Your search keyword '"Stefanie, Kankel"' showing total 16 results

1. Small supernumerary marker chromosomes derived from human chromosome 11

Author

Thomas Liehr, Monika Ziegler, Luisa Person, Stefanie Kankel, Niklas Padutsch, Anja Weise, Jörg Paul Weimer, Heather Williams, Susana Ferreira, Joana B. Melo, and Isabel M. Carreira

Subjects

small supernumerary marker chromosomes (sSMCs), chromosome 11, triplosensitive genes, pericentric region, copy number variation (CNV), uniparental disomy (UPD), Genetics, QH426-470

Abstract

Introduction: With only 39 reported cases in the literature, carriers of a small supernumerary marker chromosome (sSMC) derived from chromosome 11 represent an extremely rare cytogenomic condition.Methods: Herein, we present a review of reported sSMC(11), add 18 previously unpublished cases, and closely review eight cases classified as ‘centromere-near partial trisomy 11’ and a further four suited cases from DECIPHER.Results and discussion: Based on these data, we deduced the borders of the pericentric regions associated with clinical symptoms into a range of 2.63 and 0.96 Mb for chromosome 11 short (p) and long (q) arms, respectively. In addition, the minimal pericentric region of chromosome 11 without triplo-sensitive genes was narrowed to positions 47.68 and 60.52 Mb (GRCh37). Furthermore, there are apparent differences in the presentation of signs and symptoms in carriers of larger sSMCs derived from chromosome 11 when the partial trisomy is derived from different chromosome arms. However, the number of informative sSMC(11) cases remains low, with overlapping presentation between p- and q-arm-imbalances. In addition, uniparental disomy (UPD) of ‘normal’ chromosome 11 needs to be considered in the evaluation of sSMC(11) carriers, as imprinting may be an influencing factor, although no such cases have been reported. Comprehensively, prenatal sSMC(11) cases remain a diagnostic and prognostic challenge.

Published

2023

2. Broad genomic workup including optical genome mapping uncovers a DDX3X: MLLT10 gene fusion in acute myeloid leukemia

Author

Verena Nilius-Eliliwi, Marco Tembrink, Wanda Maria Gerding, Krzystof P. Lubieniecki, Joanna M. Lubieniecka, Stefanie Kankel, Thomas Liehr, Thomas Mika, Fotios Dimopoulos, Konstanze Döhner, Roland Schroers, Hoa Huu Phuc Nguyen, and Deepak Ben Vangala

Subjects

acute myeloid leukemia, optical genome mapping, DDX3X, MLLT10, FLT3-ITD, SUZ12, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

In acute myeloid leukemia (AML), treatment decisions are currently made according to the risk classification of the European LeukemiaNet (ELN), which is based on genetic alterations. Recently, optical genome mapping (OGM) as a novel method proved to yield a genome-wide and detailed cytogenetic characterization at the time of diagnosis. A young female patient suffered from a rather unexpected aggressive disease course under FLT3 targeted therapy in combination with induction chemotherapy. By applying a “next-generation diagnostic workup“ strategy with OGM and whole-exome sequencing (WES), a DDX3X: MLLT10 gene fusion could be detected, otherwise missed by routine diagnostics. Furthermore, several aspects of lineage ambiguity not shown by standard diagnostics were unraveled such as deletions of SUZ12 and ARPP21, as well as T-cell receptor recombination. In summary, the detection of this particular gene fusion DDX3X: MLLT10 in a female AML patient and the findings of lineage ambiguity are potential explanations for the aggressive course of disease. Our study demonstrates that OGM can yield novel clinically significant results, including additional information helpful in disease monitoring and disease biology.

