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Dive into the research topics where Konrad Szymański is active.

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Featured researches published by Konrad Szymański.


Current Genomics | 2011

The Genetic Basis of Graves' Disease

Rafał Płoski; Konrad Szymański; Tomasz Bednarczuk

The presented comprehensive review of current knowledge about genetic factors predisposing to Graves’ disease (GD) put emphasis on functional significance of observed associations. In particular, we discuss recent efforts aimed at refining diseases associations found within the HLA complex and implicating HLA class I as well as HLA-DPB1 loci. We summarize data regarding non-HLA genes such as PTPN22, CTLA4, CD40, TSHR and TG which have been extensively studied in respect to their role in GD. We review recent findings implicating variants of FCRL3 (gene for FC receptor-like-3 protein), SCGB3A2 (gene for secretory uteroglobin-related protein 1- UGRP1) as well as other unverified possible candidate genes for GD selected through their documented association with type 1 diabetes mellitus: Tenr–IL2–IL21, CAPSL (encoding calcyphosine-like protein), IFIH1(gene for interferon-induced helicase C domain 1), AFF3, CD226 and PTPN2. We also review reports on association of skewed X chromosome inactivation and fetal microchimerism with GD. Finally we discuss issues of genotype-phenotype correlations in GD.


Journal of Human Genetics | 2017

Gender-dependent and age-of-onset-specific association of the rs11675434 single-nucleotide polymorphism near TPO with susceptibility to Graves’ ophthalmopathy

Aleksander Kuś; Konrad Szymański; Beata Jurecka-Lubieniecka; Edyta Pawlak-Adamska; Dorota Kula; Piotr Miśkiewicz; Marek Bolanowski; Rafał Płoski; Artur Bossowski; Jacek Daroszewski; Barbara Jarząb; Tomasz Bednarczuk

The role of TPO gene polymorphism in the susceptibility to Graves’ disease (GD) remains unclear. However, single-nucleotide polymorphisms (SNPs) near TPO have been recently associated with serum levels of thyroid peroxidase (TPO) antibody in two independent genome-wide association studies. Moreover, we have observed a strong association between the rs11675434 SNP located near TPO and the presence of clinically evident Graves’ ophthalmopathy (GO). The aim of the current study was to reevaluate and dissect this association in an extended group of 1231 well-characterized patients with GD (1043 adults and 188 children) and 1130 healthy controls from the Polish Caucasian population, considering possible gender-dependent and age-of-onset-specific effects of the studied SNP. We found that the T allele of rs11675434 was significantly more frequent in GD patients with than without GO (odds ratio (OR)=1.26, 95% confidence interval (CI)=1.05–1.51, P=0.012), which was consistent with our previous findings. Further analyses performed in subgroups of patients showed that the association with GO was significant in adult patients with age of GD onset ⩾45 years (OR=1.34, 95% CI=1.03–1.75, P=0.031), but not in children and adolescents or adult patients with earlier onset of the disease (OR=1.72, 95% CI=0.77–3.84, P=0.18 and OR=1.05, 95% CI=0.79–1.40, P=0.75, respectively). Moreover, a strong association with GO was present in males (OR=2.06, 95% CI=1.40–3.02, P=0.0002), whereas it was absent in females (OR=1.10, 95% CI=0.90–1.35, P=0.35). The results of our study further suggest that rs11675434 SNP located near TPO is associated with the development of GO, especially in males and patients with later age of GD onset.


Scientific Reports | 2018

Value of multilocus genetic risk score for atrial fibrillation in end-stage kidney disease patients in a Polish population

Bartłomiej Kisiel; Artur Bachta; Maria Franaszczyk; Dorota Brodowska-Kania; Wawrzyniec Żmudzki; Konrad Szymański; Antoni Sokalski; Wiesław Klatko; Marek Stopiński; Janusz Grochowski; Marek Papliński; Zdzisław Goździk; Longin Niemczyk; Barbara Bober; Maciej Kołodziej; Witold Tłustochowicz; Grzegorz Kamiński; Rafał Płoski; Stanisław Niemczyk

