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6. Cytogenetic and molecular analyses of de novo translocation dic(9;13)(p11.2;p12) in an infertile male

Author

Wiland, E, Olszewska, M, Georgiadis, A, Huleyuk, N, Panasiuk, B, Zastavna, D, Yatsenko, SA, Jedrzejczak, P, Midro, AT, Yatsenko, AN, Kurpisz, M, Wiland, E, Olszewska, M, Georgiadis, A, Huleyuk, N, Panasiuk, B, Zastavna, D, Yatsenko, SA, Jedrzejczak, P, Midro, AT, Yatsenko, AN, and Kurpisz, M

Abstract

Background: Whole arm t(9;13)(p11;p12) translocations are rare and have been described only a few times; all of the previously reported cases were familial. Results: We present here an infertile male carrier with a whole-arm reciprocal translocation dic(9;13)(p11.2;p12) revealed by GTG-, C-, and NOR-banding karyotypes with no mature sperm cells in his ejaculate. FISH and genome-wide 400 K CGH microarray (Agilent) analyses demonstrated a balanced chromosome complement and further characterised the abnormality as a dicentric chromosome (9;13): dic(9;13)(pter→p11.2::p12→qter),neo(9) (pter→p12→neo→p11.2). An analysis of the patient's ejaculated cells identified immature germ cells at different phases of spermatogenesis but no mature spermatozoa. Most (82.5%) of the germ cells were recognised as spermatocytes at stage I, and the cell nuclei were most frequently found in pachytene I (41.8%). We have also undertaken FISH analysis and documented an increased rate of aneuploidy of chromosomes 15, 18, X and Y in the peripheral blood leukocytes of our patient. To study the aneuploidy risk in leukocytes, we have additionally included 9 patients with non-obstructive azoospermia with normal karyotypes. Conclusions: We propose that the azoospermia observed in the patient with the dic(9;13)(p11.2;p12) translocation was most likely a consequence of a very high proportion (90%) of association between XY bivalents and quadrivalent formations in prophase I. © 2014 Wiland et al.; licensee BioMed Central Ltd.

Published
2014

7. Wolf-Hirschhorn syndrome due to pure and translocation forms of monosomy 4p16.1 → pter

Author

Iwanowski, P, Panasiuk, B, Van Buggenhout, G, Murdolo, Marina, Myśliwiec, M, Maas, Nmc, Lattante, Serena, Korniszewski, L, Posmyk, R, Pilch, J, Zajączek, S, Fryns, J, Zollino, Marcella, Midro, At, Lattante, Serena (ORCID:0000-0003-2891-0340), Zollino, Marcella (ORCID:0000-0003-4871-9519), Iwanowski, P, Panasiuk, B, Van Buggenhout, G, Murdolo, Marina, Myśliwiec, M, Maas, Nmc, Lattante, Serena, Korniszewski, L, Posmyk, R, Pilch, J, Zajączek, S, Fryns, J, Zollino, Marcella, Midro, At, Lattante, Serena (ORCID:0000-0003-2891-0340), and Zollino, Marcella (ORCID:0000-0003-4871-9519)

Abstract

The aim of this study was to obtain a quantitative definition of Wolf-Hirschhorn syndrome (WHS) through systematic phenotypic analyses in a group of six children with 4p15.32 → pter, 4p15.33 → pter, or 4p16.1 → pter monosomy (considered together as M4p16.1). These results were used for evaluation of the phenotypic effects of a double chromosome imbalance in one child with 4p16.1 → pter monosomy and additional 11q23.3 → qter trisomy. Children with pure M4p16.1 presented with a total of 227 clinical and morphological traits, of which 119 were positive in at least two of them. These traits overlap to a great extent with clinical criteria defining the WHS phenotype. Among the 103 traits identified in the child with unbalanced translocation der(4)t(4;11)(p16.1;q23.3), most clinical and developmental traits (but only 11 morphological) were found to be shared by WHS children with pure M4p16.1 and at least one reported patient with pure 11q trisomy. Forty-six traits of this child corresponded solely to those identified in at least one child with pure M4p16.1. Only five traits of the hybrid phenotype were present in at least one child with pure distal 11q trisomy but in none of the present children with pure M4p16.1. In conclusion, most of the morphological traits of the hybrid phenotype in the child with der(4)t(4;11)(p16.1;q23.3) can be attributed to the M4p16.1, whereas their overlap with those associated with pure distal 11q trisomy is less evident. Phenotype analyses based on the same systematic data acquisition may be useful in understanding the phenotypic effects of different chromosome regions in complex rearrangements. © 2011 Wiley-Liss, Inc.

Published
2011

9. Interstitial deletion 9q22.32-q33.2 associated with additional familial translocation t(9;17)(q34.11;p11.2) in a patient with Gorlin-Goltz syndrome and features of Nail-Patella syndrome

Author

Midro, A.T., Panasiuk, B., Tümer, Zeynep A, Stankiewicz, P., Silahtaroglu, Asli Nilüfer, Lupski, J.R., Zemanova, Z., Stasiewicz-Jarocka, B., Hubert, E., Tarasow, E., Famulski, W., Zadrozna-Tolwinska, B., Wasiliewska, E., Kirchhoff, M., Kalscheuer, V.M., Michalova, K., Tommerup, Niels, Midro, A.T., Panasiuk, B., Tümer, Zeynep A, Stankiewicz, P., Silahtaroglu, Asli Nilüfer, Lupski, J.R., Zemanova, Z., Stasiewicz-Jarocka, B., Hubert, E., Tarasow, E., Famulski, W., Zadrozna-Tolwinska, B., Wasiliewska, E., Kirchhoff, M., Kalscheuer, V.M., Michalova, K., and Tommerup, Niels

Published
2004

11. Maternal Inheritance in Hybrids of Three Honey Bee Subspecies

Author

Węgrzynowicz Paweł, Gerula Dariusz, Tofilski Adam, Panasiuk Beata, and Bieńkowska Małgorzata

Subjects
bee queens, hybrids, maternal inheritance, morphometric analysis, subspecies, wing venation, Zoology, QL1-991
Abstract

The identification of honey bee (Apis mellifera) subspecies is often based on the measurements of workers’ fore-wings. The interpretation of the measurements can be difficult because the phenotype of workers is affected by both genetic and environmental factors. Moreover, it is not clear how the phenotype is affected by maternal inheritance. We have used the methodology of geometric morphometrics to verify if hybrids of honey bee subspecies and their backcrosses are more similar to either the father or mother colony. The comparison was based on fore-wing venation of three honey bee subspecies: A. m. carnica, A. m. caucasica, A. m. mellifera. First generation hybrids and backcrosses of those subspecies were obtained through instrumental insemination. Workers of the hybrids were compared with their parental colonies. The shape of wing venation was more similar to the maternal than to parental colony. This phenomenon was particularly visible in first generation of hybrids but it was also present in backcrosses. There were also symptoms of genetic dominance of some subspecies but this effect interacted with maternal inheritance and was difficult to interpret.

Published
2019
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13. Balling Behavior of Workers Toward Honey Bee Queens Returning from Mating Flights

Author

Gerula Dariusz, Panasiuk Beata, Bieńkowska Małgorzata, and Węgrzynowicz Paweł

Subjects
balling of queens, mating flights, queen losses, Zoology, QL1-991
Abstract

During natural mating honeybee queens can get lost due to drifting, predators or other cases. In this work, the balling of queens returning from flights by worker bees originating from the same colony was observed. Three subspecies of bees Carniolan, Caucasian and European Black Bee were tested. Research was conducted in both spring and summer, but in the former in newly created colonies, while in the latter in new and earlier used ones. Generally 15.2% of queens were balled and in total 30.2% of queens were lost during mating flights. 269 queens performed 785 mating flights, and 5.2% of those finished with balling. Three times more queens were balled when returning from mating flight rather than orientation flight. Subspecies matches or mismatches of queens and workers in nucleuses did not significantly affect the balling or its frequency. Additionally, no bee subspecies characterized stronger tendencies to ball a queen. Worker bees from newly created nucleuses treated queens similarly to the ones in nucleuses earlier used. However, significantly more queens had been balled during the spring in comparison to summer. There were days with higher balling of queens. During some days the weather was very unstable and unpredictable with such anomalies as heat waves, thunderstorms or sudden drops in insolation. Most of the queens were balled at the entrance while returning from flight and only a few inside the hive. In the research, clear causes of balling were not found, but some factors can be excluded.

Published
2018
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14. Translocation form of Wolf-Hirschhorn syndrome -- assessment of recurrence rate probability.