Published

2022

3. Small supernumerary marker chromosomes derived from chromosome 14 and/or 22

Author

Thomas Liehr, Heather E. Williams, Monika Ziegler, Stefanie Kankel, Niklas Padutsch, and Ahmed Al-Rikabi

Subjects

Small supernumerary marker chromosomes (sSMCs), Chromosome 14, Chromosome 22, Prenatal, Postnatal, Incidence, Genetics, QH426-470

Abstract

Abstract Small supernumerary marker chromosomes (sSMCs) are additional derivative chromosomes present in an otherwise numerically and structurally normal karyotype. They may derive from each of the 24 human chromosomes, and most contain a normal centromeric region with an alphoid sequence from a single chromosome. The majority of human chromosomes have a unique centromeric DNA-sequence enabling their indubitable characterization. However, chromosomes 14 and 22 share a common centromeric sequence D14/22Z1, and sSMCs with this DNA-stretch can derive from either chromosome. Euchromatin-carrying sSMCs(14 or 22) may be further characterized by molecular cytogenetics. However, in most diagnostic laboratories, heterochromatic sSMCs cannot be differentiated between chromosomes 14 or 22 derivation and are often reported as der(14 or 22). Still, heterochromatic sSMC(14 or 22) can be distinguished from each other using the D22Z4 probe (non-commercial) localized to 22p11.2. Herein, 355 sSMC(14 or 22) analyzed in the authors’ laboratory during the last ~ 20 years are summarized to address the questions: (1) What are the true frequencies of chromosome 14- and chromosome 22- derived sSMCs within D14/22Z1-positive cases? (2) Does sub-characterization of sSMC(14) and sSMC(22) make a difference in routine diagnostics? These questions could be answered as follows: (ad 1) within the studied group of sSMCs ~ 40% are derived from chromosome 14 and ~ 60% from chromosome 22; (ad 2) the knowledge on exact sSMC origin can help to save costs in routine diagnostics; i.e. in a clinically abnormal person with sSMC(14) a test for uniparental disomy is indicated, which is not necessary if a chromosome 22 origin for the sSMC was determined.

Published

2021

4. The acrocentric part of der(Y)t(Y;acro)(q12;p1?2) contains D15Z1 sequences in the majority of cases

Author

Sigrid Fuchs, Jasmin Lisfeld, Stefanie Kankel, Luisa Person, and Thomas Liehr

Subjects

Genetics, QH426-470, Life, QH501-531

Abstract

Infertility: The origin of a Y-chromosome abnormality Researchers in Germany have clarified the origin of an abnormality in the Y-chromosome linked with infertility. Some chromosome regions are susceptible to variation, such as translocation with segments of other chromosomes. A team of researchers led by Thomas Liehr of the Jena University Hospital, investigated a Y-chromosome abnormality in seven men. Visual analysis of the chromosomes of all seven showed an aberration at the tip of the long arm of the chromosome, probably derived from an exchange with another chromosome. The researchers then used fluorescent probes to characterize the Y-chromosome. A general probe that binds the short arm of any acrocentric chromosome (chrs. 13, 14, 15, 21, 22) generated a signal. Further testing with probes for specific chromosomes revealed that the aberrant region is derived predominantly from the short arm of chromosome 15.

Published

2021

5. Partial Reduction in BRCA1 Gene Dose Modulates DNA Replication Stress Level and Thereby Contributes to Sensitivity or Resistance

Author

Sandra Classen, Elena Rahlf, Johannes Jungwirth, Nina Albers, Luca Philipp Hebestreit, Alexandra Zielinski, Lena Poole, Marco Groth, Philipp Koch, Thomas Liehr, Stefanie Kankel, Nils Cordes, Cordula Petersen, Kai Rothkamm, Helmut Pospiech, and Kerstin Borgmann

Subjects

BRCA1, homologous recombination, DNA damage response, CHK1, replication stress, irradiation, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

BRCA1 is a well-known breast cancer risk gene, involved in DNA damage repair via homologous recombination (HR) and replication fork protection. Therapy resistance was linked to loss and amplification of the BRCA1 gene causing inferior survival of breast cancer patients. Most studies have focused on the analysis of complete loss or mutations in functional domains of BRCA1. How mutations in non-functional domains contribute to resistance mechanisms remains elusive and was the focus of this study. Therefore, clones of the breast cancer cell line MCF7 with indels in BRCA1 exon 9 and 14 were generated using CRISPR/Cas9. Clones with successful introduced BRCA1 mutations were evaluated regarding their capacity to perform HR, how they handle DNA replication stress (RS), and the consequences on the sensitivity to MMC, PARP1 inhibition, and ionizing radiation. Unexpectedly, BRCA1 mutations resulted in both increased sensitivity and resistance to exogenous DNA damage, despite a reduction of HR capacity in all clones. Resistance was associated with improved DNA double-strand break repair and reduction in replication stress (RS). Lower RS was accompanied by increased activation and interaction of proteins essential for the S phase-specific DNA damage response consisting of HR proteins, FANCD2, and CHK1.

