological material. Endoscopic findings and specific investigational techniques were taken into account. A total of 467 FOB with both cytological and histological diagnostic techniques were performed in 449 subjects. Patients consisted of 345 men and 104 women (median age, 65 yrs). Cytology proved malignancy in 157 patients. Cytologically diagnosed carcinomas were classified into squamous cell carcinoma (SqCC) in 56, adenocarcinoma (ADC) in 6, small cell lung carcinoma (SCLC) in 12, non-small cell lung carcinoma not otherwise specified (NSCLC-NOS) in 71, and unclassified carcinoma in 12. Cytology correlated fairly with biopsy specimens, as agreement was observed in 83% of SCLC, 100% of ADC, 74% of SqCC and 8% of NSCLC-NOS. Interestingly, 61% of cytologically identified NSCLC-NOS were classified as ADC by histology. Cytological accuracy improved in case of an endobronchial lesion, mainly for SqCC. These results indicate that cytological accuracy remains fair with regard to diagnosis of squamous and non-squamous lung cancer subtypes. Improvement of cytological accuracy is expected however with novel diagnostic strategies.

Published
2012
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14. New ZMPSTE24 (FACE1) mutations in patients affected with restrictive dermopathy or related progeroid syndromes and mutation update

Author

UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Centre de génétique médicale UCL, Navarro, Claire Laure, Esteves-Vieira, Vera, Courrier, Sébastien, Boyer, Amandine, Duong Nguyen, Thuy, Huong, Le Thi Thanh, Meinke, Peter, Schröder, Winnie, Cormier-Daire, Valérie, Sznajer, Yves, Amor, David J, Lagerstedt, Kristina, Biervliet, Martine, Van Den Akker, Peter C, Cau, Pierre, Roll, Patrice, Lévy, Nicolas, Badens, Catherine, Wehnert, Manfred, De Sandre-Giovannoli, Annachiara, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Centre de génétique médicale UCL, Navarro, Claire Laure, Esteves-Vieira, Vera, Courrier, Sébastien, Boyer, Amandine, Duong Nguyen, Thuy, Huong, Le Thi Thanh, Meinke, Peter, Schröder, Winnie, Cormier-Daire, Valérie, Sznajer, Yves, Amor, David J, Lagerstedt, Kristina, Biervliet, Martine, Van Den Akker, Peter C, Cau, Pierre, Roll, Patrice, Lévy, Nicolas, Badens, Catherine, Wehnert, Manfred, and De Sandre-Giovannoli, Annachiara

Abstract

Restrictive dermopathy (RD) is a rare and extremely severe congenital genodermatosis, characterized by a tight rigid skin with erosions at flexure sites, multiple joint contractures, low bone density and pulmonary insufficiency generally leading to death in the perinatal period. RD is caused in most patients by compound heterozygous or homozygous ZMPSTE24 null mutations. This gene encodes a metalloprotease specifically involved in lamin A post-translational processing. Here, we report a total of 16 families for whom diagnosis and molecular defects were clearly established. Among them, we report seven new ZMPSTE24 mutations, identified in classical RD or Mandibulo-acral dysplasia (MAD) affected patients. We also report nine families with one or two affected children carrying the common, homozygous thymine insertion in exon 9 and demonstrate the lack of a founder effect. In addition, we describe several new ZMPSTE24 variants identified in unaffected controls or in patients affected with non-classical progeroid syndromes. In addition, this mutation update includes a comprehensive search of the literature on previously described ZMPSTE24 mutations and associated phenotypes. Our comprehensive analysis of the molecular pathology supported the general rule: complete loss-of-function of ZMPSTE24 leads to RD, whereas other less severe phenotypes are associated with at least one haploinsufficient allele. © 2014 Macmillan Publishers Limited All rights reserved.

Published
2014

17. New ZMPSTE24 (FACE1) mutations in patients affected with restrictive dermopathy or related progeroid syndromes and mutation update

Author

Navarro, Claire Laure, primary, Esteves-Vieira, Vera, additional, Courrier, Sébastien, additional, Boyer, Amandine, additional, Duong Nguyen, Thuy, additional, Huong, Le Thi Thanh, additional, Meinke, Peter, additional, Schröder, Winnie, additional, Cormier-Daire, Valérie, additional, Sznajer, Yves, additional, Amor, David J, additional, Lagerstedt, Kristina, additional, Biervliet, Martine, additional, van den Akker, Peter C, additional, Cau, Pierre, additional, Roll, Patrice, additional, Lévy, Nicolas, additional, Badens, Catherine, additional, Wehnert, Manfred, additional, and De Sandre-Giovannoli, Annachiara, additional

Published
2013
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19. Platelet receptor and clotting factor polymorphisms as genetic risk factors for thromboembolic complications in heparin-induced thrombocytopenia.

