Your search keyword '"I N, Lebedev"' showing total 88 results

1. Aberrant methylation of placental development genes in chorionic villi of spontaneous abortions with trisomy 16

Author

О. Yu. Vasilyeva, E. N. Tolmacheva, A. E. Dmitriev, Ya. A. Darkova, E. A. Sazhenova, T. V. Nikitina, I. N. Lebedev, and S. A. Vasilyev

Subjects

aneuploidy, trisomy 16, dna methylation, chorionic villi, miscarriage, bisulfite sequencing, spontaneous abortions, Genetics, QH426-470

Abstract

In humans, aneuploidy is incompatible with the birth of healthy children and mainly leads to the death of embryos in the early stages of development in the first trimester of pregnancy. Trisomy 16 is the most common aneup loidy among spontaneous abortions of the first trimester of pregnancy. However, the mechanisms leading to the death of embryos with trisomy 16 remain insufficiently investigated. One of these potential mechanisms is abnormal placental development, including aberrant remodeling of spiral arteries. Spiral artery remodeling involves the migration of trophoblast cells into the maternal spiral arteries, replacing their endothelium and remodeling to ensure a stable embryonic nutrition and oxygen supply. This is a complex process which depends on many factors from both the embryo and the mother. We analyzed the methylation level of seven genes (ADORA2B, NPR3, PRDM1, PSG2, PHTLH, SV2C, and TICAM2) involved in placental development in the chorionic villi of spontaneous abortions with trisomy 16 (n = 14), compared with spontaneous abortions with a normal karyotype (n = 31) and the control group of induced abortions (n = 10). To obtain sequencing libraries, targeted amplification of individual gene regions using designed oligonucleot ide primers for bisulfite-converted DNA was used. The analysis was carried out using targeted bisulfite massive parallel sequencing. In the group of spontaneous abortions with trisomy 16, the level of methylation of the PRDM1 and PSG2 genes was significantly increased compared to induced abortions (p = 0.0004 and p = 0.0015, respectively). In the group of spontaneous abortions, there was no increase in the level of methylation of the PRDM1 and PSG2 genes, but the level of methylation of the ADORA2B gene was significantly increased compared to the induced abortions (p = 0.032). The results obtained indicate the potential mechanisms of the pathogenetic effect of trisomy 16 on the placental development with the participation of the studied genes.

Published

2024

2. A case report of Pallister-Killian syndrome with an unusual mosaic supernumerary marker chromosome 12 with interstitial 12p13.1-p12.1 duplication

Author

T. V. Karamysheva, I. N. Lebedev, L. I. Minaycheva, L. P. Nazarenko, A. A. Kashevarova, D. A. Fedotov, N. A. Skryabin, M. E. Lopatkina, A. D. Cheremnykh, E. A. Fonova, T. V. Nikitina, E. A. Sazhenova, M. M. Skleimova, N. A. Kolesnikov, G. V. Drozdov, Y. S. Yakovleva, G. N. Seitova, K. E. Orishchenko, and N. B. Rubtsov

Subjects

Pallister-Killian syndrome (PKS), mosaic trisomy 12p, a supernumerary marker of chromosome 12, the chromosomal region 12pter-12q11, chromosomal abnormalities, duplication 12p13.33-p11.1, Genetics, QH426-470

Abstract

Pallister-Killian syndrome (PKS) is a rare inherited disease with multiple congenital anomalies, profound intellectual disability, and the presence in the karyotype of sSMC - i(12)(p10). The frequency of PKS may be underestimated due to problems with cytogenetic diagnosis caused by tissue-specific mosaicism and usually a low percentage of peripheral blood cells containing sSMC. Such tissue-specific mosaicism also complicates a detailed analysis of the sSMC, which, along with the assessment of mosaicism in different tissues, is an important part of cytogenetic diagnosis in PKS. Unfortunately, a full-fledged diagnosis in PKS is either practically impossible or complicated. On the one hand, this is due to problems with the biopsy of various tissues (skin biopsy with fibroblast culture is most often used in practice); on the other - a low percentage of dividing peripheral blood cells containing sSMC, which often significantly complicates the analysis of its composition and organization. In the present study, a detailed analysis of sSMC was carried out in a patient with a characteristic clinical picture of PKS. A relatively high percentage of peripheral blood cells with sSMC (50%) made it possible to perform a detailed molecular cytogenetic analysis of de novo sSMC using chromosomal in situ suppression hybridization (CISS-hybridization), multicolor FISH (mFISH), multicolor chromosome banding (MCB), array CGH (aCGH), and quantitative real-time PCR (qPCR), and short tandem repeat (STR) - analysis. As a result, it was found that the sSMC is not a typical PKS derivative of chromosome 12. In contrast to the classical i(12)(p10) for PKS, the patient’s cells contained an acrocentric chromosome consisting of 12p material. Clusters of telomeric repeats were found at the both ends of the sSMC. Furthemore, the results of aCGH and qPCR indicate the presence of interstitial 8.9 Mb duplication at 12p13.1-p12.1 within the sSMC, which leads to different representations of DNA from different segments of 12p within cells containing sSMC. The obtained data raise the question of the instability of the sSMC and, as a consequence, the possible presence of additional rearrangements, which, in traditional cytogenetic analysis of patients with PKS, are usually described as i(12)(p10).

Published

2024

3. Comparative cytogenetics of anembryonic pregnancies and missed abortions in human

Author

T. V. Nikitina, E. A. Sazhenova, E. N. Tolmacheva, N. N. Sukhanova, S. A. Vasilyev, and I. N. Lebedev

Subjects

anembryonic pregnancy, missed abortion, miscarriage, karyotype, chromosomal abnormalities, sex chromosomes, triploidy, tetraploidy, Genetics, QH426-470