Published

2022

6. First cytogenomic characterization of murine testis tumor cell line MLTC-1

Author

Shaymaa Azawi, Stefanie Kankel, Thomas Liehr, and Martina Rincic

Subjects

General Medicine

Abstract

The cell line MLTC-1 was established in 1982 as a transplantable Leydig cell tumor from a C57BL/6 mouse. The cell line has already been applied in >100 studies: still, the only information about its genetic content is given in the first description: MLTC-1 initially had a polyploid karyotype. Here, a molecular karyotyping and multicolor banding-based molecular cytogenetic study was done to provide the first chromosomal/ (molecular) cytogenetic characterization of MLTC-1. A hexaploid karyotype with 72 to 105 chromosomes was hereby characterized. Besides polyploidy, unbalanced two- and three-way translocations, dicentrics and one neocentric derivative were identified. Also, no Y-chromosome could be detected in this clearly male derived cell line. Overall, a completely unbalanced genome is present in MLTC-1 with ~20 regions being subject to copy number losses or gains. After translating these imbalances into the human genome in a standardized way, a 40% match of imbalances with human Leydig cell tumors was evident; however, about the same rate of concordance was detectable for human spermatocytic seminomas and non-seminomas as well as testicular germ cell tumor. Accordingly, MLTC-1 is better suited as an advanced testicular germ cell tumor model in general, rather than specifically for human Leydig cell tumors.

Published

2022

7. Early Bacterial Colonization and Antibiotic Resistance Gene Acquisition in Newborns

Author

Tilman E. Klassert, Cristina Zubiria-Barrera, Stefanie Kankel, Magdalena Stock, Robert Neubert, Fabian Lorenzo-Diaz, Norman Doehring, Dominik Driesch, Doris Fischer, and Hortense Slevogt

Subjects

newborns, microbiome, antibiotic resistance gene, neonatology, 16S rDNA sequencing, Microbiology, QR1-502

Abstract

Several studies have recently identified the main factors contributing to the bacterial colonization of newborns and the dynamics of the infant microbiome development. However, most of these studies address large time periods of weeks or months after birth, thereby missing on important aspects of the early microbiome maturation, such as the acquisition of antibiotic resistance determinants during postpartum hospitalization. The pioneer bacterial colonization and the extent of its associated antibiotic resistance gene (ARG) dissemination during this early phase of life are largely unknown. Studies addressing resistant bacteria or ARGs in neonates often focus only on the presence of particular bacteria or genes from a specific group of antibiotics. In the present study, we investigated the gut-, the oral-, and the skin-microbiota of neonates within the first 72 h after birth using 16S rDNA sequencing approaches. In addition, we screened the neonates and their mothers for the presence of 20 different ARGs by directed TaqMan qPCR assays. The taxonomic analysis of the newborn samples revealed an important shift of the microbiota during the first 72 h after birth, showing a clear site-specific colonization pattern in this very early time frame. Moreover, we report a substantial acquisition of ARGs during postpartum hospitalization, with a very high incidence of macrolide resistance determinants and mecA detection across different body sites of the newborns. This study highlights the importance of antibiotic resistance determinant dissemination in neonates during hospitalization, and the need to investigate the implication of the mothers and the hospital environment as potential sources of ARGs.