Author

Panasiuk, B., Leśniewicz, R., SpóŁczyńska, A., Myśliwiec, M., De Die Smulders, Ch., Sawicka, A., and Midro, A. T.

Subjects
*SYNDROMES in children, *PREGNANCY, *MISCARRIAGE, *RECURSIVE sequences (Mathematics), *CHROMOSOMAL translocation, *CYTOGENETICS, *PRENATAL diagnosis, *WOLF-Hirschhorn syndrome
Abstract

Purpose: The families experienced by occurrence of child with Wolf-Hirschhorn syndrome (WHS: OMIM # 194190) and by other unfavourable pregnancy outcomes (miscarriages or stillbirths/early deaths and partial trisomy 4p imbalance leading to intellectual disability in live born progeny) are asking for genetic counseling. In order to obtain the recurrence probability rates for the particular forms of unfavourable pregnancy we collected the empirical data and evaluated pedigrees of reciprocal chromosome translocations (RCT) carriers involving 4p. Results were applied to family of carrier of t(4;11)(p16.1;q23.3) ascertained by four miscarriages, in which latter the girl with WHS was born. Material and methods: Total empirical data about 170 pregnancies of 46 carriers were collected from 25 pedigrees RCT at risk for single segment imbalance. Classification was based mostly on cytogenetic methods. The probability rates of particular type of pathology related to total number of pregnancies after ascertainment correction have been calculated according to the method of Stengel-Rutkowski and Stene. Results: The risk figures for unbalanced offspring after 2:2 disjunction and adjacent-1 segregation for whole group of pedigrees were calculated as 15.2±3.5% (16/105), for unbalanced fetuses at second trimester of prenatal diagnosis as 50±13.4% (7/14), for miscarriages about 19±3.8% (20/105) and for stillbirths/early death as 15.2±3.5% (16/105). The higher probability rate for RCT carriers at risk for distal 4p -- shorter segment imbalance (28.6±12%, 4/14) in comparison to the rate for proximal (medium) one as 15.4±4.5% (10/65) and to more proximal (longer) one as 7.7±5.2% (2/26) were found. Conclusions: Our results confirm that the recurrence probability rates are different for particular categories of unfavourable pregnancy outcomes and dependent on size and genetic content of unbalanced 4p segments. [ABSTRACT FROM AUTHOR]

Published
2007

15. Hygienic Behaviour of Honeybee Colonies with Different Levels of Polyandry and Genotypic Composition

Author

Gerula Dariusz, Węgrzynowicz Paweł, Panasiuk Beata, Bieńkowska Małgorzata, and Skowronek Wojciech

Subjects
genetic diversity, genotypic variation, hygienic behaviour, instrumental insemination, Zoology, QL1-991
Abstract

Honey bee queens were inseminated with diluted, homogenised semen collected from a few dozen drones. This procedure was carried out to increase the diversity of the queens’ offspring, which is in comparison to the offspring of queens inseminated with semen from only a few drones coming from one colony. Queens and drones were mated within carniolan bee (Apis mellifera carnica) subspecies, but 3 selected lines were used. Queens were reared from one line and drones from the same line, and two additional lines differing in hygienic behaviour wherein in one of them that trait was strongly evident. The aim of this study was to examine whether the level of enhanced genetic variability in colonies and simultaneously the participation of hygienic bees, would increase the performance of hygienic behaviour. Overall hygienic behaviour of colonies with a lower and greater genetic variability did not differ significantly and amounted to 52.1 and 47.0%, respectively. Colonies within the lower variability group, in which drones from line selected in hygienic behaviour performance were used for inseminating queens, had a significantly greater percent of cleaned pupae than other colonies (63.2%). Hygienic behaviour in other colonies was more dependent on the gene quotas of hygienic bees in the colonies rather than on the level of polyandry.

Published
2015
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16. Performance of Bee Colonies Headed by Queens Instrumentally Inseminated with Semen of Drones Who Come from a Single Colony or Many Colonies

Author

Gerula Dariusz, Węgrzynowicz Paweł, Panasiuk Beata, Bieńkowska Małgorzata, and Skowronek Wojciech

Subjects
genetic diversity, honey yield, instrumental insemination, polyandry, wintering, Zoology, QL1-991
Abstract

The aim of the study was to determine the effect of honey bee worker diversity within the colony on: development, honey productivity, and wintering. Two different levels of diversity within the colony were tested. The appropriate levels of diversity within the colony were obtained by selecting drones for inseminating the queens. Lower genetic diversity was obtained in the colonies headed by a queen inseminated with semen collected from drones originating from a single colony. Higher genetic diversity was obtained in the colonies with queens inseminated with semen from drones of 30 different colonies. Colonies with a higher genetic variation of workers in the colonies had greater levels of functional characteristics. However, apart from the number of dead bees in winter, the genetic diversity level of the workers on the colony development and honey production, did not have a significant influence. There was an averaging effect observed concerning that male component in the colonies with a higher genetic variation of workers - on honey yield, when compared to the non-additive effect of the best drones.

Published
2014
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17. Causes and Scale of Winter Flights in Honey Bee (Apis Mellifera Carnica ) Colonies

Author

Węgrzynowicz Paweł, Gerula Dariusz, Bieńkowska Małgorzata, and Panasiuk Beata

Subjects
bees fallen as debris, bees flying out in winter, colony overwintering, nosema spp., varroa destructor, winter losses of bees, Zoology, QL1-991
Abstract

Winter honey bee losses were evaluated during the two overwintering periods of 2009/2010 and 2010/2011. The research included dead bee workers that fell on the hive bottom board (debris) and the ones that flew out of the hive. Differences were observed in the number of bees fallen as debris between the two periods, whereas the number of bees flying out was similar in both years. No differences were found between the numbers of dead bees in strong and weak colonies. The percentage of bees flying out of the colony increased in the presence of Nosema spores, Varroa infestation, increased average air temperature, and insolation during the day. In addition, both the presence of Nosema and insolation during the day had an impact on the number of bees that died and fell on the hive board.

Published
2014
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18. Susceptibility of Bee Larvae to Chalkbrood in Relation to Hygienic Behaviour of Worker Bees in Colonies of Chosen Races of Honeybee (Apis Mellifera )

Author

Panasiuk Beata, Bieńkowska Małgorzata, Gerula Dariusz, and Węgrzynowicz Paweł

Subjects
ascosphaera apis, freeze-killed brood, hygienic behaviour, larvae susceptibility, Zoology, QL1-991
Abstract

The susceptibility of bee larvae to Ascosphaera apis infestation and the hygienic behaviour of worker bees in relation to A. apis infected and freeze-killed brood were evaluated in three races of bees: Apis mellifera carnica, Apis mellifera caucasica, and Apis mellifera mellifera. Experimental bee colonies were evaluated in field conditions during the three beekeeping seasons. The lowest percentage of infected larvae was observed in car GR1 and mel A colonies (8.5% and 15%, respectively) and the highest in car Mr and cau P colonies (21% and 24.3%, respectively). Bees in the car GR1 and mel A colonies removed mummified brood in a shorter period of time (6.5 and 7.1 days on average, respectively) than car Mr and cau P colonies (above 8 days). Bees in the mel A and car GR1 colonies cleaned significantly more cells with freeze-killed brood within 24 and 48 hours (above 70% and 80% on average, respectively) than car Mr and cau P colonies (on average 10 - 20% lower cleaning rate). A low correlation coefficient was found for the susceptibility of larvae to A. apis infection and hygienic behaviour.