Author

Carlsson, Lena E, Lubenow, Norbert, Blumentritt, Carmen, Kempf, Reiner, Papenberg, Stephanie, Schröder, Winnie, Eichler, Petra, Herrmann, Falko H, Santoso, Sentot, Greinacher, Andreas, Carlsson, Lena E, Lubenow, Norbert, Blumentritt, Carmen, Kempf, Reiner, Papenberg, Stephanie, Schröder, Winnie, Eichler, Petra, Herrmann, Falko H, Santoso, Sentot, and Greinacher, Andreas

Abstract

Heparin-induced thrombocytopenia (HIT) is an immune mediated adverse reaction to heparin treatment often associated with limb- and/or life-threatening thromboembolic complications (TECs). Presently, no prognostic marker has been identified that allows differentiation between mildly (isolated thrombocytopenia) and severely (TECs) affected patients. This study assesses the impact of platelet glycoprotein- and clotting factor polymorphisms in HIT-patients with isolated thrombocytopenia compared to HIT-patients with TECs. Sixty-three HIT-patients with isolated thrombocytopenia and 79 HIT-patients with HIT-related TECs were genotyped for GPIIb-IIIa polymorphisms (HPA-1, HPA-3), GPIa-IIa polymorphisms (HPA-5, GPIaC807T), GPIb-IX-V polymorphisms (HPA-2, Kozak-5, VNTR), and clotting factor polymorphisms (FV-Leiden R506Q, prothrombin PT-G20210A and MTHFR C677T). Women more often presented with TECs than men (P = 0.04). No differences in genotype frequencies could be seen on comparing HIT-patients with and without TECs. Analysing men and women separately, the C allele of the Kozak polymorphism was overrepresented in men who developed TECs (P = 0.034). The enhanced risk of women to develop HIT-associated TECs remains unexplained but it is potentially important in view of recent data on sex-hormone related changes of haemostasis. There was no correlation between platelet glycoprotein- and clotting factor polymorphisms and the risk to develop HIT-associated TECs. An association between the development of TECs and the Kozak-5C allele could be seen among male patients. However, this would need to be assessed in further larger studies. Most likely, the high levels of thrombin generation during acute HIT are so procoagulant that less pronounced risk factors such as polymorphisms are overshadowed.

Published
2003
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23. Factor V Leiden, Prothrombin Gene G20210A Variant, and Methylenetetrahydrofolate Reductase C677T Genotype in Young Adults With Ischemic Stroke

Author

Lopaciuk, Stanislaw, primary, Bykowska, Ksenia, additional, Kwiecinski, Hubert, additional, Mickielewicz, Anatol, additional, Czlcankawska, Anna, additional, Mendel, Tadeusz, additional, Kuczynska-Zardzewialy, Arletta, additional, Szelagowska, Dorota, additional, Windyga, Jerzy, additional, Schröder, Winnie, additional, Herrmann, Falko H., additional, and Jedrzejowska, Hanna, additional

Published
2001
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26. New ZMPSTE24 (FACE1) mutations in patients affected with restrictive dermopathy or related progeroid syndromes and mutation update.

Author

Navarro, Claire Laure, Esteves-Vieira, Vera, Courrier, Sébastien, Boyer, Amandine, Duong Nguyen, Thuy, Huong, Le Thi Thanh, Meinke, Peter, Schröder, Winnie, Cormier-Daire, Valérie, Sznajer, Yves, Amor, David J, Lagerstedt, Kristina, Biervliet, Martine, van den Akker, Peter C, Cau, Pierre, Roll, Patrice, Lévy, Nicolas, Badens, Catherine, Wehnert, Manfred, and De Sandre-Giovannoli, Annachiara

Subjects
DYSPLASIA, GENETIC mutation, CONGENITAL disorders, CELL transformation, DNA replication
Abstract

Restrictive dermopathy (RD) is a rare and extremely severe congenital genodermatosis, characterized by a tight rigid skin with erosions at flexure sites, multiple joint contractures, low bone density and pulmonary insufficiency generally leading to death in the perinatal period. RD is caused in most patients by compound heterozygous or homozygous ZMPSTE24 null mutations. This gene encodes a metalloprotease specifically involved in lamin A post-translational processing. Here, we report a total of 16 families for whom diagnosis and molecular defects were clearly established. Among them, we report seven new ZMPSTE24 mutations, identified in classical RD or Mandibulo-acral dysplasia (MAD) affected patients. We also report nine families with one or two affected children carrying the common, homozygous thymine insertion in exon 9 and demonstrate the lack of a founder effect. In addition, we describe several new ZMPSTE24 variants identified in unaffected controls or in patients affected with non-classical progeroid syndromes. In addition, this mutation update includes a comprehensive search of the literature on previously described ZMPSTE24 mutations and associated phenotypes. Our comprehensive analysis of the molecular pathology supported the general rule: complete loss-of-function of ZMPSTE24 leads to RD, whereas other less severe phenotypes are associated with at least one haploinsufficient allele. [ABSTRACT FROM AUTHOR]