Published

2020

8. Parental origin of deletions and duplications – about the necessity to check for cryptic inversions

Author

Thomas Liehr, Isolde Schreyer, Alma Kuechler, Emmanouil Manolakos, Sylke Singer, Andreas Dufke, Kathleen Wilhelm, Tereza Jančušková, Radek Čmejla, Moneeb A. K. Othman, Ahmed H. Al-Rikabi, Kristin Mrasek, Monika Ziegler, Stefanie Kankel, Katharina Kreskowski, and Anja Weise

Subjects

Copy number variants (CNVs), Microdeletion/microduplication syndromes (MMSs), Three color fluorescence in situ hybridization (FISH), Inversion, Deletion, Duplication, Genetics, QH426-470

Abstract

Abstract Background Copy number variants (CNVs) are the genetic bases for microdeletion/ microduplication syndromes (MMSs). Couples with an affected child and desire to have further children are routinely tested for a potential parental origin of a specific CNV either by molecular karyotyping or by two color fluorescence in situ hybridization (FISH), yet. In the latter case a critical region probe (CRP) is combined with a control probe for identification of the chromosome in question. However, CNVs can arise also due to other reasons, like a recombination-event based on a submicroscopic, cryptic inversion in one of the parents. Results Seventy-four patients with different MMSs and overall 81 CNVs were studied here by a novel three color FISH approach. The way how three locus-specific probes are selected (one is the CRP and two are flanking it in a distance of 5-10 Mb) enables to detect or exclude two possible parental conditions as origins of the CNV seen in the index: (i) direct parental origin of the CNV (deletion or duplication) or (ii) a parental cryptic inversion. Thus, for overall 51/81 CNVs (63%) a parental origin could be determined. 36/51 (70.5%) inherited the CNV directly from one of the parents, but 15/51 (29.5%) were due to an exclusively by three color FISH detectable parental inversion. A 2:1 ratio of maternal versus paternal inheritance was found. Also almost two times more male than female were among the index patients. Conclusion The new, here suggested three color FISH approach is suited for more comprehensive parental studies of patients with MMS. The detection rate for parental origin was increased by 140% in this study. Still, for 30/81 cases (37%) no reason for the ‘de novo’ MMS in the affected index patient could be found by the here suggested FISH-probe set.

Published

2018

9. About the origin of the acrocentric part of non-acrocentric satellited chromosomes in humans

Author

T Liehr, Stefanie Kankel, and Mohammed Abdulazeez

Subjects

Evolutionary biology, Centromere, General Medicine, Biology

Abstract

Variants in size of the acrocentric short arms (acro-ps) are normally not reported and considered as chromosomal heteromorphisms (CHMs) without any influence on the carrier’s phenotype. However, if acro-ps are translocated to ends of A-chromosomes (i.e. human chromosomes 1-22 and X or Y), those rearrangements are studied in more detail. The aim of the study: Here we characterized 11 healthy carriers of a non-acrocentric satellited chromosomes der(A)t(A;acro)(pter or qter;p1?1.2) to determine the frequency of chromosome 15p and 22p in such rearrangements. Materials and methods: 11 carriers of one (10 cases) or two (1 case) der(A)t(A;acro) were identified during routine cytogenetic analyses. They were originally referred due to infertility or due to a mentally retarded child with otherwise abnormal karyotype. Here derivative chromosomes were studied by fluorescence in situ hybridization applying probes D15Z1 (specific for 15p11.2) and D22Z4 (specific for 22p11.2). As there are no DNA-sequences available for 13p11.2, 14p11.2 and 21p11.2 these regions could not be tested. Results: D15Z1 sequences were identified in 1 out of 12 derivatives der(A)t(A;acro). D22Z1 could not be detected in any of the 11 remainder derivatives. However, only 3 of the 12 der(A)t(A;acro) had acro-ps large enough to potentially comprise sub-band p11.2. Conclusion: In contrast to der(Y)t(Y;acro)(q12;p1?1.2), where in at least 65% of the cases the acro-p part contains D15Z1 sequences, here it could be shown that in der(A)t(A;acro) 15p involvement can be substantiated much less frequently. Also, in none of the two groups D22Z4-sequences were detected in acro-p-parts yet. Besides, breakpoint of acro-pparts in der(A)t(A;acro) seem to be in ~75% of the cases distal from p11.2.