Abstract

Miscarriage is an important problem in human reproduction, affecting 10–15 % of clinically recognized pregnancies. The cases of embryonic death can be divided into missed abortion (MA), for which the ultrasound sign of the embryo death is the absence of cardiac activity, and anembryonic pregnancy (AP) without an embryo in the gestational sac. The aim of this study was to compare the frequency of chromosomal abnormalities in extraembryonic tissues detected by conventional cytogenetic analysis of spontaneous abortions depending on the presence or absence of an embryo. This is a retrospective study of 1551 spontaneous abortions analyzed using GTG-banding from 1990 to 2022 (266 cases of AP and 1285 cases of MA). A comparative analysis of the frequency of chromosomal abnormalities and the distribution of karyotype frequencies depending on the presence of an embryo in the gestational sac was carried out. Statistical analysis was performed using a chi-square test with a p < 0.05 significance level. The total frequency of chromosomal abnormalities in the study was 53.6 % (832/1551). The proportion of abnormal karyotypes in the AP and MA groups did not differ significantly and amounted to 57.1 % (152/266) and 52.9 % (680/1285) for AP and MA, respectively (p = 0.209). Sex chromosome aneuploidies and triploidies were significantly less common in the AP group than in the MA group (2.3 % (6/266) vs 6.8 % (88/1285), p = 0.005 and 4.9 % (13/266) vs 8.9 % (114/1285), p = 0.031, respectively). Tetraploidies were registered more frequently in AP compared to MA (12.4 % (33/266) vs. 8.2 % (106/1285), p = 0.031). The sex ratio among abortions with a normal karyotype was 0.54 and 0.74 for AP and MA, respectively. Thus, although the frequencies of some types of chromosomal pathology differ between AP and MA, the total frequency of chromosomal abnormalities in AP is not increased compared to MA, which indicates the need to search for the causes of AP at other levels of the genome organization, including microstructural chromosomal rearrangements, monogenic mutations, imprinting disorders, and epigenetic abnormalities.

Published

2023

4. Expression of the NUP153 and YWHAB genes from their canonical promoters and alternative promoters of the LINE-1 retrotransposon in the placenta of the first trimester of pregnancy

Author

V. V. Demeneva, E. N. Tolmacheva, T. V. Nikitina, E. A. Sazhenova, S. Yu. Yuriev, A. Sh. Makhmutkhodzhaev, A. S. Zuev, S. A. Filatova, A. E. Dmitriev, Ya. A. Darkova, L. P. Nazarenko, I. N. Lebedev, and S. A. Vasilyev

Subjects

miscarriage, placenta, retrotransposon line-1, dna methylation, nup153, ywhab, Genetics, QH426-470

Abstract

The placenta has a unique hypomethylated genome. Due to this feature of the placenta, there is a potential possibility of using regulatory elements derived from retroviruses and retrotransposons, which are suppressed by DNA methylation in the adult body. In addition, there is an abnormal increase in the level of methylation of the LINE-1 retrotransposon in the chorionic trophoblast in spontaneous abortions with both normal karyotype and aneuploidy on different chromosomes, which may be associated with impaired gene transcription using LINE-1 regulatory elements. To date, 988 genes that can be expressed from alternative LINE-1 promoters have been identified. Using the STRING tool, genes (NUP153 and YWHAB) were selected, the products of which have significant functional relationships with proteins highly expressed in the placenta and involved in trophoblast differentiation. This study aimed to analyze the expression of the NUP153 and YWHAB genes, highly active in the placenta, from canonical and alternative LINE-1 promoters in the germinal part of the placenta of spontaneous and induced abortions. Gene expression analysis was performed using real-time PCR in chorionic villi and extraembryonic mesoderm of induced abortions (n = 10), adult lymphocytes (n = 10), spontaneous abortions with normal karyotype (n = 10), and with the most frequent aneuploidies in the first trimester of pregnancy (trisomy 16 (n = 8) and monosomy X (n = 6)). The LINE-1 methylation index was assessed in the chorionic villi of spontaneous abortions using targeted bisulfite massive parallel sequencing. The level of expression of both genes from canonical promoters was higher in blood lymphocytes than in placental tissues (p < 0.05). However, the expression level of the NUP153 gene from the alternative LINE-1 promoter was 17 times higher in chorionic villi and 23 times higher in extraembryonic mesoderm than in lymphocytes (p < 0.05). The expression level of NUP153 and YWHAB from canonical promoters was higher in the group of spontaneous abortions with monosomy X compared to all other groups (p < 0.05). The LINE-1 methylation index negatively correlated with the level of gene expression from both canonical (NUP153 – R = –0.59, YWHAB – R = –0.52, p < 0.05) and alternative LINE-1 promoters (NUP153 – R = –0.46, YWHAB – R = –0.66, p < 0.05). Thus, the observed increase in the LINE-1 methylation index in the placenta of spontaneous abortions is associated with the level of expression of the NUP153 and YWHAB genes not only from alternative but also from canonical promoters, which can subsequently lead to negative consequences for normal embryogenesis.

Published

2023

5. Influence of human peripheral blood samples preprocessing on the quality of Hi-C libraries

Author

M. M. Gridina, E. Vesna, M. E. Minzhenkova, N. V. Shilova, O. P. Ryzhkova, L. P. Nazarenko, E. O. Belyaeva, I. N. Lebedev, and V. S. Fishman

Subjects

hi-c, human peripheral blood, blood samples storage, Genetics, QH426-470

Abstract

The genome-wide variant of the chromatin conformation capture technique (Hi-C) is a powerful tool for revealing patterns of genome spatial organization, as well as for understanding the effects of their disturbance on disease development. In addition, Hi-C can be used to detect chromosomal rearrangements, including balanced translocations and inversions. The use of the Hi-C method for the detection of chromosomal rearrangements is becoming more widespread. Modern high-throughput methods of genome analysis can effectively reveal point mutations and unbalanced chromosomal rearrangements. However, their sensitivity for determining translocations and inversions remains rather low. The storage of whole blood samples can affect the amount and integrity of genomic DNA, and it can distort the results of subsequent analyses if the storage was not under proper conditions. The Hi-C method is extremely demanding on the input material. The necessary condition for successfully applying Hi-C and obtaining high-quality data is the preservation of the spatial chromatin organization within the nucleus. The purpose of this study was to determine the optimal storage conditions of blood samples for subsequent Hi-C analysis. We selected 10 different conditions for blood storage and sample processing. For each condition, we prepared and sequenced Hi-C libraries. The quality of the obtained data was compared. As a result of the work, we formulated the requirements for the storage and processing of samples to obtain high-quality Hi-C data. We have established the minimum volume of blood sufficient for conducting Hi-C analysis. In addition, we have identified the most suitable methods for isolation of peripheral blood mononuclear cells and their long-term storage. The main requirement we have formulated is not to freeze whole blood.