Published
2014
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28. World distribution of factor V Leiden mutation

Author

de Maat, MoniekP.M., primary, Kluft, Cornelis, additional, Jespersen, Jørgen, additional, Gram, Jørgen, additional, Schröder, Winnie, additional, Koessling, Manuela, additional, Wulff, Karin, additional, Wehnert, Manfred, additional, Herrmann, FalkoH., additional, Fouéré, S., additional, Guibal, F., additional, Morel, P., additional, Gou, D., additional, Naipal, A., additional, and Reitsma, P.H., additional

Published
1996
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33. A de novo translocation 46,X,t(X;15) causing haemophilia B in a girl: a case report.

Author

Schröder, Poetsch, Gazda, Werner, Reichelt, Knoll, Rokicka-Milewska, Zieleniewska, Herrmann, and Schröder, Winnie

Subjects
HEMOPHILIA, TURNER'S syndrome, X chromosome
Abstract

Haemophilia B is an X-linked recessive bleeding disorder caused by mutations in the factor IX gene with an incidence of 1:25 000–30 000. Usually female carriers are clinically normal, and severe phenotypic expression of the disease in females is extremely rare. In this report we describe a girl with a clinically severe course of haemophilia B who had no signs of Turner syndrome or any other dysmorphic features. Cytogenetic and molecular studies in the patient and her parents showed a de novo translocation 46,X,t(X;15)(q27.1;p11.2) in the patient, indicating a possible break near the factor IX gene. The structurally normal X chromosome was late replicating and inactivated in all metaphases as shown by high-resolution R-banding. By fluorescence in situ hybridization (FISH) with YAC and cosmid probes we could further characterize the breakpoint region on the X chromosome and the involvement of the factor IX gene. [ABSTRACT FROM AUTHOR]

Published
1998
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34. Prevalence of eight molecular markers associated with thrombotic diseases in six Amerindian tribes and two African groups of Costa Rica

Author

Herrmann, Falko H., Salazar‐Sánchez, Lizbeth, Schuster, Gudrun, Jiménez‐Arce, Gerardo, Grimm, Rita, Gomez, Xinia, Chavez, Mario, Wulff, Karin, and Schröder, Winnie

Abstract

Individuals belonging to six different Amerindian tribes and two African groups of Costa Rica were genotyped for factor V Leiden (FV), factor V haplotype HR2 (FV HR2), Factor II 20210G>A (FII), the methylenetetrahydrofolate reductase (MTHFR), factor VII polymorphisms (FVII IVS7, FVII R353Q), factor XIII (FXIII V34L), and the insertion/deletion (I/D) polymorphism of the gene of angiotensin converting enzyme (ACE). Clear differences in the prevalence were found and are first reported. The prevalence of some of the established genetic risk factors was low in Amerindians of Costa Rica (ACE) or even absent (FVL, FII), and others (MTHFR, FVHR2) had an extremely high prevalence. People of African origin carried very rare FVL or FII polymorphisms, but the DD genotype of ACE is the highest reported. Concerning the protective factors, the QQ genotype of FVII R353Q was absent in Amerindians, but the protective 7/7 genotype of FVII IVS7 frequently found. Novel alleles of FVII IVS7 (4, 8, and 9 monomers) were found. Intertribal heterogeneity was observed that may reflect the evolutionary history of these tribal groups and their admixture with other populations. Am. J. Hum. Biol. 16:82–86, 2004. © 2003 Wiley‐Liss, Inc.

Published
2004
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35. Platelet receptor and clotting factor polymorphisms as genetic risk factors for thromboembolic complications in heparininduced thrombocytopenia

Author

Carlsson, Lena E., Lubenow, Norbert, Blumentritt, Carmen, Kempf, Reiner, Papenberg, Stephanie, Schröder, Winnie, Eichler, Petra, Herrmann, Falko H., Santoso, Sentot, and Greinacher, Andreas