Published

2021

10. Partial Reduction in

Author

Sandra, Classen, Elena, Rahlf, Johannes, Jungwirth, Nina, Albers, Luca Philipp, Hebestreit, Alexandra, Zielinski, Lena, Poole, Marco, Groth, Philipp, Koch, Thomas, Liehr, Stefanie, Kankel, Nils, Cordes, Cordula, Petersen, Kai, Rothkamm, Helmut, Pospiech, and Kerstin, Borgmann

Subjects

DNA Replication, DNA Repair, BRCA1 Protein, Cell Line, Tumor, Genes, BRCA1, Humans, Female, Breast Neoplasms, Homologous Recombination, DNA Damage

Published

2022

11. How to Obtain High‐Quality Metaphase Spreads for Molecular Cytogenetics

Author

Thomas, Liehr, Anja, Weise, Luisa, Person, Niklas, Padutsch, and Stefanie, Kankel

Subjects

Cytogenetics, Medical Laboratory Technology, General Immunology and Microbiology, General Neuroscience, Cytogenetic Analysis, Health Informatics, General Pharmacology, Toxicology and Pharmaceutics, Interphase, In Situ Hybridization, Fluorescence, Metaphase, General Biochemistry, Genetics and Molecular Biology

Abstract

Interphase or metaphase nuclei can be accessed in molecular cytogenetic analyses. Metaphase spreads are routinely studied by fluorescence in situ hybridization (FISH) to answer clinical genetic questions. Even though metaphase quality is essential for FISH studies, there is limited ability in clinical cases to improve the quality of cytogenetic preparations. However, the quality of preps is important for the exact localization of FISH signals, which is necessary to identify individual chromosomes and chromosomal sub-regions using inverted DAPI banding. Here we present an efficient and easy-to-perform variant of standard slide pretreatment before a normal FISH procedure. This method reproducibly leads to solid, "steel," nonfuzzy, and well-DAPI-banded metaphases. This protocol works in blood lymphocyte and amniotic fluid-derived fibroblasts. © 2022 The Authors. Current Protocols published by Wiley Periodicals LLC. Basic Protocol: Slide pretreatment for high-quality metaphases for molecular cytogenetics.

Published

2022

12. Analysis and pharmacological modulation of senescence in human epithelial stem cells

Author

Vanessa Barbaro, Antonio Orvieto, Gualtiero Alvisi, Marina Bertolin, Filippo Bonelli, Thomas Liehr, Tigran Harutyunyan, Stefanie Kankel, Gordana Joksic, Stefano Ferrari, Elena Daniele, Diego Ponzin, Daniela Bettio, Leonardo Salviati, and Enzo Di Iorio

Subjects

DAPT (γ-secretase inhibitor, N-[N-(3,5-difluorophenacetyl)-L-alanyl]-S-phenylglycine T-butyl ester), p63, Stem Cells, Cleft Lip, EEC syndrome, RNAseq, lifespan, self-renewal, stem cells, Humans, Platelet Aggregation Inhibitors, Cleft Palate, Ectodermal Dysplasia, Cell Biology, N-[N-(3, Molecular Medicine, 5-difluorophenacetyl)-L-alanyl]-S-phenylglycine T-butyl ester)

Abstract

Human epithelial stem cells (ESCs) are characterized by long-term regenerative properties, much dependent on the tissue of origin and varying during their lifespan. We analysed such variables in cultures of ESCs isolated from the skin, conjunctiva, limbus and oral mucosa of healthy donors and patients affected by ectrodactyly-ectodermal dysplasia-clefting syndrome, a rare genetic disorder caused by mutations in the p63 gene. We cultured cells until exhaustion in the presence or in the absence of DAPT (gamma-secretase inhibitor; N-[N-(3, 5-difluorophenacetyl)-L-alanyl]-S-phenylglycine T-butyl ester). All cells were able to differentiate in vitro but exhibited variable self-renewal potential. In particular, cells carrying p63 mutations stopped prematurely, compared with controls. Importantly, administration of DAPT significantly extended the replicative properties of all stem cells under examination. RNA sequencing analysis revealed that distinct sets of genes were up- or down-regulated during their lifetime, thus allowing to identify druggable gene networks and off-the-shelf compounds potentially dealing with epithelial stem cell senescence. These data will expand our knowledge on the genetic bases of senescence and potentially pave the way to the pharmacological modulation of ageing in epithelial stem cells., Journal of Cellular and Molecular Medicine, 26 (14), ISSN:1582-1838, ISSN:1582-4934

