Your search keyword '"Ring Chromosomes"' showing total 2,232 results

1. Multiple desmoplastic Spitz nevi with BRAF fusions in a patient with ring chromosome 7 syndrome

Author

Roy, Simon F, Bastian, Boris C, Maguiness, Sheilagh, Giubellino, Alessio, Vemula, Swapna S, McCalmont, Timothy H, and Yeh, Iwei

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Adult, Chromosome Disorders, Chromosomes, Human, Pair 7, Ear Neoplasms, Humans, Male, Nevus, Epithelioid and Spindle Cell, Oncogene Proteins, Fusion, Proto-Oncogene Proteins B-raf, Ring Chromosomes, Skin Neoplasms, BRAF fusion, BRAF gene, ring chromosome 7, ring chromosome seven, melanocytic nevi, melanocytic nevus, Spitz nevus, Spitz tumor, spitzoid, Biological Sciences, Medical and Health Sciences, Dermatology & Venereal Diseases, Biochemistry and cell biology, Genetics, Oncology and carcinogenesis

Abstract

Patients with non-supernumerary ring chromosome 7 syndrome have an increased incidence of hemangiomas, café-au-lait spots, and melanocytic nevi. The mechanism for the increased incidence of these benign neoplasms is unknown. We present the case of a 22-year-old man with ring chromosome 7 and multiple melanocytic nevi. Two nevi, one on the right ear and the other on the right knee, were biopsied and diagnosed as desmoplastic Spitz nevi. Upon targeted next-generation DNA sequencing, both harbored BRAF fusions. Copy number alterations and fluorescence in situ hybridization (FISH) for BRAF suggested that the fusions arose on the ring chromosome 7. Hence, one reason for increased numbers of nevi in patients with non-supernumerary ring chromosome 7 syndrome may be increased likelihood of BRAF fusions, due to the instability of the ring chromosome.

Published

2021

2. Ring Chromosomes in Hematological Malignancies Are Associated with TP53 Gene Mutations and Characteristic Copy Number Variants.

Author

Boyd, Rachel J., Murry, Jaclyn B., Morsberger, Laura A., Klausner, Melanie, Chen, Suping, Gocke, Christopher D., McCallion, Andrew S., and Zou, Ying S.

Subjects

*CHROMOSOME analysis, *GENETICS, *GENETIC mutation, *MYELOID leukemia, *KARYOTYPES, *HEMATOLOGIC malignancies, *CHROMOSOME abnormalities, *DESCRIPTIVE statistics, *LYMPHOCYTIC leukemia, *RESEARCH funding, *MYELOID cells, *TUMOR markers

Abstract

Simple Summary: Ring chromosomes (RCs) are formed when chromosome ends fuse to form a circular structure. RCs are seen in <10% of patients with blood cancers (i.e., leukemias, lymphomas, and myelomas), and are associated with poor disease outcomes. We sought to evaluate how frequently RCs arise in patients diagnosed with these cancers and determine if there are any associated genetic variants, regions, or chromosomal abnormalities. Most patients with RCs have mutations in the TP53 gene and gross chromosomal rearrangements, particularly among chromosomes 5, 7, 11, and 17. Most of these patients also possess marker chromosomes with genetic material of unknown origin. The majority of RCs that resemble identifiable chromosomes, as well as chromosomes lacking gross rearrangements, were seen in patients without TP53 mutations. Our data suggest that mechanisms underlying RC generation may arise differently in patient groups with the presence or absence of functional TP53, a potentially important distinction for clinical decision making. Ring chromosomes (RC) are present in <10% of patients with hematological malignancies and are associated with poor prognosis. Until now, only small cohorts of patients with hematological neoplasms and concomitant RCs have been cytogenetically characterized. Here, we performed a conventional chromosome analysis on metaphase spreads from >13,000 patients diagnosed with hematological malignancies at the Johns Hopkins University Hospital and identified 98 patients with RCs—90 with myeloid malignancies and 8 with lymphoid malignancies. We also performed a targeted Next-Generation Sequencing (NGS) assay, using a panel of 642 cancer genes, to identify whether these patients harbor relevant pathogenic variants. Cytogenetic analyses revealed that RCs and marker chromosomes of unknown origin are concurrently present in most patients by karyotyping, and 93% of patients with NGS data have complex karyotypes. A total of 72% of these individuals have pathogenic mutations in TP53, most of whom also possess cytogenetic abnormalities resulting in the loss of 17p, including the loss of TP53. All patients with a detected RC and without complex karyotypes also lack TP53 mutations but have pathogenic mutations in TET2. Further, 70% of RCs that map to a known chromosome are detected in individuals without TP53 mutations. Our data suggest that RCs in hematological malignancies may arise through different mechanisms, but ultimately promote widespread chromosomal instability. [ABSTRACT FROM AUTHOR]

Published

2023

3. [Prenatal diagnosis of a fetus with mosaicism ring chromosome 2].

Author

Zhou Y, Xu L, Yan L, Chen C, and Li H

Subjects

Humans, Female, Pregnancy, Adult, Karyotyping, Prenatal Diagnosis methods, Chromosomes, Human, Pair 2 genetics, DNA Copy Number Variations, Fetus abnormalities, Heart Defects, Congenital genetics, Retrospective Studies, Ultrasonography, Prenatal, Mosaicism embryology, Ring Chromosomes

Abstract

Objective: To explore the genetic basis for a fetus with increased risk for Down syndrome and cardiac anomalies discovered by prenatal ultrasonography., Methods: A pregnant woman presented at the Women and Children's Hospital of Ningbo University on August 21, 2023 were selected as the study subject. Clinical data were retrospectively analyzed. Maternal peripheral blood sample was collected for non-invasive prenatal testing (NIPT) based on fetal free DNA. Amniotic fluid sample was collected for G-banded chromosomal karyotyping analysis. Trio-whole exome sequencing (WES) was also carried out on the amniotic fluid sample and peripheral blood samples from the couple. Copy number variation (CNV) identified by the WES was validated by real-time fluorescent quantitative PCR (qPCR). Chromosomal karyotyping was also carried out for the couple. This study has been approved by the Medical Ethics Committee of Women and Children's Hospital of Ningbo University (No. EC2020-048)., Results: Ultrasound examination at 22 +6 gestational weeks had indicated intrauterine growth retardation (IUGR). The fetus was also found to have ventricular septal defect, overriding aorta and pulmonary stenosis. NIPT indicated a low risk for aneuploidy of chromosomes 13, 18 and 21. G-banding analysis revealed that the fetus had a karyotype of 45,XY,-2[5]/46,XY,r(2)(p25q37)[55]. WES has identified a deletion of approximately 1 614.28 kb in the 2p25.3 region, namely seq[hg38]del(2)(p25.3p25.3)chr2: g.10500&#95;1624775del. The same deletion was found in neither parent, suggesting a de novo origin. qPCR results confirmed the expression of target genes in the fetal sample to be significantly reduced, whilst no similar anomaly was found in either parent., Conclusion: The mosaicism ring chromosome 2 probably underlay the IUGR and cardiovascular malformations in this fetus.

Published

2024

4. Imaging Findings and MRI Patterns in a Cohort of 18q Chromosomal Abnormalities.

Author

Malik P, Branson H, Yoon G, Shroff M, Blaser S, and Krishnan P

Subjects

Humans, Female, Male, Infant, Retrospective Studies, Child, Preschool, Chromosome Deletion, Brain diagnostic imaging, Brain pathology, Ring Chromosomes, Cohort Studies, Trisomy 18 Syndrome diagnostic imaging, Trisomy 18 Syndrome genetics, White Matter diagnostic imaging, White Matter pathology, Chromosome Disorders diagnostic imaging, Chromosome Disorders genetics, Chromosomes, Human, Pair 18 genetics, Magnetic Resonance Imaging methods

Abstract

Background and Purpose: The abnormalities of the long arm of chromosome 18 (18q) constitute a complex spectrum. We aimed to systematically analyze their MR imaging features. We hypothesized that there would be variable but recognizable white matter and structural patterns in this cohort., Materials and Methods: In this retrospective cohort study, we included pediatric patients with a proved abnormality of 18q between 2000-2022. An age- and sex-matched control cohort was also constructed., Results: Thirty-six cases, median MR imaging age 19.6 months (4.3-59.3), satisfied our inclusion criteria. Most were female (25, 69%, F:M ratio 2.2:1). Fifty MR imaging studies were analyzed, and 35 (70%) had delayed myelination. Two independent readers scored brain myelination with excellent interrater reliability. Three recognizable evolving MR imaging patterns with distinct age distributions and improving myelination scores were identified: Pelizaeus-Merzbacher disease-like (9.9 months, 37), intermediate (22 months, 48), and washed-out pattern (113.6 months, 53). Etiologically, MRIs were analyzed across 3 subgroups: 18q deletion (34, 69%), trisomy 18 (10, 21%), and ring chromosome 18 (5, 10%). Ring chromosome 18 had the highest myelination lag (27, P = .005) and multifocal white matter changes ( P  = .001). Trisomy 18 had smaller pons and cerebellar dimensions (anteposterior diameter pons, P = .002; corpus callosum vermis, P < .001; and transverse cerebellar diameter, P  = .04)., Conclusions: In this cohort of 18q chromosomal abnormalities, MR imaging revealed recognizable patterns correlating with improving brain myelination. Imaging findings appear to be on a continuum with more severe white matter abnormalities in ring chromosome 18 and greater prevalence of structural abnormalities of the pons and cerebellum in trisomy 18., (© 2024 by American Journal of Neuroradiology.)

Published

2024

5. [Comprehensive diagnosis and genetic analysis of two children with ring chromosome 18].

Author

Ding Z, Mei S, Zhang B, Kong J, Liu L, Zhang Z, Wang C, and Zhang Y

Subjects

Humans, Male, DNA Copy Number Variations, Child, Preschool, Genetic Testing methods, Infant, Child, Female, Exome Sequencing, Chromosome Deletion, Developmental Disabilities genetics, Developmental Disabilities diagnosis, Phenotype, Chromosomes, Human, Pair 18 genetics, Ring Chromosomes, Karyotyping

Abstract

Objective: To clarify the genetic diagnosis of two children with ring chromosome 18 and explore their mechanisms and clinical phenotypes., Methods: Two patients treated at the Children's Hospital of Henan Province respectively in June 2022 and March 2023 were selected as the study subjects. Genetic testing and diagnosis were carried out through copy number variation sequencing (CNV-seq), G-banded chromosomal karyotyping, and whole exome sequencing (WES)., Results: Child 1 had mainly manifested developmental delay, white matter hypoplasia, type 1 diabetes mellitus, and micropenis. He was found to have a chromosomal karyotype of 46,XY,r(18)(p11.21q22.1)[40]/46,XY[7], and CNV-seq results showed that he has a 14.86 Mb deletion at 18p11.21p11.32 and a 14.02 Mb deletion at 18q22.1q23. Child 2 had peculiar facial features, delayed white matter myelination, developmental delay, atrial septal defect, severe sensorineural deafness, and congenital laryngeal stridor. He was found to have a chromosomal karyotype of 46,XY,r(18)(p11.2q23). CNV-seq result proved that he had a 14.86 Mb deletion at 18p11-21p11.32 and a 20.74 Mb deletion at 18q21.32q23. WES has failed to detect single nucleotide variants (SNVs) in either child, but revealed a large segmental deletion at chromosome 18 in both of them., Conclusion: Both children were diagnosed with ring chromosome 18 syndrome. The different size of the deletional fragments in the 18q region and mosaicism of ring chromosome 18 in child 1 may underlay the variation in their clinical phenotypes. The type 1 diabetes mellitus and micropenis noted in both children are novel features for ring chromosome 18 syndrome.