Published
2014
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22. Looking for ' the best bee ' An experiment about interactions between origin and environment of honey bee strains in Europe

Author

Meixner, M., Buchler, R., Costa, C., Andonov, S., Bienkowska, M., Bouga, M., Filipi, J., Hatjina, F., Evgeniya N. Ivanova, Kezic, N., Kryger, P., Conte, Y. L., Panasiuk, B., Petrov, P., Ruottinen, L., Uzunov, A., Wilde, J., LLH Bieneninstitut Kirchhain, Consiglio per la Ricerca e Sperimentazione in Agricoltura, Faculty for Agricultural Science and Food, Partenaires INRAE, Research Institute of Horticulture, Laboratory of Agricultural Zoology and Entomology, Agricultural University of Athens, University of Applied Sciences, Hellenic Agricultural Organization Demeter (HAO Demeter), Agricultural University [Plovdiv], Faculty of Agriculture [Zagreb] (UNIZG), University of Zagreb, Research Centre Flakkebjerg, Abeilles & Environnement (UR 406 ), Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Agrifood Research Finland, and University of Warmia and Mazury

Subjects
[SDV]Life Sciences [q-bio], fungi, behavior and behavior mechanisms
Abstract

International audience; The honey bee Apis mellifera, of which there are currently 28 identified subspecies and numerous ecotypes, have been evolving and adapting to a wide range of environments for hundreds of thousands of years within their native range of Europe, Africa and Asia. Honey bees have been widely dispersed over the past several hundred years and are now also established in the Americas and Australia. Today, the high loss of colonies worldwide is attributed to a combination of factors, including parasitic mites, pathogens, pesticides and malnutrition. The COLOSS network of European scientists asks the questions: Does beekeeper selection for productivity lead to genetic deficiency, and are locally adapted populations being displaced by the movement of various honey bee types to locations beyond their native range? A major research effort explores these questions, looking at numerous types of honey bees that are endemic to specific areas of Europe or have become adapted after several decades of breeding. Beekeepers in the U.S. also consider these questions through interest in locally adapted bees and “survivor” feral bees, although the situation is very different. Our honey bees are not native and were derived from relatively small founder populations, thus we lack the evolutionary diversity of subspecies and ecotypes that exist in Europe. We also lack the strong support of institutions and beekeeper organizations devoted to the selection and maintenance of specific subspecies, as established in many European countries. Feral populations in the U.S., previously considered a mixed source of raw genetic variation, have been devastated by the impact of Varroa mites. Through semen collections from Old World sources, Washington State University has been involved in the importation and distribution of additional honey bee genetic diversity in the U.S. Associated with the importations, cryopreserved germplasm from “pure” Old World subspecies has been deposited in the WSU Germplasm Repository for future breeding and conservation needs.Through such measures, we hope to enhance domestic bee breeding programs by providing additional genetic diversity to improve bee health in the U.S.

26. Global climate change and the economy.

Author

Panasiuk, B. Y.

Subjects
CLIMATE change, ECONOMICS, ENVIRONMENTAL economics
Abstract

Copyright of Ekonomika APK is the property of Economy of Argo-Industrial Complex and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2015

27. Evaluation of Suppressed Mite Reproduction (SMR) Reveals Potential for Varroa Resistance in European Honey Bees ( Apis mellifera L.).

Author

Mondet F, Parejo M, Meixner MD, Costa C, Kryger P, Andonov S, Servin B, Basso B, Bieńkowska M, Bigio G, Căuia E, Cebotari V, Dahle B, Dražić MM, Hatjina F, Kovačić M, Kretavicius J, Lima AS, Panasiuk B, Pinto MA, Uzunov A, Wilde J, and Büchler R

Abstract

In the fight against the Varroa destructor mite, selective breeding of honey bee ( Apis mellifera L.) populations that are resistant to the parasitic mite stands as a sustainable solution. Selection initiatives indicate that using the suppressed mite reproduction (SMR) trait as a selection criterion is a suitable tool to breed such resistant bee populations. We conducted a large European experiment to evaluate the SMR trait in different populations of honey bees spread over 13 different countries, and representing different honey bee genotypes with their local mite parasites. The first goal was to standardize and validate the SMR evaluation method, and then to compare the SMR trait between the different populations. Simulation results indicate that it is necessary to examine at least 35 single-infested cells to reliably estimate the SMR score of any given colony. Several colonies from our dataset display high SMR scores indicating that this trait is present within the European honey bee populations. The trait is highly variable between colonies and some countries, but no major differences could be identified between countries for a given genotype, or between genotypes in different countries. This study shows the potential to increase selective breeding efforts of V. destructor resistant populations.

Published
2020
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28. Two unrelated families with variable expression of Fraser syndrome due to the same pathogenic variant in the FRAS1 gene.

Author

Midro AT, Stasiewicz-Jarocka B, Borys J, Hubert E, Skotnicka B, Hassmann-Poznańska E, Sierpińska T, Panasiuk B, Schanze D, and Zenker M

Subjects
Abnormalities, Multiple genetics, Adult, Female, Fraser Syndrome genetics, Humans, Infant, Newborn, Male, Pedigree, Phenotype, Pregnancy, Prognosis, Young Adult, Abnormalities, Multiple pathology, Extracellular Matrix Proteins genetics, Fraser Syndrome pathology, Mutation
Abstract

We report on two unrelated families of Polish origin with variable expression of Fraser syndrome (FS; MIM#219000) due to homozygosity for the same pathogenic variant, c.6963_6964dup, of FRAS1. In one family, the disorder presented with perinatal and prenatal lethality. One affected female from family 2 who was followed-up for 32 years, represented a relatively favorable long-term outcome. She displayed the typical craniofacial dysmorphism, including right cryptophthalmos, cutaneous syndactyly, abnormalities of the stomathognatic system, bilateral atresia of the external ear canals resulting in conductive hearing loss, and malformations of the larynx, spleen, kidney, and genitourinary tract. Her intellectual capacities were normal. Our observations illustrate that expression and severity of FS, even when caused by the same pathogenic variant, may be quite different ranging from a lethal disorder to a condition with multiple physical malformations but normal psychomotor development. In addition, we propose that the FRAS1 c.6963_6964dup variant may be a founder mutation in the Polish population. Therefore, it would be reasonable to test specifically for this variant first in any FS1 patient of Polish ancestry., (© 2020 Wiley Periodicals, Inc.)

Published
2020
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29. Neurodevelopmental disorder with dysmorphic facies and distal limb anomalies syndrome due to disruption of BPTF in a 35-year-old man initially diagnosed with Silver-Russell syndrome.

Author

Midro AT, Tommerup N, Borys J, Panasiuk B, Kosztyła-Hojna B, Zalewska R, Konstantynowicz J, Łebkowska U, Cooper L, Scherer SE, Mehrjouy MM, Liu Q, Skowroński R, and Stankiewicz P

Subjects
Adult, Diagnosis, Differential, Humans, Male, Musculoskeletal Abnormalities diagnosis, Musculoskeletal Abnormalities genetics, Radiography, Syndrome, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Facies, Neurodevelopmental Disorders diagnosis, Neurodevelopmental Disorders genetics, Phenotype, Silver-Russell Syndrome diagnosis
Published
2019
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30. A 23-year follow-up of a male with Hajdu-Cheney syndrome due to NOTCH2 mutation.

Author

Midro AT, Stasiewicz-Jarocka B, Borys J, Kozłowski K, Skotnicka B, Tarasów E, Hubert E, Konstantynowicz J, Panasiuk B, Rydzanicz M, Pollak A, Stawiński P, Skowroński R, and Płoski R

Subjects
Adolescent, Adult, Base Sequence, Child, DNA Mutational Analysis, Disease Progression, Follow-Up Studies, Hajdu-Cheney Syndrome diagnostic imaging, Humans, Male, Phenotype, Young Adult, Hajdu-Cheney Syndrome genetics, Mutation genetics, Receptor, Notch2 genetics
Abstract

We present a natural history of a 32-year-old man with Hajdu-Cheney syndrome (HJCYS), because of the de novo truncating mutation in the exon 34 of NOTCH2 (c.6424-6427delTCTG, p.Ser2142ArgfsX4), who has been followed up for a period of 23 years (between 9 and 32 years). During follow-up, we observed abnormalities of vision, hearing, voice, and progression of craniofacial features in the form of skeletal dysplasia with affected skull, dentition, spine, limbs, fingers, and toes. Low bone mineral density and history of fragility fractures also suggested primary osteoporosis being a clinical manifestation. According to Stengel-Rutkowski, Schimanek, and Wernheimer (1984; Human Genetics, 6, 272-295), systematic data acquisition has been used for quantitative analysis of anthropological, radiographic, and clinical features at childhood, adolescence, and young adulthood separately. A detailed phenotype description together with the results of reanalysis of 14 reports so far published on patients with HJCYS and NOTCH2 mutation showed similar phenotype evolution with age. The spectrum of observed features may improve diagnostic tools for HJCYS at different periods of the lifespan., (© 2018 Wiley Periodicals, Inc.)

Published
2018
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31. Clonal chromosomal aberrations in Philadelphia negative cells such as monosomy 7 and trisomy 8 may persist for years with no impact on the long term outcome in patients with chronic myeloid leukemia.