Published

2022

13. Molecular cytogenetic characterization of the urethane-induced murine lung cell line LA-4 as a model for human squamous cell lung cancer

Author

Shaymaa Azawi, Martina Rincic, Stefanie Kankel, Thomas Liehr, Milash Balachandran, and Fritz Kramer

Subjects

Cancer Research, Oncogene, business.industry, Cell, Cancer, murine cell line LA-4, murine multicolor banding, Articles, Cell cycle, medicine.disease, Molecular medicine, lung cancer, medicine.anatomical_structure, Oncology, Apoptosis, Cell culture, array comparative genomic hybridization, medicine, Cancer research, adenoma, business, Gene

Abstract

The murine tumor cell line LA-4 (also known as LA4 or LA 4) has been extensively used in ~70 studies from 1975 to present. However, the genetic characteristics have not been comprehensively delineated, apart from a single solid-stain cytogenetic study, which reported an average of 116 chromosomes per cell. LA-4 was created via urethane induction in an A/He mouse and demonstrated characteristic features of lung adenoma cells. In the present study, multicolor banding-based molecular cytogenetics was combined with molecular karyotyping to characterize ploidy, copy number alterations and chromosomal breakpoints of LA-4. A hyper-tetraploid karyotype with 85-93 chromosomes per cell, three distinct (pseudo-) dicentric derivatives, two neocentrics, four unbalanced translocations, two chromosomes with terminal deletions and one chromosome with a balanced inversion were detected. The results were translated into the human genome and a comparison with the literature revealed that LA-4 is well-suited as a murine model for human squamous cell lung cancer.

Published

2021

14. Small supernumerary marker chromosomes derived from chromosome 14 and/or 22

Author

Thomas, Liehr, Heather E, Williams, Monika, Ziegler, Stefanie, Kankel, Niklas, Padutsch, and Ahmed, Al-Rikabi

Subjects

Postnatal, Chromosome 22, Small supernumerary marker chromosomes (sSMCs), Research, Incidence, Prenatal, Chromosome 14

Abstract

Small supernumerary marker chromosomes (sSMCs) are additional derivative chromosomes present in an otherwise numerically and structurally normal karyotype. They may derive from each of the 24 human chromosomes, and most contain a normal centromeric region with an alphoid sequence from a single chromosome. The majority of human chromosomes have a unique centromeric DNA-sequence enabling their indubitable characterization. However, chromosomes 14 and 22 share a common centromeric sequence D14/22Z1, and sSMCs with this DNA-stretch can derive from either chromosome. Euchromatin-carrying sSMCs(14 or 22) may be further characterized by molecular cytogenetics. However, in most diagnostic laboratories, heterochromatic sSMCs cannot be differentiated between chromosomes 14 or 22 derivation and are often reported as der(14 or 22). Still, heterochromatic sSMC(14 or 22) can be distinguished from each other using the D22Z4 probe (non-commercial) localized to 22p11.2. Herein, 355 sSMC(14 or 22) analyzed in the authors’ laboratory during the last ~ 20 years are summarized to address the questions: (1) What are the true frequencies of chromosome 14- and chromosome 22- derived sSMCs within D14/22Z1-positive cases? (2) Does sub-characterization of sSMC(14) and sSMC(22) make a difference in routine diagnostics? These questions could be answered as follows: (ad 1) within the studied group of sSMCs ~ 40% are derived from chromosome 14 and ~ 60% from chromosome 22; (ad 2) the knowledge on exact sSMC origin can help to save costs in routine diagnostics; i.e. in a clinically abnormal person with sSMC(14) a test for uniparental disomy is indicated, which is not necessary if a chromosome 22 origin for the sSMC was determined.