Published

2024

6. Effect of Heracleum sosnowskyi extract aqueous solution on the Allium cepa root meristem

Author

M. V. Smirnova and V. A. Kotelnikov

Subjects

genotoxicity, mitosis, plant extract, mitotic activity, lagging and sticking chromosomes, anaphase bridges, ring chromosomes, nuclear buds, Science

Abstract

Heracleum sosnowskyi (Apiaceae) contains a lot of useful chemical ingredients that can be used in industry, medicine and other fields as plant component extracts and as chemical compounds that have been extracted in different ways, which requires the last to be tested for chemical safety, including a genotoxic test in vivo. In the present paper, the 96-hour effect of the H. sosnowskyi extract aqueous solution at concentrations of 0.01, 0.05, 0.10, and 0.50 mL/L on the genetic apparatus and mitotic activity of the cells of the Allium cepa (Alliaceae) root meristem is discussed. Distilled water was applied as a negative control, and hydrogen peroxide 1% as a positive one. The extract was prepared from the plant’s fresh leaves by soaking them in acetone. It was then distilled at 57 ºС and diluted with distilled water to obtain the experimental concentrations. As extract content in the aqueous solution increased, a statistically significant decrease in mitotic activity, an increase in aberrant cell percentage and a concentration-dependent inhibition of root growth were observed. In the 0.5 mL/L solution, if compared against the other experimental concentrations, an increase in the metaphase, anaphase and telophase indices along with a decrease in the prophase index were observed. The most common aberrations for all the concentrations were lagging and sticking chromosomes, anaphase bridges, ring chromosomes and nuclear buds. The same solution and the positive control produced membrane damage; giant and ghost cells. The results of the experiment performed have demonstrated the extract’s aneugenic effect that causes spindle disturbance, mitodepression and inhibits the cells of the Allium cepa root meristem, prevails over its clastogenic effect.

Published

2021

7. Detection of mosaic ring chromosome 12 or 46,XY,r(12) (p13.3q24.33)/46, XY in a 37-year-old male associated with oligospermia but no other apparently phenotypic abnormalities.

Author

Chen CP

Subjects

Humans, Male, Adult, Chromosomes, Human, Pair 12 genetics, Phenotype, Karyotyping, Oligospermia genetics, Oligospermia diagnosis, Mosaicism, Ring Chromosomes

Abstract

Competing Interests: Declaration of competing interest The authors have no conflicts of interest relevant to this article.

Published

2024

8. Cell-autonomous correction of ring chromosomes in human induced pluripotent stem cells.

Author

Bershteyn, Marina, Hayashi, Yohei, Desachy, Guillaume, Sami, Salma, Tsang, Kathryn, Wynshaw-Boris, Anthony, Kriegstein, Arnold, Hsiao, Edward, Weiss, Lauren, and Yamanaka, Shinya

Subjects

Aneuploidy, Animals, Cellular Reprogramming, Chromosomal Instability, Chromosome Deletion, Chromosome Disorders, Chromosomes, Human, Pair 13, Chromosomes, Human, Pair 17, Clone Cells, Fibroblasts, Humans, Induced Pluripotent Stem Cells, Karyotype, Karyotyping, Male, Mice, Models, Genetic, Ring Chromosomes, Uniparental Disomy

Abstract

Ring chromosomes are structural aberrations commonly associated with birth defects, mental disabilities and growth retardation. Rings form after fusion of the long and short arms of a chromosome, and are sometimes associated with large terminal deletions. Owing to the severity of these large aberrations that can affect multiple contiguous genes, no possible therapeutic strategies for ring chromosome disorders have been proposed. During cell division, ring chromosomes can exhibit unstable behaviour leading to continuous production of aneuploid progeny with low viability and high cellular death rate. The overall consequences of this chromosomal instability have been largely unexplored in experimental model systems. Here we generated human induced pluripotent stem cells (iPSCs) from patient fibroblasts containing ring chromosomes with large deletions and found that reprogrammed cells lost the abnormal chromosome and duplicated the wild-type homologue through the compensatory uniparental disomy (UPD) mechanism. The karyotypically normal iPSCs with isodisomy for the corrected chromosome outgrew co-existing aneuploid populations, enabling rapid and efficient isolation of patient-derived iPSCs devoid of the original chromosomal aberration. Our results suggest a fundamentally different function for cellular reprogramming as a means of chromosome therapy to reverse combined loss-of-function across many genes in cells with large-scale aberrations involving ring structures. In addition, our work provides an experimentally tractable human cellular system for studying mechanisms of chromosomal number control, which is of critical relevance to human development and disease.

Published

2014

9. Ring Chromosome 20 Syndrome: Genetics, Clinical Characteristics, and Overlapping Phenotypes

Author

Angela Peron, Ilaria Catusi, Maria Paola Recalcati, Luciano Calzari, Lidia Larizza, Aglaia Vignoli, and Maria Paola Canevini

Subjects

ring chromosome 20 syndrome r(20), ring chromosomes, mosaicism, cytogenetics, karyotype, seizures, Neurology. Diseases of the nervous system, RC346-429

Abstract

Ring chromosome 20 [r(20)] syndrome is a rare condition characterized by a non-supernumerary ring chromosome 20 replacing a normal chromosome 20. It is commonly seen in a mosaic state and is diagnosed by means of karyotyping. r(20) syndrome is characterized by a recognizable epileptic phenotype with typical EEG pattern, intellectual disability manifesting after seizure onset in otherwise normally developing children, and behavioral changes. Despite the distinctive phenotype, many patients still lack a diagnosis—especially in the genomic era—and the pathomechanisms of ring formation are poorly understood. In this review we address the genetic and clinical aspects of r(20) syndrome, and discuss differential diagnoses and overlapping phenotypes, providing the reader with useful tools for clinical and laboratory practice. We also discuss the current issues in understanding the mechanisms through which ring 20 chromosome causes the typical manifestations, and present unpublished data about methylation studies. Ultimately, we explore future perspectives of r(20) research. Our intended audience is clinical and laboratory geneticists, child and adult neurologists, and genetic counselors.

Published

2020

10. Transcriptome analysis of a ring chromosome 20 patient cohort.

Author

Myers, Kenneth A., Bennett, Mark F., Hildebrand, Michael S., Coleman, Matthew J., Zhou, Geyu, Hollingsworth, Georgie, Cairns, Anita, Riney, Kate, Berkovic, Samuel F., Bahlo, Melanie, and Scheffer, Ingrid E.

Subjects

*CHROMOSOME analysis, *CHROMOSOME abnormalities, *POLYMERASE chain reaction, *CHROMOSOMES, *GENE expression, *CHROMOSOME duplication

Abstract

Ring chromosomes occur when the ends of normally rod‐shaped chromosomes fuse. In ring chromosome 20 (ring 20), intellectual disability and epilepsy are usually present, even if there is no deleted coding material; the mechanism by which individuals with complete ring chromosomes develop seizures and other phenotypic abnormalities is not understood. We investigated altered gene transcription as a contributing factor by performing RNA‐sequencing (RNA‐seq) analysis on blood from seven patients with ring 20, and 11 first‐degree relatives (all parents). Geographic analysis did not identify altered expression in peritelomeric or other specific chromosome 20 regions. RNA‐seq analysis revealed 97 genes potentially differentially expressed in ring 20 patients. These included one epilepsy gene, NPRL3, but this finding was not confirmed on reverse transcription Droplet Digital polymerase chain reaction analysis. Molecular studies of structural chromosomal anomalies such as ring chromosome are challenging and often difficult to interpret because many patients are mosaic, and there may be genome‐wide chromosomal instability affecting gene expression. Our findings nevertheless suggest that peritelomeric altered transcription is not the likely pathogenic mechanism in ring 20. Underlying genetic mechanisms are likely complex and may involve differential expression of many genes, the majority of which may not be located on chromosome 20. [ABSTRACT FROM AUTHOR]

Published

2021

11. MDM2 amplification in rod-shaped chromosomes provides clues to early stages of circularized gene amplification in liposarcoma.

Author

Sydow S, Piccinelli P, Mitra S, Tsagkozis P, Hesla A, B R De Mattos C, Köster J, Magnusson L, Nilsson J, Ameur A, Wardenaar R, Foijer F, Spierings D, and Mertens F

Subjects

Humans, Chromosomes, Human, Pair 12 genetics, Chromothripsis, Ring Chromosomes, Liposarcoma genetics, Liposarcoma pathology, Gene Amplification, Proto-Oncogene Proteins c-mdm2 genetics

Abstract

Well-differentiated liposarcoma (WDLS) displays amplification of genes on chromosome 12 (Chr12) in supernumerary ring or giant marker chromosomes. These structures have been suggested to develop through chromothripsis, followed by circularization and breakage-fusion-bridge (BFB) cycles. To test this hypothesis, we compared WDLSs with Chr12 amplification in rod-shaped chromosomes with WDLSs with rings. Both types of amplicons share the same spectrum of structural variants (SVs), show higher SV frequencies in Chr12 than in co-amplified segments, have SVs that fuse the telomeric ends of co-amplified chromosomes, and lack interspersed deletions. Combined with the finding of cells with transient rod-shaped structures in tumors with ring chromosomes, this suggests a stepwise process starting with the gain of Chr12 material that, after remodeling which does not fit with classical chromothripsis, forms a dicentric structure with other chromosomes. Depending on if and when telomeres from other chromosomes are captured, circularized or linear gain of 12q sequences will predominate., (© 2024. The Author(s).)

Published

2024

12. Atypical teratoid/rhabdoid tumour-TYR subtype arising in the setting of germline ring chromosome 22: An uncommon form of tumour predisposition.

Author

Lee JC, Tran QT, McGee RB, Perrino MR, Upadhyaya SA, Hanzlik EM, Pytel N, Carroll AJ, Orisme W, Eldomery M, Wang L, Blackburn PR, Furtado LV, Viaene AN, Luo M, Kalish JM, Pinto SN, Bag AK, and Orr BA

Subjects

Humans, SMARCB1 Protein genetics, Germ Cells pathology, Rhabdoid Tumor genetics, Rhabdoid Tumor pathology, Ring Chromosomes, Central Nervous System Neoplasms, Teratoma genetics

Published

2024

13. Ring 20 syndrome: A call to action.

Author

James WD, Roth R, and Fitzgerald M

Subjects

Humans, Ring Chromosomes

Published

2024

14. [Application of optical genome mapping technology for the detection of chromosomal structural variations].