Author

Wasilewska EM, Panasiuk B, Gniot M, Sawicka A, Kozłowska K, Lewandowski K, Kłoczko J, and Midro AT

Subjects
Aged, Chromosome Deletion, Chromosomes, Human, Pair 7 genetics, Chromosomes, Human, Pair 8 genetics, Clone Cells, Cytogenetic Analysis, Female, Humans, Male, Middle Aged, Treatment Outcome, Leukemia, Myelogenous, Chronic, BCR-ABL Positive genetics, Leukemia, Myelogenous, Chronic, BCR-ABL Positive pathology, Philadelphia Chromosome, Trisomy genetics
Abstract

The appearance of clonal chromosomal aberrations in Philadelphia negative cells (CCA/Ph-) during the treatment of chronic myeloid leukemia (CML) was recently confirmed. Importance of these findings has not been clearly defined. We present data on the time of appearance, persistence, size of the CCA/Ph- clone in terms of drugs used and hematological, cytogenetic and molecular response rates. The focus was on the peripheral blood cytopenias and myelodysplastic changes in the bone marrow microscopic evaluation. In 5 out of 155 (3,2%) CML patients, the persistent presence (up to nine years) of CCA/Ph- was found (monosomy 7 and trisomy 8 in unrelated clones in two patients treated with tyrosine kinase inhibitors; trisomy 8 in two patients on imatinib; trisomy 21 in one patient on interferon alfa treatment). Aberrations were present in median 24% Ph- cells in 3-15 subsequent analyses at different cytogenetic and molecular response time points. No evident myelodysplastic changes nor transformation to MDS/AML occurred in patients with CCA/Ph-. All the patients achieved major molecular response (MMR). It seems that CCA/Ph- presence does not affect the long term outcome in patients with chronic myeloid leukemia. Further complex monitoring of the CML patients with CCA/Ph- is still needed., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published
2017
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32. An Exploration of the Associations Among Hearing Loss, Physical Health, and Visual Memory in Adults From West Central Alabama.

Author

Hay-McCutcheon MJ, Hyams A, Yang X, Parton J, Panasiuk B, Ondocsin S, James MM, and Scogin F

Subjects
Adult, Aged, Aged, 80 and over, Alabama epidemiology, Auditory Threshold, Disability Evaluation, Educational Status, Female, Hearing Tests, Humans, Male, Middle Aged, Neuropsychological Tests, Rural Population, Urban Population, Young Adult, Health Status, Hearing Loss epidemiology, Hearing Loss psychology, Memory, Visual Perception
Abstract

Purpose: The purpose of this preliminary study was to explore the associations among hearing loss, physical health, and visual memory in adults living in rural areas, urban clusters, and an urban city in west Central Alabama., Method: Two hundred ninety-seven adults (182 women, 115 men) from rural areas, urban clusters, and an urban city of west Central Alabama completed a hearing assessment, a physical health questionnaire, a hearing handicap measure, and a visual memory test., Results: A greater number of adults with hearing loss lived in rural areas and urban clusters than in an urban area. In addition, poorer physical health was significantly associated with hearing loss. A greater number of individuals with poor physical health who lived in rural towns and urban clusters had hearing loss compared with the adults with other physical health issues who lived in an urban city. Poorer hearing sensitivity resulted in poorer outcomes on the Emotional and Social subscales of the Hearing Handicap Inventory for Adults. And last, visual memory, a working-memory task, was not associated with hearing loss but was associated with educational level., Conclusions: The outcomes suggest that hearing loss is associated with poor physical and emotional health but not with visual-memory skills. A greater number of adults living in rural areas experienced hearing loss compared with adults living in an urban city, and consequently, further research will be necessary to confirm this relationship and to explore the reasons behind it. Also, further exploration of the relationship between cognition and hearing loss in adults living in rural and urban areas will be needed.

Published
2017
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33. Limited survivability of unbalanced progeny of carriers of a unique t(4;19)(p15.32;p13.3): a study in multiple generations.

Author

Šumanović-Glamuzina D, Lozić B, Iwanowski PS, Zemunik T, Bilinovac Z, Stasiewicz-Jarocka B, Panasiuk B, and Midro AT

Abstract

Background: Carriership of a reciprocal chromosomal translocation (RCT) involving the short arm of chromosome 4 (4p) may result in birth of a child with Wolf-Hirschhorn syndrome (WHS) due to monosomy 4p, a priori modified by the impact of the partner chromosome imbalance. Familial transmission studies of RCT enable obtaining empirical risk figures that are essential for genetic counseling. In this study, pedigree data from carriers of a unique t(4;19)(p15.32;p13.3), ascertained by two children with WHS phenotype, were collected through five generations and empirical risk for different pregnancy outcomes was assessed. In addition, the phenotype-karyotype correlation was studied in two unbalanced children against the phenotypes of children (literature data) with pure monosomy 4p15.32 → pter and pure trisomy 19p13.3 → pter, accordingly. The phenotype analysis was conducted using the catalogue of traits according to the Munich Dysmorphology Database. Pedigree segregation analysis was conducted by the direct method according to Stengel- Rutkowski et al., Results: A double segment imbalance, trisomy 19p13.3 → pter with monosomy 4p15.32 → pter, was diagnosed in WHS progeny at birth. No essential modification of WHS phenotype by the additional trisomy 19p was observed, except for a limited survivability (death in infancy). Pedigree segregation analysis covered 39 relatives showed the probability rate for liveborn with unbalanced karyotype of 3.7 ± 3.6% (1/27), for stillbirth/neonatal death at 7.4 ± 5.0% (2/27), for miscarriage at 22.2 ± 8.0% (6/27), for the chance of having a baby without unbalanced karyotype was estimated at 66.7 ± 9.1% (18/27). In addition, the value of 7.4% for genetic counseling for any carrier of RCT at risk for single segment 19p13.3 → pter imbalance at birth was evaluated as such value have not been estimated so far., Conclusion: Carriership of a t(4;19)(p15.32;p13.3) is at low risk for an unbalanced child at birth and for stillbirth/neonatal death but high for miscarriages. The chance of having a baby without unbalanced karyotype was estimated to be high. Monosomy 4p15.32 → pter together with trisomy 19p13.3 → pter as a double segment imbalance in children with WHS may be connected with a limited survivability in infancy.

Published
2017
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34. Meiotic and pedigree segregation analyses in carriers of t(4;8)(p16;p23.1) differing in localization of breakpoint positions at 4p subband 4p16.3 and 4p16.1.

Author

Midro AT, Zollino M, Wiland E, Panasiuk B, Iwanowski PS, Murdolo M, Śmigiel R, Sąsiadek M, Pilch J, and Kurpisz M

Subjects
Adult, Chromosome Breakpoints, Female, Genetic Counseling, Heterozygote, Humans, In Situ Hybridization, Fluorescence, Karyotyping, Male, Pedigree, Spermatozoa pathology, Trisomy genetics, Wolf-Hirschhorn Syndrome genetics, Wolf-Hirschhorn Syndrome pathology, Chromosome Segregation genetics, Chromosomes, Human, Pair 4 genetics, Meiosis genetics, Translocation, Genetic genetics
Abstract

Purpose: The purpose of this study was to compare meiotic segregation in sperm cells from two carriers with t(4;8)(p16;p23.1) reciprocal chromosome translocations (RCTs), differing in localization of the breakpoint positions at the 4p subband-namely, 4p16.3 (carrier 1) and 4p16.1 (carrier 2)-and to compare data of the pedigree analyses performed by direct method., Methods: Three-color fluorescent in situ hybridization (FISH) on sperm cells and FISH mapping for the evaluation of the breakpoint positions, data from pedigrees, and direct segregation analysis of the pedigrees were performed., Results: Similar proportions of normal/balanced and unbalanced sperm cells were found in both carriers. The most common was an alternate type of segregation (about 52 % and about 48 %, respectively). Unbalanced adjacent I and adjacent II karyotypes were found in similar proportions about 15 %. The direct segregation analysis (following Stengel-Rutkowski) of the pedigree of carriers of t(4;8)(p16.1;p23.1) was performed and results were compared with the data of the pedigree segregation analysis obtained earlier through the indirect method. The probability of live-born progeny with unbalanced karyotype for carriers of t(4;8)(p16.1;p23.1) was moderately high at 18.8 %-comparable to the value obtained using the indirect method for the same carriership, which was 12 %. This was, however, markedly lower than the value of 41.2 % obtained through the pedigree segregation indirect analysis estimated for carriers of t(4;8)(p16.3;p23.1), perhaps due to the unique composition of genes present within the 4p16.1-4p 16.3 region., Conclusions: Revealed differences in pedigree segregation analysis did not correspond to the very similar profile of meiotic segregation patterns presented by carrier 1 and carrier 2. Most probably, such discordances may be due to differences in embryo survival rates arising from different genetic backgrounds.

Published
2016
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35. Co-segregation of Freiberg's infraction with a familial translocation t(5;7)(p13.3;p22.2) ascertained by a child with cri du chat syndrome and brachydactyly type A1B.