Published

2023

6. Diagnostic yield of chromosomal microarray and trio whole exome sequencing in congenital brain anomalies

Author

E. A. Fonova, A. A. Kashevarova, M. E. Lopatkina, A. A. Sivtsev, A. A. Zarubin, V. V. Demeneva, G. N. Seitova, L. I. Minaycheva, O. A. Salyukova, S. V. Fadyushina, V. V. Petrova, E. O. Belyaeva, L. P. Nazarenko, and I. N. Lebedev

Subjects

Psychiatry, RC435-571

Abstract

Introduction The deductive method: from karyotyping to aCGH and WES is an important aspect in the diagnosis and search for the causes of intellectual disability due to congenital brain anomalies. There is recommendation to exclude the presence of CNV or monogenic variants for patients with a normal karyotype, but with a clinical picture of syndromic disease. Objectives Improvement of diagnosis of intellectual disability. Methods aCGH with 60K Agilent microarrays, WES with SureSelect Human All Exon V8 Results Pathogenic or potentially pathogenic CNVs were excluded previously by aCGH for 10 families (total 32 people, 2 families had 2 children) with intellectual disability and congenital brain anomalies (for example, polymicrogyria, pachygyria, lissencephaly). The WES identified candidate variants for all families that can lead to impaired neurodevelopment, including 3 pathogenic variants in 3 families, 3 likely pathogenic in three other families, and 10 variants with uncertain clinical significance for 4 families. Almost all of these variants were identified de novo, except for one family, where the proband has been a compound heterozygous for two variants in the RELN gene. The first case of pathogenic mutation de novo was detected in a girl with agenesis of the corpus callosum. It was a missense mutation DYNC1H1 (NM_001376.5): c.4868G>A (p.Arg1623Gln), which leads to impaired intellectual development in autosomal dominant type 13 (OMIM 614563). The second variant was detected in a boy with corpus callosum agenesis, pontine hypogenesis, pachygyria in the frontal lobes. It was a missense variant MACF1 (ENST00000567887.5): c.21989A>G(p.Asp7330Gly), which leads to lissencephaly 9 with complex brainstem malformation (OMIM 614563). The third variant was found in a girl with epilepsy and impaired myelination of the white matter of the parietal-occipital areas of the cerebral hemispheres. It was a missense variant CDKL5 (NM_001323289.2):c.404-1G>A that leads to developmental and epileptic encephalopathy 2 (OMIM 300672). Conclusions Sixteen candidate variants potentially responsible for mental health were reported in this study. Most of these variants were missense changes in genes. All except one anomalies arisen de novo. Trio-based WES has been shown to be an important step in making a genetic diagnosis if other chromosomal and subchromosomal abnormalities had been excluded. The clinical description of the patient is the most important step for the correct interpretation of WES results, which allows to establish the exact genetic cause of the disease if several variants with unclear clinical significance were previously identified. This study was supported by the Russian Science Foundation, grant 21-65-00017, https://rscf.ru/project/21-65-00017/ Disclosure of Interest None Declared

Published

2023

7. Combined whole exome sequencing and chromosomal microarray analysis improve clinical interpretation of genomic variants in patients with intellectual disability

Author

A. A. Kashevarova, E. O. Belyaeva, E. A. Fonova, M. E. Lopatkina, O. Y. Vasilyeva, D. A. Fedotov, A. A. Zarubin, A. A. Sivtsev, V. V. Demeneva, O. A. Salyukova, V. V. Petrova, S. V. Fadiushina, L. I. Minaycheva, G. N. Seitova, L. P. Nazarenko, and I. N. Lebedev

Subjects

Psychiatry, RC435-571

Abstract

Introduction aCGH determines pathogenic copy number variations (CNVs) in about 10% of patients with intellectual disability (ID). In another 20% of patients, probably pathogenic CNVs or variants with uncertain clinical significance are detected. It may be variants that do not fully explain the patient’s symptoms, aberrations with reduced penetrance or inherited from healthy parents. The use of a sequencing method for such cases is advisable. Objectives Improvement of diagnosis of intellectual disability. Methods aCGH with 60K Agilent microarrays, qPCR, targeted sequencing, whole exome sequencing (WES). Results Six patients with ID and inherited deletions/duplications detected by aCGH and their parents if available were further examined by sequencing. Four patients had maternal CNVs: (1) del1q41 (SPATA17, LINC00210, RRP15), (2) del7q35 (TCAF2, exon 8), (3) dup8p22p21.3 (PSD3, exons 1-11), and (4) del12p11.1 (SYT10, exons 1-2). Two patients had paternal CNVs: (5) dup1q44 (SMYD3, exons 2-5) and (6) del15q11.2 (TUBGCP5, CYFIP1, NIPA1, NIPA2, LOC283683). The severe phenotype of patient (5) with dup1q44 could not be explained by the paternally inherited disruption of the single SMYD3 gene. WES determined probably pathogenic SNV in the MID1 gene associated with Opitz GBBB syndrome (OMIM 300000), which corresponds better to the patient’s phenotype and is likely to be the cause of the disease. Although del1q41 is included in the region of chromosome 1q41-q42 deletion syndrome (OMIM 612530) the phenotype of the patient (1) is much milder; WES in the patient detected two pathogenic (MPO, MAN2C1) and one probably pathogenic (ARID1B) SNVs. In patient (6) with del15q11.2 pat WES detected additional pathogenic SNV in exon 7 of the ARSE gene. In patient (3) with dup8p22p21.3 WES determined two SNVs with uncertain significance in the KIDINS220, FOXG1 genes. No SNVs were detected by WES in patient (2) with del7q35. For patient (4) with del12p11.1 targeted SYT10 sequencing revealed no pathogenic SNVs as well. Conclusions Sometimes aCGH-analysis is sufficient to identify the causes of ID, however, in the case of detection of CNVs with uncertain clinical significance and/or inherited from healthy parents, it may be necessary to further examine the patient using sequencing methods. So, the accurate diagnosis was made by WES for one patient of eight. For another two patients the combination of CNVs and SNPs should be considered. For the last three patients the described aberrations could not explain the phenotype and whole genome sequencing may be the solution.This study was supported by the Russian Science Foundation, grant 21-65-00017, https://rscf.ru/project/21-65-00017/ Disclosure of Interest None Declared