Author

Zhang Z, He S, Li X, Cheng K, Wei Y, and Ren Z

Subjects

Humans, In Situ Hybridization, Fluorescence, Chromosomes, Human, Pair 6, Translocation, Genetic, Chromosome Mapping, Chromosomes, Human, Pair 3, Ring Chromosomes

Abstract

Objective: To assess the value of optical genome mapping (OGM) for the detection of chromosomal structural abnormalities including ring chromosomes, balanced translocations, and insertional translocations., Methods: Clinical data of four patients who underwent pre-implantation genetic testing concurrently with OGM and chromosomal microarray analysis at the Center of Reproductive Medicine of the Sixth Affiliated Hospital of Sun Yat-sen University from January to October 2022 due to chromosomal structural abnormalities were selected as the study subjects. Some of the results were verified by multi-color fluorescence in situ hybridization., Results: The OGM has successfully detected a balanced translocation and fine mapped the breakpoints in a patient. Among two patients with insertional translocations, OGM has provided more refined breakpoint locations than karyotyping analysis in a patient who had chromosome 3 inserted into chromosome 6 and determined the direction of the inserted fragment. However, OGM has failed to detect the chromosomal abnormality in a patient with chromosome 8 inserted into the Y chromosome. It has also failed to detect circular signals in a patient with ring chromosome mosaicism., Conclusion: OGM has successfully detected chromosomal structural variations in the four patients and provided assistance for their diagnosis.

Published

2024

15. Bilateral Cleft Lip and Palate in Ring Chromosome 7 Syndrome: A Case Report and Review of Clinical Characteristics.

Author

Bangun K, Kreshanti P, Tania V, Ariani Aswin Y, Menna C, and Aurino L

Subjects

Male, Humans, Child, Preschool, Chromosomes, Human, Pair 7, Cleft Lip genetics, Cleft Lip surgery, Cleft Palate genetics, Cleft Palate surgery, Chromosome Disorders genetics, Ring Chromosomes

Abstract

This report presents a case of ring chromosome 7 syndrome with bilateral cleft lip and palate. A four-year-old boy presented with bilateral cleft lip and palate, microcephaly, clenched toes, cafe-au-lait spots, a history of epilepsy, and severe intellectual disability. Genetic karyotyping revealed 46 XY r(7) (p22q36). His cheiloplasty and delayed palatoplasty were successful. A review of 22 previous r(7) patients revealed that 22.7% had cleft lip and/or palate. This case demonstrates the importance of a multidisciplinary evaluation for cleft patients, particularly those with syndromic features and global developmental delay., Competing Interests: Declaration of Conflicting InterestsThe author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

16. Ring Chromosome 20 Syndrome: Genetics, Clinical Characteristics, and Overlapping Phenotypes.

Author

Peron, Angela, Catusi, Ilaria, Recalcati, Maria Paola, Calzari, Luciano, Larizza, Lidia, Vignoli, Aglaia, and Canevini, Maria Paola

Subjects

CHROMOSOMES, GENETICS, SUPERNUMERARY teeth, BEHAVIOR, PHENOTYPES, ADULT-child relationships

Abstract

Ring chromosome 20 [r(20)] syndrome is a rare condition characterized by a non-supernumerary ring chromosome 20 replacing a normal chromosome 20. It is commonly seen in a mosaic state and is diagnosed by means of karyotyping. r(20) syndrome is characterized by a recognizable epileptic phenotype with typical EEG pattern, intellectual disability manifesting after seizure onset in otherwise normally developing children, and behavioral changes. Despite the distinctive phenotype, many patients still lack a diagnosis—especially in the genomic era—and the pathomechanisms of ring formation are poorly understood. In this review we address the genetic and clinical aspects of r(20) syndrome, and discuss differential diagnoses and overlapping phenotypes, providing the reader with useful tools for clinical and laboratory practice. We also discuss the current issues in understanding the mechanisms through which ring 20 chromosome causes the typical manifestations, and present unpublished data about methylation studies. Ultimately, we explore future perspectives of r(20) research. Our intended audience is clinical and laboratory geneticists, child and adult neurologists, and genetic counselors. [ABSTRACT FROM AUTHOR]

Published

2020

17. Superparamagnetic hematite nanoparticle: Cytogenetic impact on onion roots and seed germination response of major crop plants.

Author

Rath, Kalyani, Ranganathan, Parameswari, Vasappa, Rashmi Kanugodu, and Balasundaram, Sridharan Thalaivarisai

Abstract

Augmented escape of nanostructures to the ecosystem has necessitated the comprehensive study of their impact, especially on plants. In the current study, hematite nanoparticles were prepared by employing garlic extract and checked for their cytogenetic effect on onion roots and germination characteristics of five agricultural crops (Vigna radiata, Triticum aestivum, Trigonella foenum‐graecum, Cicer arietinum and Vicia faba) in the concentration range of 20–100 mg/L. Onion roots exhibited an increased mitotic index till 60 mg/L dosage, beyond which trend decreased marginally. Percentage of aberrant chromosomes reported for 100 mg/L exposure was very low (3.358 ± 0.13%) and included common defects such as clumped/sticky metaphase, ring chromosomes, laggards, spindle abnormality, chromosome bridges etc. Moreover, comet assay, DNA laddering experiment and electron micrograph study confirmed negligible damage to onion roots. Seed germination study indicated a positive response in different agronomic traits (germination index, root length, fold change in weight and vigour index) up to 60 mg/L, beyond which either negative or neutral effect was observed. However, none of the samples showed 50% inhibition in germination index; highest being 33.33% inhibition for V. faba, compared to the control. In brief, biogenic hematite nanoparticles caused insignificant phytotoxicity and were likely assimilated as iron source at lower dosage. [ABSTRACT FROM AUTHOR]

Published

2020

18. A patient with a ring chromosome 2 and microdeletion of 2q detected using FISH: Further support for “ring chromosome 2 syndrome”

Author

Alkuraya, Fowzan S, Kimonis, Virginia E, Holt, Laura, and Murata‐Collins, Joyce L

Subjects

Chromosome Deletion, Chromosomes, Human, Pair 2, Humans, Infant, Newborn, Male, Ring Chromosomes, Syndrome, Genetics, Clinical Sciences

Published

2005

19. Whole-genome sequencing analysis of an atypical teratoid/rhabdoid tumor in a patient with Phelan–McDermid syndrome: a case report and systematic review

Author

Haruki Yamashita, Yoshiki Arakawa, Yukinori Terada, Yasuhide Takeuchi, Yohei Mineharu, Sosuke Sumiyoshi, Shinya Tokunaga, Kohei Nakajima, Naoko Kawabata, Kuniaki Tanaka, Masahiro Tanji, Katsutsugu Umeda, Sachiko Minamiguchi, Seishi Ogawa, Hironori Haga, Junko Takita, and Susumu Miyamoto

Subjects

Cancer Research, Oncology, Child, Preschool, Chromosomes, Human, Pair 22, Humans, Chromosome Disorders, Female, Ring Chromosomes, Neurology (clinical), General Medicine, Chromosome Deletion, Child, Rhabdoid Tumor

Abstract

Atypical teratoid/rhabdoid tumor (AT/RT) is a rare pediatric brain tumor with abnormalities in SMARCB1 located in 22q11.2. We report a case of AT/RT associated with Phelan-McDermid syndrome (PMS) characterized by congenital developmental disorder, mental retardation, and ring chromosome 22 with 22q13.3-qter depletion, for which we performed whole-genome sequencing (WGS). A 4-year-old girl with a developmental disability was referred to our hospital due to dysphoria. Brain magnetic resonance imaging showed a 5-cm well-demarcated mass that extended bilaterally in the frontal lobes. G-banding was performed preoperatively due to a history of developmental retardation. Ring chromosome 22 and deletion of 22q13.3-qter were observed, and she was diagnosed with PMS. She underwent gross total resection of the tumor, and the pathological diagnosis was AT/RT. WGS showed somatic SMARCB1 mutation (p.R201X) and somatic loss of the entire chromosome 22 in the tumor, but not in the blood sample. WGS confirmed previously unreported BRCA2 mutations, 6q loss, and 14q acquisition during tumor progression, but no other significant findings associated with tumor progression. The present case is discussed with reference to a systematic review of previous reports of AT/RT associated with PMS. PMS patients with ring chromosome 22 should be carefully followed up for AT/RT occurrence.

Published

2022

20. Live-born autosomal ring chromosomes at the Johns Hopkins Hospital Cytogenomics Laboratory: Case series-Spanning 52 years of experience in a single center.

Author

Kushwaha S, Stinnett V, Zou YS, and Murry JB

Subjects

Humans, In Situ Hybridization, Fluorescence, Mosaicism, Phenotype, Hospitals, Ring Chromosomes

Abstract

Ring chromosomes (RCs) are a structural aberration that can be tolerated better in acrocentric or gonosomal chromosomes. Complete RCs arise from telomere-telomere fusions. Alternatively, genomic imbalances corresponding to the ends of the chromosomal arms can be seen with RC formation. RCs are unstable in mitosis, result in mosaicism, and are associated with a "ring syndrome," which presents with growth and development phenotypes and differs from those features more frequently observed with pure terminal copy number changes. Due to variability in mosaicism, size, and genomic content, clear genotype-phenotype correlations may not always be possible. Given the rarity of RCs, this historical data is invaluable. We performed a retrospective review of individuals bearing RCs to investigate the incidence in our laboratory. This work details the methods and features seen in association with twenty-three autosomal RCs. In decreasing order, the most frequently seen autosomal RCs were 18, 22, 4, 13, 17, and 9. The additional cases detail clinical and cytogenomic events similar to those reported in RCs. As methodologies advance, insights may be gleaned from following up on these cases to improve genotype-phenotype correlations and understand the cryptic differences or other predisposing factors that lead to ring formation and development., (© 2023 Wiley Periodicals LLC.)