Author

Myśliwiec M, Panasiuk B, Dębiec-Rychter M, Iwanowski PS, Łebkowska U, Nowakowska B, Marcinkowska A, Stankiewicz P, and Midro AT

Subjects
Adolescent, Brachydactyly diagnosis, Child, Cri-du-Chat Syndrome diagnosis, Facies, Fatal Outcome, Female, Humans, Osteochondritis diagnosis, Osteochondritis genetics, Phenotype, Radiography, Spine abnormalities, Spine diagnostic imaging, Brachydactyly genetics, Chromosomes, Human, Pair 5, Chromosomes, Human, Pair 7, Cri-du-Chat Syndrome genetics, Metatarsus abnormalities, Osteochondritis congenital, Translocation, Genetic
Abstract

The identification of chromosomal breakpoints in association with human abnormal phenotypes can enable elucidation of gene function. We report on epiphyseal aseptic necrosis of the lesser head of the second metatarsal bone, known as Freiberg's infraction (FI), in two female carriers of the apparently balanced t(5;7)(p13.3;p22.2) ascertained by a 16-year-old girl with cri-du-chat syndrome and unusual skeletal features in association with an unbalanced translocation der(5) t(5;7)(p13.3;p22.2). Mapping of the chromosome breakpoints using fluorescent in situ hybridization (FISH) narrowed them to the coding sequence of ADAMTS12 on chromosome 5p13.3 and SDK1 on 7p22.2. In addition, several skeletal abnormalities classified as brachydactyly type A1B (BDA1B) were present in the proband and in both carriers of t(5;7)(p13.3;p22.2), suggesting a potential role of ADAMTS12 in the development of the BDA1B observed in this family.

Published
2015
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36. [Systemic sclerosis. Part 2. Epigenetic factors in the pathogenesis of clinical manifestations].

Author

Fryc J, Midro AT, Panasiuk B, and Sierakowski S

Subjects
Genes, Regulator genetics, Humans, RNA, Messenger genetics, DNA Methylation, Epigenesis, Genetic, Scleroderma, Systemic genetics
Abstract

Systemic sclerosis is a complex autoimmune disease characterized by immune activation, fibrosis of the skin and internal organs and vasculopathy affecting predominantly the microvessels with a predilection for women. The genetic background of systemic sclerosis is still full of unanswered questions, with classical genetics able to explain only some systemic sclerosis cases. Novel advances concerning epigenetics give us new insight into pathogenesis of systemic sclerosis. This review focuses on results of recent reports on epigenetic modifications of the gene functions and X inactivation changes in pathogenesis of systemic sclerosis. Current evidence demonstrates DNA heavy methylation (FLI1, NOS3, BMPRII) and hypomethylation of regulatory genes (CD40L, CD70), histone code modifications, abnormal expression of large spectrum of microRNAs.

Published
2015

37. Recurrence risks for different pregnancy outcomes and meiotic segregation analysis of spermatozoa in carriers of t(1;11)(p36.22;q12.2).

Author

Midro AT, Panasiuk B, Stasiewicz-Jarocka B, Olszewska M, Wiland E, Myśliwiec M, Kurpisz M, Shaffer LG, and Gajecka M

Subjects
Abortion, Habitual pathology, Adult, Chromosome Segregation, Chromosomes, Human, Pair 1 genetics, Chromosomes, Human, Pair 11 genetics, Female, Humans, Hydrocephalus pathology, In Situ Hybridization, Fluorescence, Karyotyping, Male, Meningomyelocele physiopathology, Pedigree, Pregnancy, Spermatozoa pathology, Abortion, Habitual genetics, Hydrocephalus genetics, Meningomyelocele genetics, Pregnancy Outcome, Translocation, Genetic genetics
Abstract

Cumulative data obtained from two relatively large pedigrees of a unique reciprocal chromosomal translocation (RCT) t(1;11)(p36.22;q12.2) ascertained by three miscarriages (pedigree 1) and the birth of newborn with hydrocephalus and myelomeningocele (pedigree 2) were used to estimate recurrence risks for different pregnancy outcomes. Submicroscopic molecular characterization by fluorescent in situ hybridization (FISH) of RCT break points in representative carriers showed similar rearrangements in both families. Meiotic segregation patterns after sperm analysis by three-color FISH of one male carrier showed all possible outcomes resulting from 2:2 and 3:1 segregations. On the basis of empirical survival data, we suggest that only one form of chromosome imbalance resulting in monosomy 1p36.22→pter with trisomy 11q12.2→qter may be observed in progeny at birth. Segregation analysis of these pedigrees was performed by the indirect method of Stengel-Rutkowski and showed that probability rate for malformed child at birth due to an unbalanced karyotype was 3/48 (6.2±3.5%) after ascertainment correction. The risk for stillbirths/early neonatal deaths was -/48 (<1.1%) and for miscarriages was 17/48 (35.4±6.9%). However, the probability rate for children with a normal phenotype at birth was 28/48 (58.3±7.1%). The results obtained from this study may be used to determine the risks for the various pregnancy outcomes for carriers of t(1;11)(p36.22;q12.2) and can be used for genetic counseling of carriers of this rearrangement.

Published
2014
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38. Cytogenetic and molecular analyses of de novo translocation dic(9;13)(p11.2;p12) in an infertile male.

Author

Wiland E, Olszewska M, Georgiadis A, Huleyuk N, Panasiuk B, Zastavna D, Yatsenko SA, Jedrzejczak P, Midro AT, Yatsenko AN, and Kurpisz M

Abstract

Background: Whole arm t(9;13)(p11;p12) translocations are rare and have been described only a few times; all of the previously reported cases were familial., Results: We present here an infertile male carrier with a whole-arm reciprocal translocation dic(9;13)(p11.2;p12) revealed by GTG-, C-, and NOR-banding karyotypes with no mature sperm cells in his ejaculate. FISH and genome-wide 400 K CGH microarray (Agilent) analyses demonstrated a balanced chromosome complement and further characterised the abnormality as a dicentric chromosome (9;13): dic(9;13)(pter→p11.2::p12→qter),neo(9)(pter→p12→neo→p11.2). An analysis of the patient's ejaculated cells identified immature germ cells at different phases of spermatogenesis but no mature spermatozoa. Most (82.5%) of the germ cells were recognised as spermatocytes at stage I, and the cell nuclei were most frequently found in pachytene I (41.8%). We have also undertaken FISH analysis and documented an increased rate of aneuploidy of chromosomes 15, 18, X and Y in the peripheral blood leukocytes of our patient. To study the aneuploidy risk in leukocytes, we have additionally included 9 patients with non-obstructive azoospermia with normal karyotypes., Conclusions: We propose that the azoospermia observed in the patient with the dic(9;13)(p11.2;p12) translocation was most likely a consequence of a very high proportion (90%) of association between XY bivalents and quadrivalent formations in prophase I.

Published
2014
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39. [Probability rate of unbalanced offspring at birth and risk of unfavorable pregnancy outcomes in families of carriers of chromosomal reciprocal translocations involving chromosome 7].

Author

Kozłowska K, Panasiuk B, Stasiewicz-Jarocka B, Lurie IW, Chrzanowska K, Lenkiewicz M, Gutkowska A, Iliszko M, and Midro AT

Subjects
Adult, Congenital Abnormalities mortality, Fathers, Female, Genetic Predisposition to Disease, Humans, Male, Mothers, Pedigree, Pregnancy, Probability, Stillbirth epidemiology, Survival Rate, Abortion, Habitual genetics, Chromosomes, Human, Pair 7, Congenital Abnormalities genetics, Genetic Carrier Screening, Stillbirth genetics, Translocation, Genetic
Abstract