Published

2023

8. On the 40th anniversary of the Research Institute of Medical Genetics, Tomsk National Research Medical Center

Author

V. A. Stepanov and I. N. Lebedev

Subjects

Genetics, QH426-470

Published

2023

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

Author

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

Subjects

Medicine, Science

Abstract

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

10. Runs of homozygosity in spontaneous abortions from families with recurrent pregnancy loss

Author

N. A. Skryabin, S. A. Vasilyev, T. V. Nikitina, D. I. Zhigalina, R. R. Savchenko, N. P. Babushkina, M. E. Lopatkina, A. A. Kashevarova, and I. N. Lebedev

Subjects

recurrent pregnancy loss, array-based comparative genomic hybridization, runs of homozygosity, spontaneous abortions, genomic imprinting, Genetics, QH426-470

Abstract

Recurrent pregnancy loss (RPL) is a severe reproductive pathology with a significant component of unexplained etiology. Extended homozygous regions as a possible etiological factor for RPL were sought in the genomes of embryos. Twenty-two paired first-trimester spontaneously aborted embryos from eleven women with recurrent miscarriage were analyzed. All embryos had normal karyotypes according to metaphase karyotyping and conventional comparative genomic hybridization. SurePrint G3 Human CGH + SNP 4 × 180K microarrays (Agilent Technologies) were used to search for homozygous regions. As a result, 39 runs of homozygosity (ROH) were identified in extraembryonic tissues of 15 abortuses. Verification of recurrent homozygous regions was performed by Sanger sequencing. The presence of occasional heterozygous SNPs was shown in 25 extended ROHs, which may indicate that they did not arise de novo but were inherited from parents. In the course of inheritance in a series of generations, they may accumulate mutations, leading to heterozygosity for several sites in the initially homozygous population-specific regions. Homozygotization of recessive mutations is one of the putative mechanisms of the influence of such inherited ROHs on RPL development. The high frequency of extended ROHs detected in the present study may point to a role of inbreeding in RPL etiology. Homozygous regions may also occur due to uniparental disomy, and abnormalities of genomic imprinting may be another mechanism responsible for the pathological manifestation of ROHs in embryogenesis. Indeed, five predicted imprinted genes were identified within ROHs according to the Geneimprint database: OBSCN, HIST3H2BB, LMX1B, CELF4, and FAM59A. This work reports the first finding of a high frequency of extended ROHs in spontaneously aborted embryos with normal karyotypes from families with RPL.

Published

2019

11. Variation of DNA copies number in etiology of congenital heart defects

Author

A. A. Slepukhina, I. N. Lebedev, and G. I. Lifshitz

Subjects

dna copy number variation, cnv, congenital heart defects, inborn heart defects, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Past decade, there is a remarkable evidence of that the variation of DNA copies number (copy number variation, CNV) is related with onset of inborn heart defects (IHD). The review is focused on an impact of CNV in IHD development. Attention is paid on widely known variations, as the microdeletions of 22q 11 chromosome region, as the novel unique variations that were discovered recent years. We assume that common regard on causation of CNV includes a description of their part and characteristics of the pathology caused. Special place does take the analysis of candidate genes in IHD etiology and mechanisms of their pathological influence under the circumstances of gene doses change. A discussion provided on which genetic characteristics of CNV are more informing in assessment of probable pathogenicity of microstructural chromosomes recomposition.

Published

2018

12. Pleiotropy of Copy Number Variation in Human Genome

Author

A. A. Kashevarova, G. V. Drozdov, D. A. Fedotov, and I. N. Lebedev

Subjects

Genetics

Published

2022

13. Interloci CNV Interactions in Variability of the Phenotypes of Neurodevelopmental Disorders

Author

E. O. Belyaeva and I. N. Lebedev

Subjects

Genetics

Published

2022

14. Diferentefects of pulsed X-rays in MOLT-4 cel line and human peripheral blod lymphocytes

Author

S. A. Vasilyev, A. A. Belenko, O. P. Kutenkov, M. A. Bolshakov, I. N. Lebedev, and V. V. Rostov

Subjects

pulsed x-rays, low doses, hyperradiosensitivity, γh2ax and 53bp1 foci, dna double-strand breaks, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Effects of ionizing radiation registered in cells after low dose irradiation are still poorly understood. Thus, the aim of this study was to analyze effects of pulsed X-rays on level of radiation-induced DNA double-strand breaks and their repair kinetics in cancer and normalhuman cells in vitro. Analysis of radiation-induced γH2AX and 53BP1 repair foci in MOLT-4 cells with lymphoblastic origin was used for assessment of DNA double-strand breaks (DSB) in these cells. Number of residual radiation-induced γH2AX and 53BP1 foci at 18 hafter irradiation depended on frequency of X-ray pulses: at 8 pulses per second effect was highest in MOLT-4 cells and lowest in peripheral blood lymphocytes. It suggests that pulsed X-rays with various frequencies could be used for target influence on cancer cells being lessdeleterious for normal human cells.

Published

2016

15. Methods of DNa methylation analysis:possibilities and limitations of their application in oncology

Author

N. A. Skryabin, A. A. Kashevarova, E. V. Denisov, and I. N. Lebedev

Subjects

dna methylation, bisulphite modification, methylation-sensitive restriction enzymes, methylated dna immunoprecipitation, microarrays, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abnormalities of DNA methylation play a significant role in initiation and progression of tumors. In this regard it is necessary to study these aberrations in order to better understand the malignant transformation pathogenesis. For this purpose the adequate and objective methods are required. The principles and possibilities of application of basic methods of DNA methylation analysis are reviewed in the paper

Published

2016

16. <scp>BiasCorrector</scp> : Fast and accurate correction of all types of experimental biases in quantitative <scp>DNA</scp> methylation data derived by different technologies

Author

Arndt Hartmann, Evgeny A. Moskalev, Lorenz A. Kapsner, Sebastian Mate, Mikhail G. Zavgorodnij, Hans-Ulrich Prokosch, Agnes Hotz-Wagenblatt, Florian Haller, Jörg D. Hoheisel, Svetlana P. Majorova, Andrea S. Bauer, Oleg V. Kolychev, and I. N. Lebedev

Subjects

Technology, Cancer Research, Computer science, Calibration (statistics), Polymerase Chain Reaction, 03 medical and health sciences, 0302 clinical medicine, Software, Bias, Neoplasms, Humans, business.industry, Oligonucleotide, Pcr bias, Pattern recognition, Sequence Analysis, DNA, DNA Methylation, Regression, Oncology, 030220 oncology & carcinogenesis, DNA methylation, Pyrosequencing, CpG Islands, Artificial intelligence, business, Algorithms