Published

2024

21. Gene amplification in neoplasia: A cytogenetic survey of 80 131 cases.

Author

Mandahl N, Mertens F, and Mitelman F

Subjects

Humans, Gene Amplification, Chromosome Aberrations, Cytogenetic Analysis, Sarcoma genetics, Neuroblastoma genetics, Bone Neoplasms genetics

Abstract

Gene amplification is a crucial process in cancer development, leading to the overexpression of oncogenes. It manifests cytogenetically as extrachromosomal double minutes (dmin), homogeneously staining regions (hsr), or ring chromosomes (r). This study investigates the prevalence and distribution of these amplification markers in a survey of 80 131 neoplasms spanning hematologic disorders, and benign and malignant solid tumors. The study reveals distinct variations in the frequency of dmin, hsr, and r among different tumor types. Rings were the most common (3.4%) sign of amplification, followed by dmin (1.3%), and hsr (0.8%). Rings were particularly frequent in malignant mesenchymal tumors, especially liposarcomas (47.5%) and osteosarcomas (23.4%), dmin were prevalent in neuroblastoma (30.9%) and pancreatic carcinoma (21.9%), and hsr frequencies were highest in head and neck carcinoma (14.0%) and neuroblastoma (9.0%). Combining all three amplification markers (dmin/hsr/r), malignant solid tumors consistently exhibited higher frequencies than hematologic disorders and benign solid tumors. The structural characteristics of these amplification markers and their potential role in tumorigenesis and tumor progression highlight the complex interplay between cancer-initiating gene-level alterations, for example, fusion genes, and subsequent amplification dynamics. Further research integrating cytogenetic and molecular approaches is warranted to better understand the underlying mechanisms of these amplifications, in particular, the enigmatic question of why certain malignancies display certain types of amplification. Comparing the present results with molecular genetic data proved challenging because of the diversity in definitions of amplification across studies. This study underscores the need for standardized definitions in future work., (© 2023 The Authors. Genes, Chromosomes and Cancer published by Wiley Periodicals LLC.)

Published

2024

22. [Prenatal genetic diagnosis of a case with ring chromosome 13].

Author

Sun L, Wen J, Chu G, Lai G, and He R

Subjects

Humans, Pregnancy, Female, Chromosomes, Human, Pair 13 genetics, In Situ Hybridization, Fluorescence, DNA Copy Number Variations, Prenatal Diagnosis methods, Amniotic Fluid, Ring Chromosomes

Abstract

Objective: To carry out cyto- and molecular genetic analysis for a fetus with a ring chromosome identified through non-invasive prenatal testing (NIPT)., Methods: A pregnant woman presented at the Shengjing Hospital Affiliated to China Medical University on May 11, 2021 was selected as the study subject. Maternal peripheral blood sample was screened by NIPT, and G-banded chromosomal karyotyping was carried out on amniotic fluid and peripheral blood samples from the couple. The fetus and the pregnant woman were also subjected to genomic copy number variation sequencing (CNV-seq), chromosomal microarray analysis (CMA), and fluorescence in situ hybridization (FISH) assay., Results: NIPT result suggested that the fetus had monomeric mosaicism or fragment deletion on chromosome 13. G banded chromosomal analysis showed that both the fetus and its mother had a karyotype of 47,XX,der(13)(pter→p11::q22→q10),+r(13)(::p10::q22→qter::), whilst her husband had a normal karyotype. FISH has verified the above results. No abnormality was detected with CNV-seq and CMA in both the fetus and the pregnant woman., Conclusion: The ring chromosome 13 in the fetus has derived from its mother without any deletion, duplication and mosaicism. Both the fetus and the pregnant woman were phenotypically normal.

Published

2023

23. Somatic homozygous loss of SH2B3, and a non-Robertsonian translocation t(15;21)(q25.3;q22.1) with NTRK3 rearrangement, in an adolescent with progenitor B-cell acute lymphoblastic leukemia with the iAMP21

Author

R R, Capela de Matos, Mak, Othman, G M, Ferreira, Kca, Monteso, M T, de Souza, M, Rouxinol, J B, Melo, I M, Carreira, E, Abdelhay, T, Liehr, R C, Ribeiro, and Mlm, Silva

Subjects

Chromothripsis, Cancer Research, Adolescent, Chromosomes, Human, Pair 21, Precursor Cells, B-Lymphoid, Homozygote, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Burkitt Lymphoma, Translocation, Genetic, Core Binding Factor Alpha 2 Subunit, Genetics, Humans, Ring Chromosomes, Molecular Biology, Sequence Deletion

Abstract

Intrachromosomal amplification of chromosome 21 (iAMP21) occurs in ∼2% of B-cell acute lymphoblastic leukemia (ALL) and is considered to confer a poor prognosis. The relapse risk is associated with therapy intensity, suggesting that other somatic mutations may influence iAMP21-ALL prognosis. This abnormality is characterized by multiple copies of the RUNX1 gene in chromosome 21 and appears to arise through multiple breakage-fusion bridge cycles and chromothripsis. Rob(15;21) or a ring chromosome 21 have been associated with an increased risk for iAMP21-ALL, suggesting that constitutional genetic abnormalities may also drive leukemogenesis. Here we describe homozygous deletion of the SH2B3 gene, chromothripsis of chromosome 21, and a non-Robertsonian somatic t(15;21)(q25.3;q22.1) with NTRK3 gene rearrangement in an adolescent with iAMP21-B-ALL. Molecular cytogenetic studies detected iAMP21 with aCGH analysis revealing further genomic imbalances. The RT-qPCR analysis detected elevated expression levels of RUNX1 (68-fold) and reduced expression of CDK6 (0.057-fold). Studies with constitutive cells collected from mouth swabs showed that SH2B3 biallelic deletion was a somatic alteration occurring during clonal evolution. The identification of novel secondary genetic changes was valuable to discuss sporadic iAMP21 leukemogenic mechanisms. For the first time, we show a t(15;21)(q25.3;q22.1) with NTRK3 rearrangement in an adolescent with iAMP21-ALL.

Published

2022

24. Coexistence of Growth Hormone Deficiency and Pituitary Microadenoma in a Child with Unique Mosaic Turner Syndrome: A Case Report and Literature Review

Author

Eu Gene Park, Eun-Jung Kim, Eun-Jee Kim, Hyun-Young Kim, Sun-Hee Kim, and Aram Yang

Subjects

Turner syndrome, mosaicism, ring chromosomes, growth hormone deficiency, pituitary microadenoma, Medicine (General), R5-920

Abstract

Turner syndrome (TS) is a genetic disorder with phenotypic heterogeneity caused by the monosomy or structural abnormalities of the X chromosome, and it has a prevalence of about 1/2500 females live birth. The variable clinical features of TS include short stature, gonadal failure, and skeletal dysplasia. The association with growth hormone (GH) deficiency or other hypopituitarism in TS is extremely rare, with only a few case reports published in the literature. Here, we report the first case of a patient with mosaic TS with complete GH deficiency and pituitary microadenoma, and we include the literature review. During the work-up of the patient for severe short stature, three GH provocation tests revealed peak GH levels of less than 5 ng/mL, which was compatible with complete GH deficiency. Sella magnetic resonance imaging showed an 8 mm non-enhancing pituitary adenoma with mild superior displacement of the optic chiasm. Karyotyping revealed the presence of ring chromosome X and monosomy X (46,X,r(X)/45,X/46,X,psu dic r(X;X)), which indicated a mosaic TS. It is important to consider not only chromosome analyses in females with short stature, but also the possibility of the coexistence of complete GH deficiency accompanying pituitary lesions in TS. In conclusion, the present study reports the first case of GH deficiency and pituitary adenoma in a patient with rare mosaic TS, which extends the genotype–phenotype spectrum for TS.

Published

2020

25. A rare ring chromosome 21 abnormality is associated with azoospermia in two different phenotypically normal cases.

Author

Berkay EG, Karaman B, and Başaran S

Subjects

Humans, Male, Chromosome Aberrations, Karyotyping, Chromosome Deletion, Chromosomes, Human, Y, Sex Chromosome Aberrations, Azoospermia genetics, Oligospermia genetics, Ring Chromosomes, Infertility, Male genetics

Abstract

Azoospermia can be diagnosed with spermiogram analysis, and karyotyping is the golden standard to explain the etiology. In this study, we investigated two male cases with azoospermia and male infertility for chromosomal abnormalities. Their phenotypes and physical and hormonal examinations were both normal. In karyotyping G-banding and NOR staining, a rare ring chromosome 21 abnormality was detected in the cases and no microdeletion in chromosome Y. Ring abnormality, deletion size, and deleted regions were shown with subtelomeric FISH (.ish r(21)(p13q22.3?)(D21S1446-)) and array CGH analyses. Due to the findings, bioinformatics, protein, and pathway analyses were done to detect a candidate gene through common genes in two cases' deleted regions or ring chromosome 21.

Published

2023

26. A rare case of acute megakaryoblastic leukaemia with constitutional ring chromosome 21.

Author

De John KO, De Quintal H, Mathibe MD, Albertus N, and Opie JJ

Subjects

Humans, Chromosome Aberrations, Bone Marrow, Chromosomes, Human, Pair 21 genetics, Leukemia, Megakaryoblastic, Acute diagnosis, Leukemia, Megakaryoblastic, Acute genetics, Ring Chromosomes

Published

2023

27. Intravenous methylprednisolone is a potential add on therapy for Ring chromosome 20 syndrome

Author

Vyasaraj Kalya Kishore, Lakshminarayanapuram Gopal Viswanathan, Ajay Asranna, Raghavendra Kenchiah, Ravindranadh Chowdary M, and Sanjib Sinha

Subjects

Status Epilepticus, Neurology, Seizures, Humans, Ring Chromosomes, Neurology (clinical), General Medicine, Child, Methylprednisolone

Abstract

Ring 20 syndrome is a rare cause of refractory epilepsy and non-convulsive status epilepticus in children. We report a patient with Ring 20 syndrome with refractory focal seizures and non-convulsive status epilepticus who showed good treatment response with intravenous steroids. We wish to highlight that intravenous pulse methylprednisolone is a useful treatment strategy in this setting.

Published

2022

28. <bold><italic>MYC</italic></bold> Amplification in the Form of Ring Chromosomes 8 in Acute Myeloid Leukemia with t(11;16)(q13;p11.2).

Author

Yamamoto, Katsuya, Kawamoto, Shinichiro, Kurata, Keiji, Kitao, Akihito, Mizutani, Yu, Ichikawa, Hiroya, Yakushijin, Kimikazu, Kajimoto, Kazuyoshi, Hayashi, Yoshitake, Matsuoka, Hiroshi, and Minami, Hironobu

Subjects

*CYTOGENETICS, *KARYOTYPES, *NUCLEOTIDE sequencing

Abstract

Oncogene amplification is uncommon in acute myeloid leukemia (AML). Cytogenetically, it is primarily found as double minute chromosomes (dmin) or homogeneously staining regions (hsr). A 62-year-old woman was admitted to our hospital because of anemia and thrombocytopenia. Her bone marrow was hypercellular with 78.6% myeloperoxidase- positive blasts. Some had micronuclei. The patient was diagnosed with AML M2 and remains in complete remission (CR) after induction therapy. G-banding at diagnosis showed 51,XX,t(11;16)(q13;p11.2),+r1,+mar1×4. Spectral karyotyping confirmed t(11;16) and revealed that the ring and the marker chromosomes were derived from multiple copies of ring chromosome 8. Fluorescence in situ hybridization (FISH) with a MYC probe at 8q24 detected amplified MYC signals on 1 large and 4 small ring chromosomes 8. One MYC signal was deleted from one of the 2 chromosomes 8. FISH with a FUS probe at 16p11.2 showed monoallelic deletion of FUS. Immunohistochemistry demonstrated MYC protein overexpression at diagnosis and almost negative expression in CR. These results indicate that MYC amplification could occur in ring chromosomes without dmin. A cryptic MYC deletion suggests that an episome model could be applicable to MYC amplification in ring chromosomes as observed for dmin and hsr. Furthermore, considering 2 further reported cases, t(11;16)(q13;p11) may be a very rare but recurrent translocation in AML. [ABSTRACT FROM AUTHOR]

Published

2018

29. Investigators from Mahatma Gandhi Institute of Medical Sciences Release New Data on Seizures (Molecular Characterization of De Novo Ring Chromosome 21 In a Child With Seizures, Growth Retardation, and Multiple Congenital Anomalies).