Introduction: Carriership of reciprocal chromosomal translocation (RCT) may be the reason the occurrence of congenital malformations in the offspring, early neonatal death, stillbirth, and recurrent miscarriages due to unbalanced karyotype of gametes. The probability rate for individual categories of unfavorable outcomes depends on the kind of chromosome involved and is individually variable., Objectives: The aim of study was to estimate the probability rates for unbalanced offspring and to evaluate the risk for different categories of unfavorable pregnancy outcomes, depending on the size of chromosomal segment with differentiation between maternal/paternal origin of the reciprocal chromosomal translocations involving chromosome 7p (RCT-7p) and 7q (RCT-7q). In addition, the use of the obtained results has been illustrated by the example of a family with unique RCT t(7;9)(p21.3,p23)., Material and Methods: Empirical and cytogenetic data on 341 pregnancies and offspring of 133 carriers were collected from 69 pedigrees of carriers of RCT-7p and RCT-7q at risk for a single 7 segment imbalance. The probability rates of particular form of pregnancy pathology have been calculated according to the method of Stengel-Rutkowski and Stene, including all forms of meiotic segregation and their survival rates after fertilization to term childbirth., Results: The probability rates for unbalanced offspring for carriers of RCT-7p after 2:2 disjunction and adjacent-1 segregation were calculated as 5.5% +/- 2.2% (6/108); for maternal (MAT) and paternal (PAT) carriers were about < 1% (0/56) and 13.6 +/- 5.2% (6/44) (p = 0.04) respectively. Considering different segment lengths of 7p, the following values for shorter and longer segments were obtained: 23.0 +/- 11.7% (3/13) for 7p21-->pter; 3.3 +/- 3.3% (1/30) for 7p 14-->pter and 3.1 +/- 2.1% (2/65) for 7p 1-->pter The risk figures for stillbirth/earl neonatal death were estimated at 2.8 +/- 1.6% (3/108), but for miscarriage were calculated at 25.9 +/- 4.2% (28/108) for carriers RCT-7p. The probability rates for unbalanced offspring at birth for carriers of RCT-7q were calculated as 2.7 +/- 1.5% (3/111); for MAT and PAT carriers were 3.5 +/- 2.0% (3/86) and < 2.6% (0/19) respectively. Considering different segment lengths of 7q, the following values for shorter and longer segments were obtained: 6.2 +/- 6.1% (1/16) for 7q33-->qter; 5.3 +/- 3.6% (2/38) for 7q32-->qter and < 0.82% (0/57) for 7q11-->qter. The risk figures for stillbirth/early neonatal death were estimated at 9.9 +/- 2.8% (11/111), but for miscarriage were calculated at 34.2 +/-4.5% (38/111) for carriers RCT-7q. The probability estimated values for unbalanced fetuses, evaluated prenatally in the second trimester of pregnancy for carriers of RCT-7p and RCT-7q were similar i.e. 41.7 +/- 14.2% (5/12) and 46.7 +/-12.9% (7/15), respectively., Conclusions: 1. The probability rates for unbalanced offspring and the risk values for individual categories of unfavorable outcomes for carriers of RCT-7 are different and depend on the size of chromosome 7 segment involved in RCT 2. The probability rate for unbalanced offspring for paternal carriers of RCT-7p is higher than for maternal carriers (p = 0.04). 3. It is suggested that the probability rate for unbalanced offspring for maternal carriers of RCT-7q may be higher than for paternal carriers.

Published
2013
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40. Chromatin structure analysis of spermatozoa from reciprocal chromosome translocation (RCT) carriers with known meiotic segregation patterns.

Author

Olszewska M, Fraczek M, Huleyuk N, Czernikiewicz A, Wiland E, Boksa M, Zastavna D, Panasiuk B, Midro AT, and Kurpisz M

Subjects
Adult, Chromomycin A3, Chromosome Segregation, Chromosomes, Human genetics, DNA Fragmentation, Humans, In Situ Hybridization, Fluorescence, Male, Meiosis, Middle Aged, Chromatin ultrastructure, Chromosome Aberrations, Haploidy, Spermatozoa ultrastructure, Translocation, Genetic
Abstract

The presence of reciprocal chromosome translocations (RCTs), as well as sperm chromatin disturbances, is known to exert negative influence on male fertility. The aim of this study was to identify an association between chromosome structural rearrangements in male RCT carriers and sperm seminological parameters (concentration, motility, morphology), chromatin status (fragmentation and maturity), meiotic segregation pattern and observed chromosomal hyperhaploidy. Sperm samples originated from ten male RCT carriers with reproductive failure/success. TUNEL assay (DNA fragmentation) and chromomycin A3 (CMA3)/aniline blue (AB) staining (chromatin maturity) were used to analyze sperm chromatin status while fluorescent in situ hybridization (FISH) was applied to observe meiotic segregation patterns and hyperhaploidy in spermatozoa. We found that the mean level of sperm DNA fragmentation in the RCT carrier group (18.0 ± 11.9%) was significantly higher (p=0.0006) than the mean of the control group (7.5 ± 4.3%). There was no correlation observed between sperm DNA fragmentation levels (5.6-38.0%) and the frequency of genetically normal/balanced gametes (34.3-62.4%), sperm seminological quality or revealed reproductive failure. In contrast, a correlation between the frequencies of genetically normal/balanced spermatozoa and of gametes with mature chromatin was observed (CMA3: R=0.4524, p=0.2604; AB: R=0.5238, p=0.1827). A statistically significant increase in the hyperhaploidy level of selected chromosomes in all analyzed RCT carriers was documented but was not correlated to sperm seminology or fertility status. Further evaluation and additional assays toward sperm chromatin quality assessment in RCT carriers is suggested to explain the complexity of genomic structural rearrangements and its possible relevance to reproductive success or failure., (Copyright © 2013 Society for Biology of Reproduction & the Institute of Animal Reproduction and Food Research of Polish Academy of Sciences in Olsztyn. Published by Elsevier Urban & Partner Sp. z o.o. All rights reserved.)

Published
2013
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41. [Risk estimation of different pregnancy outcomes in the families of carriers of reciprocal chromosomal translocations involving chromosome 20].

Author

Stasiewicz-Jarocka B, Kozaczuk M, Panasiuk B, Jamsheer A, Latos-Bieleńska A, and Midro AT

Subjects
Female, Humans, Male, Pregnancy, Probability, Translocation, Genetic genetics, Chromosome Disorders diagnosis, Chromosome Disorders genetics, Chromosomes, Human, Pair 20 genetics, Pedigree, Pregnancy Outcome, Prenatal Diagnosis methods, Risk Assessment methods
Abstract

Unlabelled: Carriership of reciprocal chromosome translocation (RCT) in a family may be the reason for malformation at birth, stillbirth, early neonatal death, and miscarriage due to unbalanced karyotype (monosomy/trisomy). The size of chromosome segments determined by the breakpoint position, kind of chromosome involved and the carrier gender may influence the probability rate for each category of the unfavorable pregnancy outcome in the family of the carrier of a particular RCT Until now, the literature lacks reports on the risk values for particular forms of pregnancy outcomes in case of single segment imbalance, both the short (p) and the long arm (q) of chromosome 20., Objective: The aim of the study was to evaluate individual risk rates for unbalanced offspring at birth for single segment imbalance in the form of trisomy/monosomy and a separate evaluation risk figures for different pregnancy outcomes, depending on the size of the involved chromosome segment, its origin and carrier gender in families of RCT carriers involving chromosome 20 (RCT-20). In addition, practical application of the obtained results in the family with unique RCT t(13;20)(q14.1;p11.21) carriership has been shown., Material and Methods: Total empirical data of 50 families (219 pregnancies) were collected from 19 pedigrees of RCT-20 carriers coming from different collections of RCT and available references. Cytogenetic studies were performed by GTG technique. The probability rates of particular type of pathology related to the total number of pregnancies after ascertainment correction have been done by segregation analysis according to the method of Stengel-Rutkowski and Stene., Results: The probability rate for unbalanced offspring at birth for carriers of RCT-20p was calculated as 5.5 +/- 1.8% (9/164) (medium risk). Considering parental gender of the carrier for maternal (MAT) and paternal (PAT) carriers, the probability rate values were similar i.e. 4.8 +/- 2.3% (4/84) and 4.9 +/- 2.8% (3/61), respectively. The risk figures for stillbirth/early neonatal deaths were found as 0.6 +/- 0.6% (1/164) (low risk), but separately for MAT and PAT carriers they were: 1.2 +/- 1.2% (1/84) and < 0.8% (-/61), respectively. Risk figures for miscarriages were estimated as 28.6 +/- 3.5% (47/164) (high risk), with 32.1 +/- 5.1% (27/84) for maternal carriers and 32.7 +/- 6% (20/61) for paternal carriers. The risk figures for unbalanced offspring at birth for carriers of RCT-20q were calculated as about 2.6% (0/20) (low risk), for stillbirth/early neonatal death about 2.6% (-/20) (low risk) and for miscarriage 50 +/- 11.2% (10/20) (high risk)., Conclusions: 1. The probability rates for unbalanced offspring at birth and for different categories of unfavorable outcomes show differences depending on the origin and the size of chromosome 20 segment. 2. There are no differences in the value of risk figures for particular form of pregnancy pathology in relation to carrier's gender.

Published
2013
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42. [Systemic sclerosis. Part 1: searching for genetic determinants].