Abstract

Quantification of DNA methylation in neoplastic cells is crucial both from mechanistic and diagnostic perspectives. However, such measurements are prone to different experimental biases. Polymerase chain reaction (PCR) bias results in an unequal recovery of methylated and unmethylated alleles at the sample preparation step. Post-PCR biases get introduced additionally by the readout processes. Correcting the biases is more practicable than optimising experimental conditions, as demonstrated previously. However, utilisation of our earlier developed algorithm strongly necessitates automation. Here, we present two R packages: rBiasCorrection, the core algorithms to correct biases; and BiasCorrector, its web-based graphical user interface frontend. The software detects and analyses experimental biases in calibration DNA samples at a single base resolution by using cubic polynomial and hyperbolic regression. The correction coefficients from the best regression type are employed to compensate for the bias. Three common technologies-bisulphite pyrosequencing, next-generation sequencing and oligonucleotide microarrays-were used to comprehensively test BiasCorrector. We demonstrate the accuracy of BiasCorrector's performance and reveal technology-specific PCR- and post-PCR biases. BiasCorrector effectively eliminates biases regardless of their nature, locus, the number of interrogated methylation sites and the detection method, thus representing a user-friendly tool for producing accurate epigenetic results.

Published

2021

17. A cookbook for DNase Hi-C

Author

Maria E. Lopatkina, Maria I. Yablonskaya, Emil Valeev, Nadezhda V. Shilova, Veniamin S. Fishman, M.M. Gridina, Zhanna G. Markova, I. N. Lebedev, Viktoria Yu Voinova, Ludmila P. Nazarenko, and Evgeniy A. Mozheiko

Subjects

lcsh:QH426-470, Human peripheral blood, Computational biology, Biology, Genome organization, Chromosomes, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Adapter (genetics), A549, DNAse I, Hi-C, Genetics, Deoxyribonuclease I, Humans, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, DNA ligase, Deoxyribonucleases, Genome, Oligonucleotide, LNCaP, Rational design, Methodology, Chromatin, Restriction enzyme, lcsh:Genetics, chemistry, Biotinylation, K562, 030217 neurology & neurosurgery, DNA

Abstract

Background The Hi-C technique is widely employed to study the 3-dimensional chromatin architecture and to assemble genomes. The conventional in situ Hi-C protocol employs restriction enzymes to digest chromatin, which results in nonuniform genomic coverage. Using sequence-agnostic restriction enzymes, such as DNAse I, could help to overcome this limitation. Results In this study, we compare different DNAse Hi-C protocols and identify the critical steps that significantly affect the efficiency of the protocol. In particular, we show that the SDS quenching strategy strongly affects subsequent chromatin digestion. The presence of biotinylated oligonucleotide adapters may lead to ligase reaction by-products, which can be avoided by rational design of the adapter sequences. Moreover, the use of nucleotide-exchange enzymes for biotin fill-in enables simultaneous labelling and repair of DNA ends, similar to the conventional Hi-C protocol. These improvements simplify the protocol, making it less expensive and time-consuming. Conclusions We propose a new robust protocol for the preparation of DNAse Hi-C libraries from cultured human cells and blood samples supplemented with experimental controls and computational tools for the evaluation of library quality.

Published

2021

18. 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

19. Differential DNA Methylation of the IMMP2L Gene in Families with Maternally Inherited 7q31.1 Microdeletions is Associated with Intellectual Disability and Developmental Delay

Author

Oksana Yu Vasilyeva, Arkadiy B Maslennikov, Olga L Shestovskikh, S. A. Vasilyev, N.A. Skryabin, Robert Vulić, Lyudmila P. Nazarenko, Asia R Shorina, Maria E. Lopatkina, E. N. Tolmacheva, A. A. Kashevarova, Miroslava O Filippova, Tatyana A Gayner, Alexei A. Zarubin, R. R. Savchenko, Elena O. Belyaeva, Veniamin S. Fishman, I. N. Lebedev, and Vida Čulić

Subjects

Genetics, CpG site, DNA methylation, Bisulfite sequencing, Human genome, Copy-number variation, Epigenetics, Biology, Haploinsufficiency, Molecular Biology, Penetrance, Genetics (clinical)

Abstract

Most copy number variations (CNVs) in the human genome display incomplete penetrance with unknown underlying mechanisms. One such mechanism may be epigenetic modification, particularly DNA methylation. The IMMP2L gene is located in a critical region for autism susceptibility on chromosome 7q (AUTS1). The level of DNA methylation was assessed by bisulfite sequencing of 87 CpG sites in the IMMP2L gene in 3 families with maternally inherited 7q31.1 microdeletions affecting the IMMP2L gene alone. Bisulfite sequencing revealed comparable levels of DNA methylation in the probands, healthy siblings without microdeletions, and their fathers. In contrast, a reduced DNA methylation index and increased IMMP2L expression were observed in lymphocytes from the healthy mothers compared with the probands. A number of genes were upregulated in the healthy mothers compared to controls and downregulated in probands compared to mothers. These genes were enriched in components of the ribosome and electron transport chain, as well as oxidative phosphorylation and various degenerative conditions. Differential expression in probands and mothers with IMMP2L deletions relative to controls may be due to compensatory processes in healthy mothers with IMMP2L deletions and disturbances of these processes in probands with intellectual disability. The results suggest a possible partial compensation for IMMP2L gene haploinsufficiency in healthy mothers with the 7q31.1 microdeletion by reducing the DNA methylation level. Differential DNA methylation of intragenic CpG sites may affect the phenotypic manifestation of CNVs and explain the incomplete penetrance of chromosomal microdeletions.

Published

2021

20. DNA methylation status of the cell proliferation genes in atherosclerosis

Author

M. S. Nazarenko, A. V. Markov, I. N. Lebedev, A. A. Sleptsov, A. V. Frolov, O. L. Barbarash, L. S. Barbarash, and V. P. Puzyrev

Subjects

dna methylation, atherosclerosis, infinium humanmethylation27 beadchip, Diseases of the blood and blood-forming organs, RC633-647.5, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

The purpose of this study was to identify the features of methylation status of genes whose products are involved in the cell proliferation in vascular tissues of patients with atherosclerosis. We tested the vascular samples from carotid arteries, internal mammary arteries and saphenous veins, which differ in their morphological and functional characteristics and the degree of susceptibility to pathology. DNA methylation profiling was performed by using the microarray «Infinium Human-Methylation27 BeadChip» («Illumina», USA), methylation-sensitive polymerase chain reaction and methylation-specific PCR. For the first time we identified 45 CpG-sites of 36 genes with differential DNA methylation between vascular tissues. The most pronounced differences in the DNA methylation level were registered for CpG-dinucleotides of genes ALOX12, CARD11, DAB2IP, PTPRC, RA-SIP1, THRB, TLR4, TNFRSF9 and WNT16. Our data do not support the hypothesis of epigenetic dysregulation of cell-cycle genes (CDKN2A (p16INK4a and p14ARF), CDKN2B (p15INK4b)) in atherosclerosis.