Abstract

The basis of the UCSC Genome Browser on Human (GRCh38/hg38) analysis suggests hemizygous expression of a deleted critical region of chromosome 21 in ring chromosome cell lines. Keywords: Wardha; India; Asia; Cell Nucleus; Cellular Structures; Chromosomes; Genetics; Health and Medicine; Intracellular Space; Intranuclear Space; Nervous System Diseases and Conditions; Neurologic Manifestations; Ring Chromosomes; Seizures EN Wardha India Asia Cell Nucleus Cellular Structures Chromosomes Genetics Health and Medicine Intracellular Space Intranuclear Space Nervous System Diseases and Conditions Neurologic Manifestations Ring Chromosomes Seizures 563 563 1 10/03/23 20231006 NES 231006 2023 OCT 6 (NewsRx) -- By a News Reporter-Staff News Editor at Genomics & Genetics Weekly -- Current study results on Nervous System Diseases and Conditions - Seizures have been published. Keywords for this news article include: Wardha, India, Asia, Cell Nucleus, Cellular Structures, Chromosomes, Genetics, Health and Medicine, Intracellular Space, Intranuclear Space, Nervous System Diseases and Conditions, Neurologic Manifestations, Ring Chromosomes, Seizures, Mahatma Gandhi Institute of Medical Sciences. [Extracted from the article]

Published

2023

30. Cytogenetic and molecular characterization of a patient having infertility and mild intellectual disability with a very rare unstable ring chromosome 13

Author

Murat Kaya, Ilknur Suer, Tugba Kalayci, Birsen Karaman, Sukru Ozturk, and Sukru Palanduz

Subjects

Male, Chromosomes, Human, Pair 13, Chromosomal Proteins, Non-Histone, Intellectual Disability, Karyotyping, Infertility, Humans, Ring Chromosomes, General Medicine, Phosphoproteins

Abstract

Introduction Ring chromosomes arise from breakage and fusion at distal regions of short and long arms of the chromosomes. The effect of the ring chromosome on the phenotype may vary widely depending on the amount of the deletion in the chromosomal areas and genes implicated in these regions. Case presentation We present a 35-year-old male patient with infertility and mild intellectual disability (MID) who has de novo ring 13 (r(13)) chromosomes. To determine chromosomal abnormality, we performed karyotype analysis, Y chromosome microdeletion analysis, FISH, and aCGH techniques. Conclusion The patient’s karyotype analysis result was mos46,XY,r(13)(p13q34)[75]/45,XY,-13[14]/46,XY,dic (13;13)[8]/47,XY,r(13), + r(13)[2]/46,XY,tetrac r(13;13;13;13)[1]. FISH analysis supported the findings of the cytogenetic analysis. Y microdeletion analysis showed that the AZF region was intact. On aCGH analysis, we detected a 1.5 megabase deletion at the end of chromosome 13, including the CHAMP1 gene. The loss of the CHAMP1 gene, in particular, may explain our patient's MID, and the other deleted genes at 13q34 may explain our patient's infertility.

Published

2022

31. Prenatal diagnosis of a fetus with mosaic ring chromosome 13: Case report and review of the literature

Author

Ruizhi Liu, Xiaonan Hu, Hongguo Zhang, Qingyang Shi, Leilei Li, Yuting Jiang, and Zhu-Ming Hu

Subjects

medicine.medical_specialty, Amniotic fluid, Karyotype, Ring chromosome, Prenatal diagnosis, Chromosome Disorders, Young Adult, Pregnancy, Humans, Medicine, Ring Chromosomes, Increased nuchal translucency, Gynecology, Fetus, Chromosomes, Human, Pair 13, medicine.diagnostic_test, Mosaicism, business.industry, Obstetrics and Gynecology, Gynecology and obstetrics, Microarray Analysis, Nuchal translucency, Karyotyping, Cytogenetic Analysis, Amniocentesis, RG1-991, Gestation, Female, Nuchal Translucency Measurement, business, Abortion, Eugenic, Chromosomal microarray analysis, Genetic counseling

Abstract

Objective To diagnose the ring chromosome 13 (r(13)) in a fetus, and analyze the genotype–phenotype correlation. Case report A 26-year-old woman who was second pregnancy, underwent amniocentesis at 18 weeks of gestation because of the increased nuchal translucency (NT). Prenatal ultrasound showed the NT thickness was 3.5 mm at 12+1 weeks of gestation and nuchal fold (NF) was 6.1 mm at 18 weeks of gestation, and amniotic fluid karyotype analysis revealed mosaic r(13). CMA detected a 16.293 Mb duplication at 13q21.32q31.1 and 31.303 Mb deletion at 13q31.1q34. Conclusion R(13) is a very rare chromosomal abnormality. Cytogenetic examination combined with CMA can provide accurate diagnosis and effective information for genetic counseling.

Published

2021

32. Complex biology of constitutional ring chromosomes structure and (in)stability revealed by somatic cell reprogramming

Author

Inna E. Pristyazhnyuk, A.G. Menzorov, S. A. Vasilyev, T. V. Nikitina, Oleg L. Serov, A.A. Khabarova, M.E. Lopatkina, D. A. Fedotov, I. N. Lebedev, Yu. A. Minina, Yu.S. Yakovleva, A. A. Kashevarova, and M.M. Gridina

Subjects

Male, Monosomy, Cell division, Adolescent, Somatic cell, Science, Ring chromosome, Induced Pluripotent Stem Cells, Karyotype, Chromosomal translocation, Biology, Article, Chromosomal Instability, medicine, Genetics, Humans, Ring Chromosomes, Child, Mitosis, Comparative Genomic Hybridization, Multidisciplinary, Stem Cells, Infant, medicine.disease, Cellular Reprogramming, Molecular biology, Child, Preschool, Karyotyping, Medicine, Female, Reprogramming

Abstract

Human ring chromosomes are often unstable during mitosis, and daughter cells can be partially or completely aneuploid. We studied the mitotic stability of four ring chromosomes, 8, 13, 18, and 22, in long-term cultures of skin fibroblasts and induced pluripotent stem cells (iPSCs) by GTG karyotyping and aCGH. Ring chromosome loss and secondary aberrations were observed in all fibroblast cultures except for r(18). We found monosomy, fragmentation, and translocation of indexed chromosomes. In iPSCs, aCGH revealed striking differences in mitotic stability both between iPSC lines with different rings and, in some cases, between cell lines with the same ring chromosome. We registered the spontaneous rescue of karyotype 46,XY,r(8) to 46,XY in all six iPSC lines through ring chromosome loss and intact homologue duplication with isoUPD(8)pat occurrence, as proven by SNP genotype distribution analysis. In iPSCs with other ring chromosomes, karyotype correction was not observed. Our results suggest that spontaneous correction of the karyotype with ring chromosomes in iPSCs is not universal and that pluripotency is compatible with a wide range of derivative karyotypes. We conclude that marked variability in the frequency of secondary rearrangements exists in both fibroblast and iPSC cultures, expanding the clinical significance of the constitutional ring chromosome.

Published

2021

33. [A rare case of dicentric ring chromosome and derivative ring chromosome Chimera]

Author

Junzhen, Zhu, Xiaoping, Yu, Xiaofeng, Qi, Qinying, Cao, Wenshuang, Zhu, Dan, Yang, Haoyu, Zhang, Zhanyun, Song, Shibo, Wang, and Cuixia, Wang

Subjects

Adult, Dacarbazine, Humans, Female, Chromosome Disorders, Ring Chromosomes, Chromosome Deletion, Infertility, Female, Chromosome Banding

Abstract

Utilize high-resolution chromosome analysis and microarray detection to determine the genetic etiology of infertility of a 32-year old female patient.The peripheral blood of the patient was cultured for high-resolution chromosome G and C banding karyotype analysis, and then 750K SNP-Array chip detection was performed.Karyotype analysis results showed that the patient's karyotype was 45,XX,-13 [7]/46,XX,r(13) (p13q34) [185]/46,XX,dic r(13;13)(p13q34;p13q34) [14]/ 47,XX,+der(13;13;13;13) (p13q34;p13q34;p13q34; p13q34), dic r(13;13) [1]/ 46,XX [3]. The microarray results showed that the patient had a 3.3 Mb deletion in the 13q34 segment of chromosome 13, which may be related to infertility.Infertility of the patient reported in this article may be related to the deletion of chromosome segment (13q34-qter).

Published

2022

34. B-cell acute lymphoblastic leukemia with iAMP21 in a patient with Down syndrome due to a constitutional isodicentric chromosome 21

Author

Angela M. Verdoni, Megan L. Zilla, Grant Bullock, Terri L. Guinipero, Julia Meade, and Svetlana A. Yatsenko

Subjects

Chromosome Aberrations, Chromosomes, Human, Pair 21, Genetics, Humans, Ring Chromosomes, Down Syndrome, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Child, Burkitt Lymphoma, Genetics (clinical), Translocation, Genetic

Abstract

Pediatric B-cell acute lymphoblastic leukemia (B-ALL) is associated with various specific cytogenetic and molecular markers that have significant influence on treatment and prognosis. A subset of children has a much higher risk of developing B-ALL due to constitutional genetic alterations such as trisomy 21 (Down's syndrome). In these patients, B-ALL is often associated with specific genomic profiles leading to leukemic transformation. In rare cases, constitutional structural chromosomal abnormalities involving chromosome 21, such as the der(15;21) Robertsonian translocation and a ring 21 chromosome, have been associated with intrachromosomal amplification of chromosome 21 (iAMP21) B-ALL. Here, we report the development of B-ALL in a child with Down's syndrome who carries a constitutional isodicentric chromosome 21 [idic(21)], described previously by Putra et al., 2017. This idic(21) appeared to be unstable during mitosis, leading to somatic rearrangements consistent with iAMP21 amplification, resulting in the development of leukemia. In this case, a single constitutional structural chromosome 21 rearrangement resulted in a B-ALL with Down syndrome-associated genomic lesions as well as genomic lesions not common to the Down syndrome subtype of B-ALL. Our findings highlight the need for counseling of individuals with constitutional structural chromosome 21 rearrangements regarding their risks of developing a B-ALL.