Author

Midro AT, Panasiuk B, Fryc J, Stasiewicz-Jarocka B, and Sierakowski S

Subjects
Disease Progression, Genetic Predisposition to Disease, Humans, Mosaicism, Polymorphism, Genetic, Scleroderma, Systemic genetics
Abstract

Familial aggregation of systemic sclerosis observed in the 1970 of twenty century, the presence of karyotype instability and chromosomal mosaicism and positive associations of certain polymorphisms of genes located in specific regions of the human genome may indicate the important contribution of genetic factors in the development and progression of the disease. The purpose of this paper is to present data on genetic changes found in scleroderma. Despite the enormous progress of research it is not yet clear, which disturbances in a specific way determine onset and development of the disease and which are non-specific forms of molecular abnormalities also present in other diseases with similar clinical symptoms.

Published
2012

43. Wolf-Hirschhorn syndrome due to pure and translocation forms of monosomy 4p16.1 → pter.

Author

Iwanowski PS, Panasiuk B, Van Buggenhout G, Murdolo M, Myśliwiec M, Maas NM, Lattante S, Korniszewski L, Posmyk R, Pilch J, Zajączek S, Fryns JP, Zollino M, and Midro AT

Subjects
Child, Child, Preschool, Chromosome Banding, Chromosomes, Human, Pair 11, Female, Humans, Infant, Male, Phenotype, Trisomy, Chromosome Deletion, Chromosomes, Human, Pair 4 genetics, Translocation, Genetic, Wolf-Hirschhorn Syndrome genetics
Abstract

The aim of this study was to obtain a quantitative definition of Wolf-Hirschhorn syndrome (WHS) through systematic phenotypic analyses in a group of six children with 4p15.32 → pter, 4p15.33 → pter, or 4p16.1 → pter monosomy (considered together as M4p16.1). These results were used for evaluation of the phenotypic effects of a double chromosome imbalance in one child with 4p16.1 → pter monosomy and additional 11q23.3 → qter trisomy. Children with pure M4p16.1 presented with a total of 227 clinical and morphological traits, of which 119 were positive in at least two of them. These traits overlap to a great extent with clinical criteria defining the WHS phenotype. Among the 103 traits identified in the child with unbalanced translocation der(4)t(4;11)(p16.1;q23.3), most clinical and developmental traits (but only 11 morphological) were found to be shared by WHS children with pure M4p16.1 and at least one reported patient with pure 11q trisomy. Forty-six traits of this child corresponded solely to those identified in at least one child with pure M4p16.1. Only five traits of the hybrid phenotype were present in at least one child with pure distal 11q trisomy but in none of the present children with pure M4p16.1. In conclusion, most of the morphological traits of the hybrid phenotype in the child with der(4)t(4;11)(p16.1;q23.3) can be attributed to the M4p16.1, whereas their overlap with those associated with pure distal 11q trisomy is less evident. Phenotype analyses based on the same systematic data acquisition may be useful in understanding the phenotypic effects of different chromosome regions in complex rearrangements. © 2011 Wiley-Liss, Inc., (Copyright © 2011 Wiley-Liss, Inc.)

Published
2011
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44. Genetic counseling in Robertsonian translocations der(13;14): frequencies of reproductive outcomes and infertility in 101 pedigrees.

Author

Engels H, Eggermann T, Caliebe A, Jelska A, Schubert R, Schüler HM, Panasiuk B, Zaremba J, Latos-Bieleńska A, Jakubowski L, Zerres KP, Schwanitz G, and Midro AT

Subjects
Female, Fertilization in Vitro, Genetic Counseling, Humans, Karyotyping, Pedigree, Pregnancy, Pregnancy Outcome, Abortion, Spontaneous genetics, Chromosomes, Human, Pair 13 genetics, Chromosomes, Human, Pair 14 genetics, Infertility genetics, Stillbirth genetics, Translocation, Genetic
Abstract

Robertsonian translocations 13/14 are the most common chromosome rearrangements in humans. However, most studies aimed at determining risk figures are more than 20 years old. Their results are often contradictory regarding important topics in genetic counseling such as infertility and unfavorable pregnancy outcomes. Here, we present a study on a sample of 101 previously unreported pedigrees of der(13;14)(q10;q10). In order to minimize problems of partial ascertainment, we included families with a wide range of reasons of ascertainment such as birth of a child with congenital anomalies, prenatal diagnosis due to maternal age, fertility problems and recurrent pregnancy loss. No evidence of increased infertility rates of female and male carriers was found. The detected miscarriage frequency of female carriers was higher than previously reported (27.6 +/- 4.0% of all spontaneous pregnancies). This may be explained by an over-correction of earlier studies, which excluded all unkaryotyped miscarriages. In three out of 42 amniocenteses, translocation trisomies 13 were diagnosed (7.1 +/- 4.0% of all amniocenteses). The frequency of stillbirths was 3.3 +/- 1.6% for female carriers and 1.4 +/- 1.4% for male carriers. A low risk for the live birth of translocation trisomy 13 children was confirmed since no live born children with trisomy 13 or Pätau syndrome were detected in the ascertainment-corrected sample., (2008 Wiley-Liss, Inc.)

Published
2008
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45. [Probability rates for different pregnancy outcomes in carriers of reciprocal chromosomal translocations involving chromosome 13].

Author

Panasiuk B, Dawidowska WK, Stasiewicz-Jarocka B, Lurie IW, and Midro AT

Subjects
Abnormalities, Multiple genetics, Abortion, Spontaneous genetics, Adult, Chromosome Mapping, Female, Humans, Poland, Pregnancy, Pregnancy Outcome epidemiology, Probability, Risk Assessment statistics & numerical data, Statistics as Topic, Stillbirth genetics, Chromosomes, Human, Pair 13, Genetic Carrier Screening, Heterozygote, Pregnancy Outcome genetics
Abstract

Objectives: The aim of study was to estimate the probability rates for unfavorable pregnancy outcomes in carriers of reciprocal chromosomal translocations involving 13 chromosome (RCT-13q)., Material and Methods: We collected total empirical data about 232 pregnancies of 56 carriers coming from 28 pedigrees. RCT classification was based on classic cytogenetic methods for interpretation of breakpoint position. The probability rates of particular type of pathology related to the total number of pregnancies after ascertainment correction have been calculated with the help of Stengel-Rutkowski and Stene method., Results: The risk figures for unbalanced offspring after 2:2 disjunction and adjacent-1 segregation for the whole group of pedigrees were calculated as 5.2 +/- 1.7% (9/173)--medium risk, for maternal (MAT) and paternal (PAT) carriers were about 6.2 +/- 2.3% (7/173) and 4.8 +/- 3.3% (2/42) respectively. Considering different segment lengths of 13q, similar values for shorter and longer segments were obtained [4.3 +/- 1.9% (5/115) for 13q21-->qter and 7.0 +/- 3.3% (4/58) for 13q12-->qter]. The risk figures for miscarriages as 36.4 +/-3.6% (63/173) and for stillbirths/early death as 4.6 +/- 31.6% (8/173) were obtained. The risk figures for unbalanced offspring after 3:1 disjunction were calculated as 7.7 +/- 7.45 (9/13)., Conclusions: 1. Risk figures for different pregnancy outcomes are differ among particular forms of pathology. 2. Probability rate for unbalanced progeny at birth was calculated as a medium risk and similar values for carriers of different segments of 13q were obtained. 3. Probability rate for miscarriages was high but risk for stillbirths/early deaths of newborn was low. 4. No differences in values of rate for particular forms of pathology were found for maternal and paternal carriers of RCT-13q.

Published
2008

46. Increase in expression of monocytic tissue factor (CD142) with monocytes and blood platelet activation in liver cirrhosis.

Author

Panasiuk A, Zak J, Panasiuk B, and Prokopowicz D

Subjects
Adult, Case-Control Studies, Female, Humans, Inflammation blood, Liver Cirrhosis, Alcoholic physiopathology, Male, Middle Aged, Liver Cirrhosis, Alcoholic blood, Liver Cirrhosis, Alcoholic metabolism, Monocytes metabolism, Platelet Activation immunology, Thromboplastin metabolism
Abstract

Tissue factor (TF) is one of the proteins that participate in hemostatic and inflammatory processes. Activated monocytes present in the liver increase expression of TF, and while accumulating in the organ they can intensify inflammation. The aim of the present study was to evaluate the expression of TF on monocytes in advanced liver cirrhosis with regard to other activation markers. The flow cytometric analysis of TF (CD142), CD14, adhesive molecules CD11b and CD11c, costimulatory molecules CD40, CD80 and CD86, and HLA-DR on monocytes was carried out in 45 patients with postalcoholic liver cirrhosis (Child Pugh B, 20 patients; Child Pugh C, 25 patients) and in 25 healthy persons. The positive correlation between monocytic TF expression and monocyte [soluble CD14 (sCD14), CD11b, monocyte aggregates] activation, the expression of costimulatory molecules on monocytes (CD40, CD80), blood platelet (soluble P-selectin, microplatelets) activation, the level of tumor necrosis factor-alpha, biochemical parameters of liver damage (alanine aminotransferase, aspartate aminotransferase, alkaline phosphate, gamma-glutamyltransferase, and bilirubin) as well as coagulation disorders were observed in the study. In conclusion, the study revealed that the activation of monocytes and blood platelets is accompanied by the elevation of monocytic TF expression in advanced liver cirrhosis. The monocytic TF is a significant link connecting clotting processes and inflammatory and immunological phenomena in liver cirrhosis.