Published

2013

21. FISH Diagnostics of Chromosomal Translocation with the Technology of Synthesis of Locus-Specific DNA Probes Based on Long-Range PCR

Author

V. M. Sivokha, M.E. Lopatkina, S. A. Vasiliev, I. N. Lebedev, O. Y. Vasilieva, N.A. Skryabin, Elena O. Belyaeva, R. R. Savchenko, Lyudmila P. Nazarenko, and D. I. Zhigalina

Subjects

0106 biological sciences, Genetics, 0303 health sciences, G banding, Hybridization probe, Chromosomal translocation, Locus (genetics), Karyotype, Biology, 01 natural sciences, Chromosome aberration, 03 medical and health sciences, Chromosome regions, 030304 developmental biology, 010606 plant biology & botany, Comparative genomic hybridization

Abstract

Detection of translocations in subtelomeric regions of chromosomes is a serious diagnostic problem, because they are difficult to determine by conventional cytogenetics with G banding. The aim of this work was the development of the technology of DNA probe synthesis for unique sequences of subtelomeric chromosome regions based on long-range PCR using the clinical case of determining the parental origin of unbalanced translocation between chromosomes 5 and 8. The unbalanced translocation der(5)t(5;8)(р15.33;q24.22) in a proband with physical, motor, intellectual, and speech development delay and in his sibling with speech and intellectual development delay as well, which was previously identified by array comparative genomic hybridization (aCGH), was confirmed by FISH. A balanced translocation 46,XX,t(5;8)(p15.33;q24.22) was detected in the mother’s karyotype using the created locus-specific DNA probe. This chromosome aberration was not detected by G banding of metaphase chromosomes. The father’s karyotype was normal according to FISH results. The method presented here makes it possible to create locus-specific DNA probes in a molecular cytogenetic laboratory using long-range PCR for the rapid diagnosis of cryptic chromosomal rearrangements.

Published

2020

22. Prenatal Diagnosis of Small Supernumerary Marker Chromosome 10 by Array-Based Comparative Genomic Hybridization and Microdissected Chromosome Sequencing

Author

Tatyana V. Karamysheva, Aleksander D. Cheremnykh, Gleb V. Drozdov, Alexey I. Makunin, Eugeny A. Elisaphenko, S. A. Vasilyev, Gulnara N. Seitova, Maria E. Lopatkina, Nikolay B. Rubtsov, Nazarenko Lp, Natalia B. Torkhova, Daria I. Zhigalina, A. A. Kashevarova, and I. N. Lebedev

Subjects

Genetics, prenatal diagnosis, medicine.diagnostic_test, QH301-705.5, Hybridization probe, small supernumerary marker chromosome, Ring chromosome, ring chromosome, Medicine (miscellaneous), Chromosome, Prenatal diagnosis, Biology, array-based comparative genomic hybridization, single-copy chromosome sequencing, General Biochemistry, Genetics and Molecular Biology, Article, mosaicism, medicine, Biology (General), Small supernumerary marker chromosome, Microdissection, chromosomal microdissection, Comparative genomic hybridization, Fluorescence in situ hybridization

Abstract

Interpreting the clinical significance of small supernumerary marker chromosomes (sSMCs) in prenatal diagnosis is still an urgent problem in genetic counselling regarding the fate of a pregnancy. We present a case of prenatal diagnosis of mosaic sSMC(10) in a foetus with a normal phenotype. Comprehensive cytogenomic analyses by array-based comparative genomic hybridization (aCGH), sSMC microdissection with next-generation sequencing (NGS) of microdissected library, fluorescence in situ hybridization (FISH) with locus-specific and telomere-specific DNA probes and quantitative real-time PCR revealed that sSMC(10) had a ring structure and was derived from the pericentromeric region of chromosome 10 with involvement of the 10p11.21-p11.1 and 10q11.21-q11.23 at 1.243 Mb and 7.173 Mb in size, respectively. We observed a difference in the length of sSMC(10) between NGS data of the DNA library derived from a single copy of sSMC(10), and aCGH results that may indicate instability and structural mosaicism for ring chromosomes in foetal cells. The presence of a 9 Mb euchromatin region in the analysed sSMC(10) did not lead to clinical manifestations, and a healthy girl was born at term. We suggest that the ring structure of sSMCs could influence sSMC manifestations and should be taken into account in genetic counselling during prenatal diagnosis.

Published

2021

23. P–381 Deciphering the genetic cause of recurrent and sporadic pregnancy loss

Author

Ants Kurg, Han G. Brunner, G Acharya, T. V. Nikitina, Merryn V. E. Macville, Andres Salumets, R Essers, M Zaman. Esteki, S P Deligiannis, E. A. Sazhenova, Elizaveta A. Fonova, Servi J. C. Stevens, Salwan Al-Nasiry, I. N. Lebedev, and E. N. Tolmacheva

Subjects

Pregnancy, Reproductive Medicine, business.industry, Rehabilitation, Obstetrics and Gynecology, Physiology, Medicine, business, medicine.disease