Published

2022

35. A novel system for correcting large-scale chromosomal aberrations: ring chromosome correction via reprogramming into induced pluripotent stem cell (iPSC).

Author

Kim, Taehyun, Plona, Kathleen, and Wynshaw-Boris, Anthony

Subjects

*CHROMOSOMES, *CHROMOSOME abnormalities, *INDUCED pluripotent stem cells, *GENOME editing, *GENE therapy

Abstract

Approximately 1 in 500 newborns are born with chromosomal abnormalities that include trisomies, translocations, large deletions, and duplications. There is currently no therapeutic approach for correcting such chromosomal aberrations in vivo or in vitro. When we attempted to produce induced pluripotent stem cell (iPSC) models from patient-derived fibroblasts that contained ring chromosomes, we found that the ring chromosomes were eliminated and replaced by duplicated normal copies of chromosomes through a mechanism of uniparental isodisomy (Bershteyn et al. 2014, Nature 507:99). The discovery of this previously unforeseen system for aberrant chromosome correction during reprogramming enables us for the first time to model and understand this process of cell-autonomous correction of ring chromosomes during human patient somatic cell reprograming to iPSCs. This knowledge could lead to a potential therapeutic strategy to correct common large-scale chromosomal aberrations, termed 'chromosome therapy'. [ABSTRACT FROM AUTHOR]

Published

2017

36. [Clinical features and genetic analysis of two fetuses with ring chromosome 21 mosaicism].

Author

Ji Y, Xu Y, Sun L, Ge Y, Cai M, and Wu Q

Subjects

Pregnancy, Female, Humans, Vena Cava, Superior, Chromosome Aberrations, Prenatal Diagnosis, Microarray Analysis, Fetus diagnostic imaging, Mosaicism, Ring Chromosomes

Abstract

Objective: To investigate the perinatal clinical phenotype and genetic characteristics of two fetuses with ring chromosome 21 mosaicisms., Methods: Two fetuses who were diagnosed at the Xiamen Maternal and Child Health Care Hospital in November 2021 were selected as the study subjects. Clinical data of the two fetuses were collected. Conventional G-banded karyotyping and chromosomal microarray analysis (CMA) were carried out for the fetuses and their parents., Results: Prenatal ultrasonography of fetus 1 has revealed absence of nasal bone, ventricular septal defect, persistent left superior vena cava, and mild tricuspid regurgitation. Chromosomal karyotyping was 46,X?,dic r(21;21)(p12q22;q22p12)[41]/45,X?,-21[9]. CMA has revealed a 30.00 Mb quadruplication at 21q11.2q22.3 and a 3.00 Mb deletion at 21q22.3. For fetus 2, ultrasonography has revealed pointed echo of the nasal bone. The fetus was found to have a karyotype of 46,X?,r(21)(p12q22)[83]/45,X?,-21[14]/46,X?,dic r(21;21)(p12q22;q22p12)[3]. CMA has revealed a 5.10 Mb quadruplication at 21q22.12q22.3 and a 2.30 Mb deletion at 21q22.3., Conclusion: The perinatal phenotype of the two fetuses with ring chromosome 21 mosaicisms is related to the duplication of chromosomal segments near the breakpoints of the chromosomal deletions. The combined chromosomal karyotyping and CMA has enabled prenatal diagnosis and genetic counseling for these families.

Published

2023

37. Response to growth hormone therapy in ring chromosome 15: Review and evidence from a new case on possible beneficial effect in neurodevelopment.

Author

Wannes S, El Ahmer I, Rjiba K, Jemmali N, Abdallah HH, Haj RB, Achour A, Bouzidi H, Saad A, Mougou S, and Mahjoub B

Subjects

Child, Humans, Child, Preschool, Growth Hormone, Growth Disorders drug therapy, Growth Disorders genetics, Syndrome, Human Growth Hormone therapeutic use, Ring Chromosomes, Dwarfism drug therapy

Abstract

Type 1 Insulin-like Growth Factor Receptor(IGF1R) plays a fundamental role in normal growth and development. Its disruption is usually characterized by severe intrauterine and postnatal growth retardation, microcephaly and neurodevelopmental delay.The efficacy of recombinant human growth hormone treatment remains a challenge for children with IGF1 resistance and pathogenic mutations of IGF1R, with limited data in patients carrying the most severe form of IGF1R defect, the ring chromosome 15., Subject and Method: We tested a high dose of rhGH in a new patient with ring chromosome 15, as confirmed by karyotype and CGH array. We performed a systematic review, and all published r(15) syndrome cases treated by growth hormone(GH) up to April 2023 were searched, and their response to GH therapy was recorded and summarized., Results: Twelve patients with ring chromosome 15 received GH therapy according to a literature review. We expand the spectrum by the 13th case treated by GH, and we report an impressive improvement in intellectual performance and progressive catch-up growth after 5 and 20 months of follow-up. By introducing our new case in the analysis, the sex ratio was 3:10, and GH therapy was started at the age of 5.5 (3/9.4) (years) for an age of diagnosis of 4.75 (1.3/9.5) (years). The height before GH therapy was -5.1(-5.9/-4.1) SDS. The median duration of treatment was 1.7(0.9/2) (years), with a median height gain of 1(0.3/1.8) SDS and an improvement in growth velocity of 4.1(2.8/5.3) (cm/year)., Conclusion: GH seems to be effective for r(15) syndrome patients with short stature., Competing Interests: Declaration of Competing Interest Selmen Wannes was a member on advisory boards of pfizer KSA, rare growth disorder Adv Brd and long acting Growth Hormone Adv Brd. The co-authors do not have any conflicts of interest relevant to this manuscript., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023

38. Consensus recommendations on counselling in Phelan-McDermid syndrome, with special attention to recurrence risk and to ring chromosome 22.

Author

Koza SA, Tabet AC, Bonaglia MC, Andres S, Anderlid BM, Aten E, Stiefsohn D, Evans DG, van Ravenswaaij-Arts CMA, and Kant SG

Subjects

Adolescent, Female, Humans, Pregnancy, Chromosome Deletion, Chromosomes, Human, Pair 22 genetics, Counseling, Chromosome Disorders genetics, Neurofibromatosis 2 genetics, Ring Chromosomes

Abstract

This paper focuses on genetic counselling in Phelan-McDermid syndrome (PMS), a rare neurodevelopmental disorder caused by a deletion 22q13.3 or a pathogenic variant in SHANK3. It is one of a series of papers written by the European PMS consortium as a consensus guideline. We reviewed the available literature based on pre-set questions to formulate recommendations on counselling, diagnostic work-up and surveillance for tumours related to ring chromosome 22. All recommendations were approved by the consortium, which consists of professionals and patient representatives, using a voting procedure. PMS can only rarely be diagnosed based solely on clinical features and requires confirmation via genetic testing. In most cases, the family will be referred to a clinical geneticist for counselling after the genetic diagnosis has been made. Family members will be investigated and, if indicated, the chance of recurrence discussed with them. Most individuals with PMS have a de novo deletion or a pathogenic variant of SHANK3. The 22q13.3 deletion can be a simple deletion, a ring chromosome 22, or the result of a parental balanced chromosomal anomaly, influencing the risk of recurrence. Individuals with a ring chromosome 22 have an increased risk of NF2-related schwannomatosis (formerly neurofibromatosis type 2) and atypical teratoid rhabdoid tumours, which are associated with the tumour-suppressor genes NF2 and SMARCB1, respectively, and both genes are located on chromosome 22. The prevalence of PMS due to a ring chromosome 22 is estimated to be 10-20%. The risk of developing a tumour in an individual with a ring chromosome 22 can be calculated as 2-4%. However, those individuals who do develop tumours often have multiple. We recommend referring all individuals with PMS and their parents to a clinical geneticist or a comparably experienced medical specialist for genetic counselling, further genetic testing, follow-up and discussion of prenatal diagnostic testing in subsequent pregnancies. We also recommend karyotyping to diagnose or exclude a ring chromosome 22 in individuals with a deletion 22q13.3 detected by molecular tests. If a ring chromosome 22 is found, we recommend discussing personalised follow-up for NF2-related tumours and specifically cerebral imaging between the age of 14 and 16 years., (Copyright © 2023 The Authors. Published by Elsevier Masson SAS.. All rights reserved.)

Published

2023

39. Recurring germline mosaicism in a family due to reversion of an inherited derivative chromosome 8 from an 8;21 translocation with interstitial telomeric sequences.

Author

Bi W, Yuan B, Liu P, Murry JB, Qin X, Xia F, Quach T, Cooper LM, Wiszniewska J, Hixson P, Peacock S, Tonk VS, Huff RW, Ortega V, Lupski JR, Scherer SE, Littlejohn RO, Velagaleti GVN, Roeder ER, and Cheung SW

Subjects

Humans, Chromosomes, Human, Pair 8 genetics, Karyotyping, In Situ Hybridization, Fluorescence, Chromosome Aberrations, Translocation, Genetic genetics, Germ Cells, Mosaicism, Ring Chromosomes

Abstract

Background: Mosaicism for chromosomal structural abnormalities, other than marker or ring chromosomes, is rarely inherited., Methods: We performed cytogenetics studies and breakpoint analyses on a family with transmission of mosaicism for a derivative chromosome 8 (der(8)), resulting from an unbalanced translocation between the long arms of chromosomes 8 and 21 over three generations., Results: The proband and his maternal half-sister had mosaicism for a der(8) cell line leading to trisomy of the distal 21q, and both had Down syndrome phenotypic features. Mosaicism for a cell line with the der(8) and a normal cell line was also detected in a maternal half-cousin. The der(8) was inherited from the maternal grandmother who had four abnormal cell lines containing the der(8), in addition to a normal cell line. One maternal half-aunt had the der(8) and an isodicentric chromosome 21 (idic(21)). Sequencing studies revealed microhomologies at the junctures of the der(8) and idic(21) in the half-aunt, suggesting a replicative mechanism in the rearrangement formation. Furthermore, interstitial telomeric sequences (ITS) were identified in the juncture between chromosomes 8 and 21 in the der(8)., Conclusion: Mosaicism in the proband, his half-sister and half-cousin resulting from loss of chromosome 21 material from the der(8) appears to be a postzygotic event due to the genomic instability of ITS and associated with selective growth advantage of normal cells. The reversion of the inherited der(8) to a normal chromosome 8 in this family resembles revertant mosaicism of point mutations. We propose that ITS could mediate recurring revertant mosaicism for some constitutional chromosomal structural abnormalities., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2023. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2023

40. Human Ring Chromosomes – New Insights for their Clinical Significance

Author

Guilherme R.S., Klein E, Hamid A.B., Bhatt S, Volleth M, Polityko A, Kulpanovich A, Dufke A, Albrecht B, Morlot S, Brecevic L, Petersen M.B., Manolakos E, Kosyakova N, and Liehr T

Subjects

ring chromosomes, fluorescence in situ hybridization (fish), genotype-phenotype correlations, Genetics, QH426-470

Abstract

Twenty-nine as yet unreported ring chromosomes were characterized in detail by cytogenetic and molecular techniques. For FISH (fluorescence in situ hybridization) previously published high resolution approaches such as multicolor banding (MCB), subcentromere-specific multi-color-FISH (cenM-FISH) and two to three-color-FISH applying locus-specific probes were used. Overall, ring chromosome derived from chromosomes 4 (one case), 10 (one case), 13 (five cases), 14, (three cases), 18 (two cases), 21 (eight cases), 22 (three cases), X (five cases) and Y (one case) were studied. Eight cases were detected prenatally, eight due developmental delay and dysmorphic signs, and nine in connection with infertility and/or Turner syndrome. In general, this report together with data from the literature, supports the idea that ring chromosome patients fall into two groups: group one with (severe) clinical signs and symptoms due to the ring chromosome and group two with no obvious clinical problems apart from infertility.