Abstract

Heparininduced thrombocytopenia HIT is an immune mediated adverse reaction to heparin treatment often associated with limb andor lifethreatening thromboembolic complications TECs. Presently, no prognostic marker has been identified that allows differentiation between mildly isolated thrombocytopenia and severely TECs affected patients. This study assesses the impact of platelet glycoprotein and clotting factor polymorphisms in HITpatients with isolated thrombocytopenia compared to HITpatients with TECs. Sixtythree HITpatients with isolated thrombocytopenia and 79 HITpatients with HITrelated TECs were genotyped for GPIIbIIIa polymorphisms HPA1, HPA3, GPIaIIa polymorphisms HPA5, GPIaC807T, GPIbIXV polymorphisms HPA2, Kozak5, VNTR, and clotting factor polymorphisms FVLeiden R506Q, prothrombin PTG20210A and MTHFR C677T. Women more often presented with TECs than men P0.04. No differences in genotype frequencies could be seen on comparing HITpatients with and without TECs. Analysing men and women separately, the C allele of the Kozak polymorphism was overrepresented in men who developed TECs P0.034. The enhanced risk of women to develop HITassociated TECs remains unexplained but it is potentially important in view of recent data on sexhormone related changes of haemostasis. There was no correlation between platelet glycoprotein and clotting factor polymorphisms and the risk to develop HITassociated TECs. An association between the development of TECs and the Kozak5C allele could be seen among male patients. However, this would need to be assessed in further larger studies. Most likely, the high levels of thrombin generation during acute HIT are so procoagulant that less pronounced risk factors such as polymorphisms are overshadowed.

Published
2003
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37. High mutation detection rates in cerebral cavernous malformation upon stringent inclusion criteria: one-third of probands are minors

Author

Spiegler, Stefanie, Najm, Juliane, Liu, Jian, Gkalympoudis, Stephanie, Schröder, Winnie, Borck, Guntram, Brockmann, Knut, Elbracht, Miriam, Fauth, Christine, Ferbert, Andreas, Freudenberg, Leonie, Grasshoff, Ute, Hellenbroich, Yorck, Henn, Wolfram, Hoffjan, Sabine, Hüning, Irina, Korenke, G. Christoph, Kroisel, Peter M., Kunstmann, Erdmute, Mair, Martina, Munk-Schulenburg, Susanne, Nikoubashman, Omid, Pauli, Silke, Rudnik-Schöneborn, Sabine, Sudholt, Irene, Sure, Ulrich, Tinschert, Sigrid, Wiednig, Michaela, Zoll, Barbara, Ginsberg, Mark H., and Felbor, Ute

Subjects
10. No inequality, 3. Good health
Abstract

Molecular genetics & genomic medicine : MGGM 2(2), 176-185 (2014). doi:10.1002/mgg3.60, Published by Wiley, Chichester

41. Platelet receptor and clotting factor polymorphisms as genetic risk factors for thromboembolic complications in heparin-induced thrombocytopenia.

Author

Carlsson LE, Lubenow N, Blumentritt C, Kempf R, Papenberg S, Schröder W, Eichler P, Herrmann FH, Santoso S, and Greinacher A

Subjects
Amino Acid Substitution, Gene Frequency, Humans, Minisatellite Repeats genetics, Mutation, Missense, Platelet Membrane Glycoproteins genetics, Polymerase Chain Reaction, Risk Factors, Anticoagulants adverse effects, Blood Coagulation Factors genetics, Heparin adverse effects, Platelet Glycoprotein GPIb-IX Complex genetics, Polymorphism, Genetic genetics, Thrombocytopenia chemically induced, Thrombocytopenia genetics
Abstract

Heparin-induced thrombocytopenia (HIT) is an immune mediated adverse reaction to heparin treatment often associated with limb- and/or life-threatening thromboembolic complications (TECs). Presently, no prognostic marker has been identified that allows differentiation between mildly (isolated thrombocytopenia) and severely (TECs) affected patients. This study assesses the impact of platelet glycoprotein- and clotting factor polymorphisms in HIT-patients with isolated thrombocytopenia compared to HIT-patients with TECs. Sixty-three HIT-patients with isolated thrombocytopenia and 79 HIT-patients with HIT-related TECs were genotyped for GPIIb-IIIa polymorphisms (HPA-1, HPA-3), GPIa-IIa polymorphisms (HPA-5, GPIaC807T), GPIb-IX-V polymorphisms (HPA-2, Kozak-5, VNTR), and clotting factor polymorphisms (FV-Leiden R506Q, prothrombin PT-G20210A and MTHFR C677T). Women more often presented with TECs than men (P = 0.04). No differences in genotype frequencies could be seen on comparing HIT-patients with and without TECs. Analysing men and women separately, the C allele of the Kozak polymorphism was overrepresented in men who developed TECs (P = 0.034). The enhanced risk of women to develop HIT-associated TECs remains unexplained but it is potentially important in view of recent data on sex-hormone related changes of haemostasis. There was no correlation between platelet glycoprotein- and clotting factor polymorphisms and the risk to develop HIT-associated TECs. An association between the development of TECs and the Kozak-5C allele could be seen among male patients. However, this would need to be assessed in further larger studies. Most likely, the high levels of thrombin generation during acute HIT are so procoagulant that less pronounced risk factors such as polymorphisms are overshadowed.

Published
2003
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