Published
2007
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47. The analysis of meiotic segregation patterns and aneuploidy in the spermatozoa of father and son with translocation t(4;5)(p15.1;p12) and the prediction of the individual probability rate for unbalanced progeny at birth.

Author

Wiland E, Midro AT, Panasiuk B, and Kurpisz M

Subjects
Abortion, Habitual genetics, Aged, Female, Humans, Male, Pregnancy, Spermatozoa cytology, Aneuploidy, Chromosome Segregation genetics, Chromosomes, Human, Pair 4 genetics, Chromosomes, Human, Pair 5 genetics, Meiosis genetics, Translocation, Genetic genetics
Abstract

Reciprocal chromosomal translocations (RCT) have long been recognized as important etiological factors in reproductive failure. In the present study, the meiotic segregation patterns of the spermatozoa of two related t(4;5)(p15.1;p12) carriers (proband and his father) were compared to the empirical data from a three-generation pedigree for risk assessment. Cytogenetic analysis of the metaphase chromosomes was performed, and triple color fluorescence in situ hybridization (FISH) was applied to the sperm heads. Similar patterns of meiotic segregation were observed for both carriers, despite the finding of teratozoospermia in the proband but not in his father. In addition, an increase of aneuploidy in chromosome 15 in the proband and aneuploidy of chromosomes X and Y in the father were observed. The high rate of miscarriages (6/10 pregnancies and 4/7 pregnancies after ascertainment correction) in this family could be explained by the genetically unbalanced karyotype and fertilization mediated by the unbalanced spermatozoa observed for both men at a frequency of more than 60%. The risk assessment for unfavorable pregnancy outcomes was predicted as 1.6% for unbalanced progeny at birth and about 30% for miscarriage. These figures may be used as guidelines for the genetic counseling of families with similar RCT.

Published
2007
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48. Expression of p53, Bax and Bcl-2 proteins in hepatocytes in non-alcoholic fatty liver disease.

Author

Panasiuk A, Dzieciol J, Panasiuk B, and Prokopowicz D

Subjects
Adult, Apoptosis physiology, Female, Gene Expression, Humans, Male, Middle Aged, Proto-Oncogene Proteins c-bcl-2 metabolism, Fatty Liver metabolism, Hepatocytes metabolism, Tumor Suppressor Protein p53 metabolism, bcl-2-Associated X Protein metabolism
Abstract

Aim: To analyze the protein expression essential for apoptosis in liver steatosis., Methods: The expression of proapoptotic proteins p53, Bax, and antiapoptotic Bcl-2 in hepatocytes with steatosis (SH) and without steatosis (NSH) was evaluated in 84 patients at various stages of non-alcoholic fatty liver disease (NAFLD)., Results: Immunohistochemical staining of liver tissue showed the activation of p53 protein in SH and NSH with increased liver steatosis, diminished Bcl-2 and slightly decreased Bax protein. Positive correlation was found between the stage of liver steatosis with p53 expression in SH (r = 0.54, P < 0.01) and NSH (r = 0.49, P < 0.01). The antiapoptotic protein Bcl-2 was diminished together with the advancement of liver steatosis, especially in non-steatosed hepatocytes (r = 0.43, P < 001)., Conclusion: Apoptosis is one of the most important mechanisms leading to hepatocyte elimination in NAFLD. The intensification of inflammation in NAFLD induces proapoptotic protein p53 with the inhibition of antiapoptotic Bcl-2.

Published
2006
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49. Expression of beta2-integrin on leukocytes in liver cirrhosis.

Author

Panasiuk A, Zak J, Maciorkowska E, Panasiuk B, and Prokopowicz D

Subjects
Adult, Female, Granulocytes metabolism, Humans, Lymphocytes metabolism, Male, Middle Aged, Monocytes metabolism, CD18 Antigens metabolism, Integrin alpha Chains metabolism, Leukocytes metabolism, Liver Cirrhosis metabolism
Abstract

Aim: To analyze beta2-integrin expression on blood leukocytes in liver cirrhosis., Methods: In 40 patients with liver cirrhosis and 20 healthy individuals, the evaluation of expression of CD11a (LFA-1alpha), CD11b (Mac-1alpha), CD11c (alphaX) and CD49d (VLA-4alpha) on peripheral blood leukocytes was performed using flow cytometry. The analysis was carried out in groups of patients divided into B and C according to Child-Pugh's classification., Results: An increased CD11a, CD11b, CD11c and CD49d integrin expression was observed on peripheral blood leukocytes in liver cirrhosis. The integrin levels were elevated as the advancement of liver failure progressed. The highest expression of integrins occurred predominantly on monocytes. A slight expression of VLA-4 was found on lymphocytes and granulocytes and it increased together with liver failure. A positive correlation was noted between median intensity of fluorescence (MIF) expression on polymorphonuclear cells of CD11a and CD11c and CD49d (r = 0.42, P < 0.01; r = 053, P < 0.01, respectively) in liver cirrhosis stage C. However, no correlation was observed between integrin expression on leukocytes. The concentrations of sICAM-1, sVCAM-1, and TNFalpha, were significantly elevated in liver cirrhosis., Conclusion: beta2-integrin expression on leukocytes increases in liver cirrhosis decompensated as the stage of liver failure increases, which is a result of permanent activation of leukocytes circulating through the inflamed liver environment. beta2-integrin expression on circulating leukocytes can intensify liver cirrhosis.

Published
2006
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50. Risk evaluation of carriers with chromosome reciprocal translocation t(7;13)(q34;q13) and concomitant meiotic segregation analyzed by FISH on ejaculated spermatozoa.

Author

Midro AT, Wiland E, Panasiuk B, Leśniewicz R, and Kurpisz M

Subjects
Abortion, Spontaneous, Adult, Ejaculation, Fatal Outcome, Female, Heterozygote, Humans, In Situ Hybridization, Fluorescence, Infant, Newborn, Karyotyping, Male, Meiosis genetics, Models, Genetic, Pedigree, Pregnancy, Risk Factors, Spermatozoa cytology, Stillbirth, Chromosome Segregation genetics, Chromosomes, Human, Pair 13 genetics, Chromosomes, Human, Pair 7 genetics, Spermatozoa metabolism, Translocation, Genetic
Abstract

We performed the segregation analysis of a relatively large pedigree of t(7;13)(q34;q13) carriers together with the sperm karyotype analysis of the one carrier using a tri-color fluorescence in situ hybridization (FISH) method. The risk assessments for unfavorable pregnancy outcomes in a series of 36 pregnancies in eight reciprocal chromosome translocation (RCT) couples of carriers were estimated directly from a pedigree after ascertainment correction. The individual probability rate for unbalanced child was predicted according to Stengel-Rutkowski and co-workers. The unbalanced karyotypes in the form of monosomy 7q34-->qter and trisomy 13q13-->qter were detected among stillborn/early death newborns with holoprosencephaly (HPE), cyclopia and other malformations. Based on clinical description of unkaryotyped stillbirth progeny, it can be assumed that the phenotype distinctions were connected with the unbalanced karyotype from 2:2 segregation (monosomy 7q with trisomy 13q) and 3:1 segregation as interchange trisomy 13 (Patau syndrome). Probability rates for miscarriages, stillbirth/early death were 12.9 +/- 6% (4/31) and 29 +/- 8.2% (9/31), respectively. The results of the meiotic segregation pattern indicated the rate of unbalanced spermatozoa for about 60%, with the unusual high rate (29.4%) of 3:1 segregant (i.e., 13.4% of the tertiary segregation and 16% of the interchange segregation). Adjacent-1 segregation followed with 23.5% and adjacent-2 followed with 7.2% of analyzed spermatozoa. The high rate of unbalanced gametes in comparison to the number of stillborn/early death and miscarriages detected in pedigree suggests a strong selection against unbalanced chromosomal constitutions during fetal development. It corresponds to a very small probability rate (about 0.3%) of viable unbalanced progeny from 3:1 meiotic segregation predicted for maternal carriers. This knowledge can be used in genetic counseling of families with similar RCT ascertained in a different way., (2006 Wiley-Liss, Inc.)

Published
2006
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