Genetic factors play a key role in the pathogenesis of atrial fibrillation (AF). We would like to establish an association between previously described single-nucleotide polymorphisms (SNPs) and AF in haemodialysed patients with end-stage kidney disease (ESKD-HD) as well as to assess the cumulative effect of all genotyped SNPs on AF risk. Sixteen SNPs were genotyped in 113 patients with AF-ESKD-HD and in 157 controls: without AF (NAF) and with ESKD-HD. The distribution of the risk alleles was compared in both groups and between different sub-phenotypes. The multilocus genetic risk score (GRS) was calculated to estimate the cumulative risk conferred by all SNPs. Several loci showed a trend toward an association with permanent AF (perm-AF): CAV1, Cx40 and PITX2. However, GRS was significantly higher in the AF and perm-AF groups, as compared to NAF. Three of the tested variables were independently associated with AF: male sex, history of myocardial infarction (MI) and GRS. The GRS, which combined 13 previously described SNPs, showed a significant and independent association with AF in a Polish population of patients with ESKD-HD and concomitant AF. Further studies on larger groups of patients are needed to confirm the associations.


Tissue Antigens | 2014

rs3827440, a nonsynonymous single nucleotide polymorphism within GPR174 gene in X chromosome, is associated with Graves' disease in Polish Caucasian population.

Konrad Szymański; Piotr Miśkiewicz; K. Pirko; B. Jurecka-Lubieniecka; D. Kula; K. Hasse-Lazar; Paweł Krajewski; Tomasz Bednarczuk; Rafał Płoski


Tissue Antigens | 2012

The replication of the association of the rs6832151 within chromosomal band 4p14 with Graves' disease in a Polish Caucasian population

Konrad Szymański; T. Bednarczuk; Paweł Krajewski; Rafał Płoski


Neuropsychobiology | 2015

Association between FKBP5 Functional Polymorphisms and Completed Suicide

Sylwia Fudalej; Maciej Kopera; Dorota Wołyńczyk-Gmaj; Marcin Fudalej; Pawe lstrok Krajewski; Krystyna Wasilewska; Konrad Szymański; Izabela Chojnicka; Anna Podgórska; Marcin Wojnar; Rafał Płoski


Clinical Endocrinology | 2015

The association of thyroid peroxidase antibody risk loci with susceptibility to and phenotype of Graves' disease

Aleksander Kuś; Konrad Szymański; Robin P. Peeters; Piotr Miśkiewicz; Eleonora Porcu; Giorgio Pistis; Serena Sanna; Silvia Naitza; Rafał Płoski; Marco Medici; Tomasz Bednarczuk


Tissue Antigens | 2011

Functionally defective germline variant of sialic acid acetylesterase (Met89Val) is not associated with type 1 diabetes mellitus and Graves' disease in a Polish population.

Konrad Szymański; Agata Skórka; A. Szypowska; Tomasz Bednarczuk; Rafał Płoski


Clinical Endocrinology | 2014

Increased concentration of T-cell receptor rearrangement excision circles (TREC) in peripheral blood in Graves' disease.

Katarzyna Strawa; Anna Markowska; Piotr Miśkiewicz; Aleksander Kuś; Urszula Ambroziak; Konrad Szymański; Renata Zbiec; Magdalena Spólnicka; Paweł Krajewski; Tomasz Bednarczuk; Rafał Płoski


Clinical Endocrinology | 2018

Paediatric-onset and adult-onset Graves’ disease share multiple genetic risk factors

Aleksander Kuś; Mikołaj Radziszewski; Aleksandra Glina; Konrad Szymański; Beata Jurecka-Lubieniecka; Edyta Pawlak-Adamska; Dorota Kula; Natalia Wawrusiewicz-Kurylonek; Joanna Kuś; Piotr Miśkiewicz; Rafał Płoski; Marek Bolanowski; Jacek Daroszewski; Barbara Jarząb; Artur Bossowski; Tomasz Bednarczuk

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Rafał Płoski

Medical University of Warsaw

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Tomasz Bednarczuk

Medical University of Warsaw

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Piotr Miśkiewicz

Medical University of Warsaw

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Aleksander Kuś

Medical University of Warsaw

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Paweł Krajewski

Medical University of Warsaw

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Artur Bossowski

Medical University of Białystok

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Jacek Daroszewski

Wrocław Medical University

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Marek Bolanowski

Wrocław Medical University

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