Published

2020

15. About Cryptic Acrocentric Pericentromeric Abnormalities in Infertile

Author

Niklas Padutsch, Stefanie Kankel, Seria Tsan, Ahmed Al-Rikabi, Kristin Mrasek, Anja Weise, Luisa Person, Monika Ziegler, and T Liehr

Subjects

Molecular cytogenetics, Genetics, Meiosis, Euchromatin, medicine.diagnostic_test, Short arms, Centromere, medicine, Karyotype, Biology, Fluorescence in situ hybridization

Abstract

Cryptic balanced chromosomal aberrations can be an underlying cause of infertility. In 2003 Cockwell and coworkers highlighted the relevance of euchromatic pericentric regions of acrocentric chromosomes that may be a yet ignored genomic region hosting cryptic rearrangements. Here we offer the first follow-up study to further explore this idea. Two specific molecular cytogenetic probe sets were established to elucidate such cryptic rearrangements together with chromosomal heteromorphisms of acrocentric centromeres. In 28 infertile couples and 20 controls, the rate of centromeric heteromorphisms was almost comparable in both groups and one heteromorphism was noted in ~30% of the cases, and two heteromorphisms in ~15% and three heteromorphisms 5%. However, none of the studied groups revealed any cryptic euchromatic pericentromeric abnormalities of the acrocentrics. Nonetheless, in parallel an infertile case with an inv(13)(p12q12.1?2) was uncovered, being not part of the systematically studied group of infertile. As unbalanced products of meiosis with such or similar karyotypes can potentially contribute to abortions, the existence of rare, cryptic pericentromeric euchromatic abnormalities in the acrocentrics thus needs to be still expected in banding cytogenetic diagnostics. Accordingly, this study reflected that suspicious acrocentric short arms in infertile need special attention and further characterization by fluorescence in situ hybridization.

Published

2021

16. Parental origin of deletions and duplications - about the necessity to check for cryptic inversions

Author

Sylke Singer, Ahmed Al-Rikabi, Kristin Mrasek, Anja Weise, Radek Cmejla, Isolde Schreyer, Kathleen Wilhelm, Katharina Kreskowski, Andreas Dufke, Monika Ziegler, Thomas Liehr, Tereza Jancuskova, Moneeb A.K. Othman, Alma Kuechler, Emmanouil Manolakos, and Stefanie Kankel

Subjects

0301 basic medicine, medicine.medical_specialty, lcsh:QH426-470, Duplication, Copy number variants (CNVs), Medizin, 030105 genetics & heredity, Biology, Biochemistry, Deletion, 03 medical and health sciences, Gene duplication, Genetics, medicine, Copy-number variation, Three color fluorescence in situ hybridization (FISH), Paternal Inheritance, Molecular Biology, Genetics (clinical), medicine.diagnostic_test, Research, Biochemistry (medical), Cytogenetics, Inversion, Chromosome, Karyotype, Human genetics, lcsh:Genetics, 030104 developmental biology, Molecular Medicine, Fluorescence in situ hybridization, Microdeletion/microduplication syndromes (MMSs)

Abstract

Background Copy number variants (CNVs) are the genetic bases for microdeletion/ microduplication syndromes (MMSs). Couples with an affected child and desire to have further children are routinely tested for a potential parental origin of a specific CNV either by molecular karyotyping or by two color fluorescence in situ hybridization (FISH), yet. In the latter case a critical region probe (CRP) is combined with a control probe for identification of the chromosome in question. However, CNVs can arise also due to other reasons, like a recombination-event based on a submicroscopic, cryptic inversion in one of the parents. Results Seventy-four patients with different MMSs and overall 81 CNVs were studied here by a novel three color FISH approach. The way how three locus-specific probes are selected (one is the CRP and two are flanking it in a distance of 5-10 Mb) enables to detect or exclude two possible parental conditions as origins of the CNV seen in the index: (i) direct parental origin of the CNV (deletion or duplication) or (ii) a parental cryptic inversion. Thus, for overall 51/81 CNVs (63%) a parental origin could be determined. 36/51 (70.5%) inherited the CNV directly from one of the parents, but 15/51 (29.5%) were due to an exclusively by three color FISH detectable parental inversion. A 2:1 ratio of maternal versus paternal inheritance was found. Also almost two times more male than female were among the index patients. Conclusion The new, here suggested three color FISH approach is suited for more comprehensive parental studies of patients with MMS. The detection rate for parental origin was increased by 140% in this study. Still, for 30/81 cases (37%) no reason for the ‘de novo’ MMS in the affected index patient could be found by the here suggested FISH-probe set. Electronic supplementary material The online version of this article (10.1186/s13039-018-0369-1) contains supplementary material, which is available to authorized users.

Published

2018