Abstract

Study question To investigate the prevalence and effect of (mosaic) de novo genomic aberrations in recurrent pregnancy loss (RPL) and sporadic abortion (SA). Summary answer Prevalence of maternal uniparental disomies (UPDs) was high in both cohorts. While chromosomal UPDs were found in both cohorts, genome wide UPDs were RPL specific. What is known already Spontaneous abortion occurs in 10–15% of clinically recognized pregnancies and recurrent pregnancy loss in 1–3%. SA and RPL are associated with reduced quality of life. Multiple factors contribute to SA and RPL, such as uterine malformations and parental/fetal chromosomal abnormalities. However, in ∼60% of SA and RPL the cause remains unknown. UPD is defined as the presence of two homologues chromosomes originating from a single parent. This phenomenon can lead to imprinting disorders that are characterised by clinical features affecting growth, development and metabolism in liveborn offspring. However, it could also be responsible for pregnancy loss. Study design, size, duration We recruited 32 families with pregnancy loss (n = 16 RPL cohort, n = 16 SA cohort) with no known genetic predispositions and normal karyotyping results in both parents and the fetus. Average maternal age was 28.68 years (SD = 5.43), paternal age 30.3 years (SD = 5.53), and the gestational age at pregnancy loss was 8.65 weeks (SD = 2.47). The average number of miscarriages in the RPL group was 3.57 (SD = 0.84). We profiled the genomic landscape of both cohorts using SNP typing. Participants/materials, setting, methods We isolated DNA from blood of both parents and the placental tissues from the miscarried products of conception. The placenta tissues were sampled from two distinct extraembryonic and embryonic germ layers, the extraembryonic mesoderm and the chorionic villi cytotrophoblast. Subsequently, we performed SNP-genotyping using Illumina’s Global-Screening Array–24 v2.0 BeadChips and applied haplarithmisis to delineate allelic architecture of fetal tissues of both cohorts. This allowed us to detect large de novo copy-number and -neutral (>10kb) changes. Main results and the role of chance In this pilot study, we have analyzed 132 DNA samples (n = 32 families), of which 16 families were in the RPL cohort and 16 in the SA cohort. Within the RPL cohort, we found: one family with mosaic genome wide hexaploidy both in the extraembryonic mesoderm and chorionic villi, one family with a non-mosaic genome wide hetero UPD of the chorionic villi tissue, one family with a mosaic UPD of chromosome 14 in both tissues and tetraploidy exclusively in the chorionic villi, one family with a mosaic UPD of chromosome 16 in both tissues, one family with a mosaic UPD of chromosome 6 in both tissues, and another family with a mosaic UPD of chromosome 5 in the extraembryonic mesoderm. Within the SA group, one family showed a UPD of chromosome 7 and another family showed a segmental UPD of chromosome 5 in both tissues. Strikingly, all the UPDs found in this study were maternal in origin. Limitations, reasons for caution The main limitation of this study is the resolution of detecting copy-neutral and copy-number variations, which is an inherent limiting factor of SNP-array technology. In addition, in the sample in which we observed non-mosaic genome wide UPD, maternal contamination is likely that can be investigated by other technologies. Wider implications of the findings: Multiple genome wide UPDs are found in the RPL group but none in the SA group, indicating an association between genome wide mosaic UPD and RPL. These findings could lead to a better understanding of causative factors for SA and RPL and the need for a SNP-based non-invasive prenatal testing. Trial registration number Not applicable

Published

2021

24. Ontogenetic Pleiotropy of Genes Involved in CNVs in Human Spontaneous Abortions

Author

I. N. Lebedev, A. A. Kashevarova, D. I. Zhigalina, R. R. Savchenko, M.E. Lopatkina, N.A. Skryabin, T. V. Nikitina, and E. A. Sazhenova

Subjects

0106 biological sciences, Genetics, 0303 health sciences, Microarray analysis techniques, Chromosome, Biology, 01 natural sciences, Phenotype, Human genetics, 03 medical and health sciences, HOXD13, Pleiotropy, embryonic structures, Copy-number variation, Gene, 030304 developmental biology, 010606 plant biology & botany

Abstract

Using chromosome microarray analysis, 52 samples of placental tissues from first trimester human spontaneous abortions were examined. One hundred twenty copy number variations (CNVs) were identified, affecting one or more genes (total of 427 genes). Using enrichment analysis with the mammalian phenotype ontology, all genes were divided into 183 categories (p ≤ 0.05). The embryogenesis category included 22 genes: AIP, BMP4, BMP5, CDKN1C, EXT1, GAB1, H19, HOXD13, IGF2, KIT, LDHA, NKX2-5, NRK, PEG3, PHLDA2, SMCHD1, SMN1, TBX3, TGIF1, TH, TLX2, and TRR. In this paper, the functions of each of the above genes and pathological phenotypes associated with mutations in them are discussed. A hypothesis of the pleiotropic effect of genes involved in CNVs in spontaneous abortions is proposed.

Published

2019

25. Synthesis of Polyol Tetrabromophthalate and Its Use as a Component for Preparing Foamed Polyurethanes of Reduced Flammability

Author

E. A. Lebedeva, T. E. Oshchepkova, S. N. Lysenko, I. N. Lebedev, and S. A. Astaf’eva

Subjects

chemistry.chemical_classification, General Chemical Engineering, 02 engineering and technology, General Chemistry, 010402 general chemistry, 021001 nanoscience & nanotechnology, Combustion, 01 natural sciences, humanities, 0104 chemical sciences, chemistry.chemical_compound, fluids and secretions, Polyol, chemistry, Chemical engineering, Hydroxide, Reduced viscosity, 0210 nano-technology, Melamine, Fire retardant, Polyurethane, Flammability

Abstract

A procedure was suggested for preparing brominated polyols of reduced viscosity for the synthesis of foamed polyurethanes of reduced flammability. The flame-retarding action of the synthesized polyol tetrabromophthalate in polyurethane was studied in comparison with that of other widely used flame retardants. Evaluation of the effect exerted on the flammability of the polurethane compound by the polyol tetrabromophthalate synthesized, melamine, and aluminum hydroxide shows that all the samples containing flame retardants are self-extinguishing. The shortest combustion time was observed for the sample containing 6% polyol tetrabromophthalate synthesized. The sample containing as a flame retardant additive solely the synthesized polyole tetrabromophthalate also exhibits the highest performance as a heat-insulating material from the viewpoint of thermal conductivity.