Published

2013

41. Chromosome 14 deletions, rings, and epilepsy genes: A riddle wrapped in a mystery inside an enigma

Author

Alessandro Vaisfeld, Giuseppe Gobbi, Serena Spartano, Giovanni Neri, and Annamaria Vezzani

Subjects

Cytoplasmic Dyneins, Ribonuclease III, 0301 basic medicine, Drug Resistant Epilepsy, Mutation, Missense, Vesicular Transport Proteins, Nerve Tissue Proteins, Molecular evidence, Biology, Ring 14 syndrome, Ring (chemistry), Retina, Craniofacial Abnormalities, DEAD-box RNA Helicases, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Chromosome (genetic algorithm), Intellectual Disability, Presenilin-1, medicine, Humans, Ring Chromosomes, Deletion syndrome, Eye Abnormalities, Gene, Chromosomes, Human, Pair 14, Genetics, Otx Transcription Factors, Breakpoint, Nuclear Proteins, Forkhead Transcription Factors, medicine.disease, DNA-Binding Proteins, Phenotype, 030104 developmental biology, Neurology, Microcephaly, Neurology (clinical), Chromosome Deletion, Carrier Proteins, 030217 neurology & neurosurgery, Transcription Factors

Abstract

The ring 14 syndrome is a rare condition caused by the rearrangement of one chromosome 14 into a ring-like structure. The formation of the ring requires two breakpoints and loss of material from the short and long arms of the chromosome. Like many other chromosome syndromes, it is characterized by multiple congenital anomalies and developmental delays. Typical of the condition are retinal anomalies and drug-resistant epilepsy. These latter manifestations are not found in individuals who are carriers of comparable 14q deletions without formation of a ring (linear deletions). To find an explanation for this apparent discrepancy and gain insight into the mechanisms leading to seizures, we reviewed and compared literature cases of both ring and linear deletion syndrome with respect to both their clinical manifestations and the role and function of potentially epileptogenic genes. Knowledge of the epilepsy-related genes in chromosome 14 is an important premise for the search of new and effective drugs to combat seizures. Current clinical and molecular evidence is not sufficient to explain the known discrepancies between ring and linear deletions.

Published

2020

42. A Revisited Diagnosis of Collagen VI Related Muscular Dystrophy in a Patient with a Novel COL6A2 Variant and 21q22.3 Deletion

Author

Pelin Ozlem Simsek-Kiper, Gülen Eda Utine, Sumeyra Oguz, Mehmet Alikasifoglu, Fatma Bilge Ergen, and Goknur Haliloglu

Subjects

Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Contracture, Proximal muscle weakness, Adolescent, Chromosomes, Human, Pair 21, Ring chromosome, Collagen Type VI, Muscular Dystrophies, Muscle hypertrophy, 03 medical and health sciences, 0302 clinical medicine, Collagen VI, Humans, Medicine, Ring Chromosomes, Allele, Muscular dystrophy, business.industry, Muscle weakness, General Medicine, medicine.disease, Hypotonia, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Chromosome Deletion, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

The genetic etiology of collagen VI related muscular dystrophies is heterogenous. Genomic deletions in one allele involving COL6A2 or both COL6A1 and COL6A2 unmasking a pathogenic variant in the second nondeleted allele have been described in the etiology. We aimed to report the clinical and molecular findings of a 13-year-old boy with ring chromosome 21 who presented to our clinic with easy fatigability, muscle weakness, and waddling gait. Phenotypic delineation along with chromosomal microarray analysis and DNA sequencing were performed. Affymetrix CytoScan Optima array platform and DNA sequencing revealed a 2,202 kb de novo deletion at 21q22.3, including COL6A1 and COL6A2, and a novel heterozygous variant at position c.2875G > A;p.(Glu959Lys) in COL6A2, respectively. Before his admission to our center, the patient was evaluated for hypotonia elsewhere when he was 15 months old. He was diagnosed with ring chromosome 21 on peripheral blood karyotype analysis; however, no further assessment was performed at that time. He had normal growth with mild dysmorphic facial features, distal laxity, gastrocnemius hypertrophy, proximal muscle weakness, increased lordotic posture with mild flexion contractures at the knees, and gait disturbance. Although the phenotype does not fit into classical Ullrich congenital muscular dystrophies, muscle magnetic resonance imaging (MRI) revealed a complementary pattern consistent with collagen VI related myopathies. Genetic testing confirmed the clinical diagnosis as well. This patient yet represents another example of the effect of large genomic deletions leading to recessive disorders through unmasking a pathogenic variant in the second nondeleted allele.

Published

2020

43. Café au Lait Macules and Associated Genetic Syndromes

Author

Sharon Anderson

Subjects

medicine.medical_specialty, Neurofibromatosis 1, Ring chromosome, Population, Fibrous Dysplasia, Polyostotic, McCune–Albright syndrome, 03 medical and health sciences, 0302 clinical medicine, Neoplastic Syndromes, Hereditary, 030225 pediatrics, medicine, Humans, Genetic Predisposition to Disease, Ring Chromosomes, 030212 general & internal medicine, Birthmark, Neurofibromatosis, education, Legius syndrome, education.field_of_study, Brain Neoplasms, business.industry, Cafe-au-Lait Spots, Noonan Syndrome, medicine.disease, Dermatology, Cafe-au-lait macules, Pediatrics, Perinatology and Child Health, Colorectal Neoplasms, business, Noonan Syndrome with Multiple Lentigines

Abstract

Cafe au lait macules (CALMs) are a common, isolated dermatologic finding in the general population. But when do these irregularly shaped, jagged-edged, flat, hyperpigmented birthmarks suggest something that may warrant referral? Most pediatric providers are familiar with the association of CALMs and neurofibromatosis type 1. There are, however, other genetic conditions associated with these seemingly benign skin spots. This article provides an overview of CALMs, followed by a summary of several conditions associated with CALMs ranging from the most common (neurofibromatosis type 1) to rare, ring chromosome syndromes. It reviews the associated gene(s), pattern of inheritance, incidence, presenting symptoms, diagnosis, and management for these genetic conditions.

Published

2020

44. Prenatal diagnosis and molecular cytogenetic characterization of mosaic ring chromosome 21 associated with low PAPP-A and low PlGF in the first-trimester maternal serum screening

Author

Chih-Ping Chen, Liang-Kai Wang, Schu-Rern Chern, Peih-Shan Wu, Shin-Wen Chen, Fang-Tzu Wu, Chen-Chi Lee, Li-Feng Chen, and Wayseen Wang

Subjects

Comparative Genomic Hybridization, Pregnancy Trimester, First, Adolescent, Pregnancy, Prenatal Diagnosis, Cytogenetic Analysis, Obstetrics and Gynecology, Humans, Pregnancy-Associated Plasma Protein-A, Chromosome Disorders, Female, Ring Chromosomes, Placenta Growth Factor

Abstract

We present diagnosis and molecular cytogenetic characterization of mosaic ring chromosome 21 [r(21)].A 17-year-old, gravida 2, para 1, woman underwent amniocentesis at 17 weeks of gestation because of an abnormal result of the first-trimester maternal serum screening for Down syndrome with a free β-hCG level of 1.736 multiples of the median (MoM), a pregnancy associated plasma protein-A (PAPP-A) level of 0.275 MoM, a placental growth factor (PlGF) level of 0.281 MoM, a Down syndrome risk of 1:222 and a preeclampsia risk of 1:175. Cytogenetic analysis of cultured amniocytes revealed the result of 46,XX,r(21) (p12q22.3)[19]/45,XX,-21[13]. Array comparative genomic hybridization (aCGH) analysis of cultured amniocytes revealed the result of arr [GRCh37] 21q11.2q22.2 (15,485,008-40,625,594) × 1∼2, 21q22.2q22.3 (40,703,792-46,682,184) × 2∼3, 21q22.3 (46,761,631-48,084,156) × 1, consistent with mosaic monosomy 21 and r(21) (p12q22.3). The pregnancy was subsequently terminated, and a malformed fetus was delivered with low-set ears and hypotelorism. Postnatal cytogenetic analysis revealed a karyotype of 46,XX,r(21) (p12q22.3)[30]/45,XX,-21[8]/46,XX,idic r(21) (p12q22.3)[2] in the cord blood, 46,XX,r(21) (p12q22.3)[34]/45,XX,-21[6] in the skin, 46,XX,r(21) (p12q22.3)[37]/45,XX,-21[3] in the umbilical cord and 46,XX,dup(21) (q22.2q22.3)[32]/46,XX,r(21) (p12q22.3)[8] in the placenta. aCGH analysis of cord blood revealed the result of arr 21q11.2q22.2 (15,499,847-40,662,581) × 2.3, arr 21q22.2q22.3 (40,703,792-46,682,184) × 3.6, arr 21q22.3 (46,761,632-48,090,317) × 1, consistent with mosaic duplication of 21q11.2-q22.2 and 21q22.2-q22.3, and a 1.33-Mb 21q22.3 deletion encompassing the genes of COL18A1, SLC19A1, PCBP3, COL6A1, COL6A2, FTCD, LSS, MCM3AP, YBEY, PCNT, DIP2A, S100B and PRMT2.Mosaic r(21) at amniocentesis may be associated with monosomy 21, idic r(21) and dup(21), and low PAPP-A and low PlGF in the first-trimester maternal serum screening.

Published

2021

45. Multiple desmoplastic Spitz nevi with BRAF fusions in a patient with ring chromosome 7 syndrome

Author

Alessio Giubellino, Sheilagh Maguiness, Timothy H. McCalmont, Iwei Yeh, Swapna S. Vemula, Boris C. Bastian, and Simon F. Roy

Subjects

0301 basic medicine, Male, Pathology, Skin Neoplasms, Ring chromosome, Chromosome Disorders, Medical and Health Sciences, 0302 clinical medicine, Ring Chromosomes, skin and connective tissue diseases, ring chromosome 7, ring chromosome seven, Oncogene Proteins, integumentary system, medicine.diagnostic_test, Melanocytic nevus, Biological Sciences, Spitz nevus, Oncology, 030220 oncology & carcinogenesis, %22">Fish , Pair 7, spitzoid, Human, Proto-Oncogene Proteins B-raf, Adult, medicine.medical_specialty, BRAF fusion, Dermatology, Epithelioid and Spindle Cell, Right knee, Article, General Biochemistry, Genetics and Molecular Biology, Chromosomes, 03 medical and health sciences, medicine, Humans, In patient, melanocytic nevi, melanocytic nevus, Fusion, neoplasms, Benign neoplasms, Nevus, Ear Neoplasms, BRAF gene, business.industry, Dermatology & Venereal Diseases, medicine.disease, 030104 developmental biology, business, Spitz tumor, Fluorescence in situ hybridization

Abstract

Patients with non-supernumerary ring chromosome 7 syndrome have an increased incidence of hemangiomas, cafe-au-lait spots, and melanocytic nevi. The mechanism for the increased incidence of these benign neoplasms is unknown. We present the case of a 22-year-old man with ring chromosome 7 and multiple melanocytic nevi. Two nevi, one on the right ear and the other on the right knee, were biopsied and diagnosed as desmoplastic Spitz nevi. Upon targeted next-generation DNA sequencing, both harbored BRAF fusions. Copy number alterations and fluorescence in situ hybridization (FISH) for BRAF suggested that the fusions arose on the ring chromosome 7. Hence, one reason for increased numbers of nevi in patients with non-supernumerary ring chromosome 7 syndrome may be increased likelihood of BRAF fusions, due to the instability of the ring chromosome.

Published

2021

46. Expanding the Neurological Phenotype of Ring Chromosome 10 Syndrome: A Case Report and Review of the Literature

Author

Chiara Locatelli, Lucia Maltoni, Hodman Ahmed Sheikh Maye, Claudio Graziano, Jacopo Pruccoli, Duccio Maria Cordelli, Pruccoli J., Graziano C., Locatelli C., Maltoni L., Sheikh Maye H.A., and Cordelli D.M.

Subjects

Microcephaly, Pediatrics, Ring Chromosome, ZMYND11, Neurology, magnetic resonance imaging (MRI), Transcription Factor, Developmental Disabilities, Ring chromosome, Cell Cycle Proteins, Chromosome Disorders, QH426-470, r10, Intellectual disability, Cell Cycle Protein, Medicine, Ring Chromosomes, Genetics (clinical), Neuroradiology, Brain, Syndrome, Hypotonia, DNA-Binding Proteins, medicine.anatomical_structure, Phenotype, Child, Preschool, Female, medicine.symptom, Co-Repressor Proteins, Human, medicine.medical_specialty, DNA-Binding Protein, Developmental Disabilitie, r(10), Short stature, Co-Repressor Protein, Article, Intellectual Disability, EBF3, Genetics, neuroradiology, Humans, business.industry, Chromosomes, Human, Pair 10, neurology, medicine.disease, Chromosome Disorder, Posterior cranial fossa, business, ring chromosome 10, Transcription Factors

Abstract

Ring chromosome 10 [r(10)] syndrome is a rare genetic condition, currently described in the medical literature in a small number of case report studies. Typical clinical features include microcephaly, short stature, facial dysmorphisms, ophthalmologic abnormalities and genitourinary malformations. We report a novel case of r(10) syndrome and review the neurological and neuroradiological phenotypes of the previously described cases. Our patient, a 3 year old Italian girl, represents the 20th case of r(10) syndrome described to date. Intellectual disability/developmental delay (ID/DD), microcephaly, strabismus, hypotonia, stereotyped/aggressive behaviors and electroencephalographic abnormalities were identified in our patient, and in a series of previous cases. A brain MRI disclosed a complex malformation involving both the vermis and cerebellar hemispheres, in the literature, posterior cranial fossa abnormalities were documented by CT scan in another case. Two genes deleted in our case (ZMYND11 in 10p and EBF3 in 10q) are involved in autosomal dominant neurodevelopmental disorders, characterized by different expressions of brain and posterior cranial fossa abnormalities, ID/DD, hypotonia and behavioral problems. Our case expands the neurological and neuroradiological phenotype of r(10) syndrome. Although r(10) syndrome represents an extremely rare condition, with a clinical characterization limited to case reports, the recurrence of specific neurological and neuroradiological features suggests the need for specific genotype-phenotype studies.

Published

2021

47. The relationship of the efficiency of energy conversion into growth as an indicator for the determination of the optimal dose for mutation breeding with the appearance of chromosomal abnormalities and incomplete mitosis after gamma irradiation of kernels of Triticum turgidum ssp. durum L.

Author

Von Well E, Fossey A, and Booyse M

Subjects

Plant Breeding, Mitosis, Triticum genetics, Ring Chromosomes

Abstract

The study aim was to determine the optimal gamma irradiation dose for mutation breeding in Triticum turgidum ssp. durum L. Root, shoot and seedling growth, as well as the efficiency of energy conversion into growth were determined to examine the growth retardation effects of gamma irradiation that are the result of DNA damage (bridges, ring chromosomes, micronuclei, incomplete mitosis) in Triticum turgidum ssp. durum L. The kernels were irradiated with doses of 50, 150, 250 and 350 Gy using a 60 Cobalt gamma-ray source. The kernels were placed in germination paper at 25 °C to grow for a 132 h period for the determination of shoot and root growth and the efficiency of energy conversion into growth. Root tips were collected and fixated over a 47.5 h growth period for the determination of the chromosomal abnormalities and incomplete mitosis. The control differed highly significantly (p < 0.01) from irradiated samples at all doses in root growth and from 250 to 350 Gy samples in shoot growth and the efficiency of energy conversion into growth. There was a highly significant (p < 0.01) increase in the number of bridges and micronuclei between 50 Gy samples and samples irradiated with the higher irradiation doses while 50 Gy samples differed only from 250 and 350 Gy samples regarding ring chromosomes and interphase cells with incomplete mitosis. Root and seedling growth on the one hand and the efficiency of energy conversion into growth on the other were found to be measuring different effects of gamma irradiation on plant growth. The latter was used for the determination of the optimal dose for mutation breeding as 155.52 Gy., (© 2023. The Author(s).)

Published

2023

48. Optical Genome Mapping Reveals and Characterizes Recurrent Aberrations and New Fusion Genes in Adult ALL.

Author

Vieler LM, Nilius-Eliliwi V, Schroers R, Vangala DB, Nguyen HP, and Gerding WM

Subjects

Humans, In Situ Hybridization, Fluorescence methods, Karyotyping, Acute Disease, Chromosome Mapping, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Ring Chromosomes

Abstract

(1) Background: In acute lymphoblastic leukemia (ALL) the genetic characterization remains challenging. Due to the genetic heterogeneity of mutations in adult patients, only a small proportion of aberrations can be analyzed with standard routine diagnostics. Optical genome mapping (OGM) has recently opened up new possibilities for the characterization of structural variants on a genome-wide level, thus enabling simultaneous analysis for a broad spectrum of genetic aberrations. (2) Methods: 11 adult ALL patients were examined using OGM. (3) Results: Genetic results obtained by karyotyping and FISH were confirmed by OGM for all patients. Karyotype was redefined, and additional genetic information was obtained in 82% (9/11) of samples by OGM, previously not diagnosed by standard of care. Besides gross-structural chromosome rearrangements, e.g., ring chromosome 9 and putative isodicentric chromosome 8q, deletions in CDKN2A/2B were detected in 7/11 patients, defining an approx. 20 kb minimum region of overlap, including an alternative exon 1 of the CDKN2A gene. The results further confirm recurrent ALL aberrations (e.g., PAX5 , ETV6 , VPREB1 , IKZF1 ). (4) Conclusions: Genome-wide OGM analysis enables a broad genetic characterization in adult ALL patients in one single workup compared to standard clinical testing, facilitating a detailed genetic diagnosis, risk-stratification, and target-directed treatment strategies.

Published

2023

49. Chromosome Structural Alteration an Unusual Abnormality Characterizing Human Neoplasia.

Author

Movafagh, Abolfazl, Zare-Abdollahi, Davood, Emamalizadeh, Babak, Shahvaisizadeh, Farhad, Mansouri, Neda, Hashemi, Mehrdad, Pour, Atefeh Heidary, Heidari, Mohammad Hassan, and Tonekaboni, Seyed Hassan

Subjects

*CERVICAL intraepithelial neoplasia, *HUMAN chromosome abnormalities

Abstract

Background and Aim: Ring chromosomes are rare cytogenetic abnormalities that occur in less than 10% of hematopoietic malignancies. They are rare in blood disorder. The present review has focused on the ring chromosome associated with oncology malignancies. Materials and Methods: By reviewing the web-based search for all English scientific peer review articles published, was initiated using Medline/PubMed, Mitelman database (http://cgap.nci.nih.gov/Chromosomes/Mitelman), and other pertinent references on websites about ring chromosomes in Oncology. The software program as End Note was used to handle the proper references for instruction to author. Karyotype descriptions were cited according to ISCN. Conclusion: Ring chromosomes are rare chromosomal aberrations, almost many times are of de novo origin, presenting a different phenotype regarding the loss of genetic material. The karyotype represents the main analysis for detection of ring chromosomes, but other molecular technics are necessary for complete characterization. The information of this review article adds to the spectrum of both morphology and genetic rearrangements in the field of oncology malignancies. [ABSTRACT FROM AUTHOR]

Published

2016

50. Expanding the ocular phenotype of 14q terminal deletions: A novel presentation of microphthalmia and coloboma in ring 14 syndrome with associated 14q32.31 deletion and review of the literature.

Author

Salter, Claire G., Baralle, Diana, Collinson, Morag N., and Self, James E.

Abstract

A variety of ocular anomalies have been described in the rare ring 14 and 14q terminal deletion syndromes, yet the character, prevalence, and extent of these anomalies are not well defined. Identification of these ocular anomalies can be central to providing diagnoses and facilitating optimal individual patient management. We report a child with a 14q32.31 terminal deletion and ring chromosome formation, presenting with severe visual impairment secondary to significant bilateral coloboma and microphthalmia. This patient is compared to previously reported patients with similar ocular findings and deletion sizes to further refine a locus for coloboma in the 14q terminal region. Those with ring formation and linear deletions are compared and the possibility of ring formation affecting the proximal 14q region is discussed. This report highlights the severity of ocular anomalies that can be associated with ring 14 and 14q terminal deletion syndromes and reveals the limited documentation of ocular examination in these two related syndromes. This suggests that many children with these genetic changes do not undergo an ophthalmology examination as part of their clinical assessment, yet it is only when this evaluation becomes routine that the true prevalence and extent of ocular involvement can be defined. This report therefore advocates for a thorough ophthalmological exam in children with ring 14 or 14q terminal deletion syndrome. © 2016 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2016