Published

2019

26. Method of targeted bisulfite massive parallel sequencing of the human LINE-1 retrotransposon promoter

Author

Lada A. Zatula, Anton V. Markov, S. A. Vasilyev, Oksana Yu Vasilyeva, Victoria V. Demeneva, Diana V. Sharysh, I. N. Lebedev, D. I. Zhigalina, and E. N. Tolmacheva

Subjects

DNA methylation, Massive parallel sequencing, NGS-based LINE-1 retrotransposon methylation analysis, Science, Clinical Biochemistry, Bisulfite sequencing, Retrotransposon, Methylation, Computational biology, Method Article, Targeted bisulfite massive parallel sequencing, Biology, Genome, Bisulfite, Medical Laboratory Technology, LINE-1 retrotransposon, Pyrosequencing

Abstract

The methylation index of the LINE-1 promoter is one of the most commonly used markers for assessing the global level of genome methylation in various human cells and tissues. We developed an NGS-based protocol for DNA methylation analysis of the LINE-1 retrotransposon promoter. This approach allows assessment of the DNA methylation index of 19 CpG sites in the LINE-1 promoter that have the highest tissue- or tumor-specific variability. The method provides a DNA methylation profile for analyzing either the methylation index of each CpG site independently or the mean DNA methylation index across the LINE-1 promoter. The results obtained using the developed method corresponded well to the level of methylation assessed using a commercially available kit for DNA pyrosequencing. In addition, our method provides much more information: 1) the DNA methylation profile of a significant part of the LINE-1 promoter and 2) the level of DNA methylation at individual LINE-1 loci in the genome. The method of targeted bisulfite massive parallel sequencing of the human LINE-1 retrotransposon promoter can be used in large-scale studies of the global level of genome methylation in normal human cells or tumors. To accomplish this, we modified the targeted massive parallel sequencing method based on 16S Metagenomic Sequencing Library Preparation protocol (Illumina, USA) by:•Introduction of the stage of bisulfite conversion of DNA.•Development of specific primers for the LINE-1 sequence., Graphical abstract Image, graphical abstract

Published

2021

27. Aneuploidy and DNA Methylation as Mirrored Features of Early Human Embryo Development

Author

S. A. Vasilyev, I. N. Lebedev, and E. N. Tolmacheva

Subjects

0301 basic medicine, Epigenomics, lcsh:QH426-470, epigenetic reprogramming, Aneuploidy, Embryonic Development, Context (language use), Review, Biology, medicine.disease_cause, Genome, Genomic Instability, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, human embryogenesis, aneuploidy, Genetics (clinical), 030219 obstetrics & reproductive medicine, DNA methylation, Genome, Human, Chromosome, Methylation, medicine.disease, Embryo, Mammalian, lcsh:Genetics, 030104 developmental biology, Carcinogenesis, Reprogramming

Abstract

Genome stability is an integral feature of all living organisms. Aneuploidy is the most common cause of fetal death in humans. The timing of bursts in increased aneuploidy frequency coincides with the waves of global epigenetic reprogramming in mammals. During gametogenesis and early embryogenesis, parental genomes undergo two waves of DNA methylation reprogramming. Failure of these processes can critically affect genome stability, including chromosome segregation during cell division. Abnormal methylation due to errors in the reprogramming process can potentially lead to aneuploidy. On the other hand, the presence of an entire additional chromosome, or chromosome loss, can affect the global genome methylation level. The associations of these two phenomena are well studied in the context of carcinogenesis, but here, we consider the relationship of DNA methylation and aneuploidy in early human and mammalian ontogenesis. In this review, we link these two phenomena and highlight the critical ontogenesis periods and genome regions that play a significant role in human reproduction and in the formation of pathological phenotypes in newborns with chromosomal aneuploidy.

Published

2020

28. LINE-1 retrotransposon methylation in chorionic villi of first trimester miscarriages with aneuploidy

Author

D. I. Zhigalina, Vasilissa A Lee, T. V. Nikitina, S. A. Vasilyev, Oksana Yu Vasilyeva, E. A. Sazhenova, I. N. Lebedev, E. N. Tolmacheva, Lada A. Zatula, Ekaterina S Serdyukova, A. A. Kashevarova, and Anton V. Markov

Subjects

0301 basic medicine, Adult, Aneuploidy, Embryonic Development, Biology, Miscarriage, Andrology, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, Genetics, medicine, Humans, Genetics (clinical), 030219 obstetrics & reproductive medicine, метилирование ДНК, анеуплоидия, Obstetrics and Gynecology, Trisomy 16, Karyotype, General Medicine, Methylation, DNA Methylation, medicine.disease, Abortion, Spontaneous, Pregnancy Trimester, First, 030104 developmental biology, medicine.anatomical_structure, Long Interspersed Nucleotide Elements, Reproductive Physiology and Disease, Reproductive Medicine, ретротранспозоны, DNA methylation, Chorionic villi, Female, Chorionic Villi, Trisomy, Developmental Biology

Abstract

Purpose High frequency of aneuploidy in meiosis and cleavage stage coincides with waves of epigenetic genome reprogramming that may indicate a possible association between epigenetic mechanisms and aneuploidy occurrence. This study aimed to assess the methylation level of the long interspersed repeat element 1 (LINE-1) retrotransposon in chorionic villi of first trimester miscarriages with a normal karyotype and aneuploidy. Methods The methylation level was assessed at 19 LINE-1 promoter CpG sites in chorionic villi of 141 miscarriages with trisomy of chromosomes 2, 6, 8-10, 13-15, 16, 18, 20-22, and monosomy X using massive parallel sequencing. Results The LINE-1 methylation level was elevated statistically significant in chorionic villi of miscarriages with both trisomy (45.2 +/- 4.3%) and monosomy X (46.9 +/- 4.2%) compared with that in induced abortions (40.0 +/- 2.4%) (p < 0.00001). The LINE-1 methylation levels were specific for miscarriages with different aneuploidies and significantly increased in miscarriages with trisomies 8, 14, and 18 and monosomy X (p < 0.05). The LINE-1 methylation level increased with gestational age both for group of miscarriages regardless of karyotype (R = 0.21, p = 0.012) and specifically for miscarriages with trisomy 16 (R = 0.48, p = 0.007). LINE-1 methylation decreased with maternal age in miscarriages with a normal karyotype (R = - 0.31, p = 0.029) and with trisomy 21 (R = - 0.64, p = 0.024) and increased with paternal age for miscarriages with trisomy 16 (R = 0.38, p = 0.048) and monosomy X (R = 0.73, p = 0.003). Conclusion Our results indicate that the pathogenic effects of aneuploidy in human embryogenesis can be supplemented with significant epigenetic changes in the repetitive sequences.

Published

2020

29. Generation of two induced pluripotent stem cell lines from peripheral blood mononuclear cells of a patient with Wilson's disease

Author

O.Yu. Vasilyeva, Suren M. Zakian, D. I. Zhigalina, N.A. Skryabin, I. N. Lebedev, N.A. Kolesnikov, A.O. Bueverov, E.V. Grigor'eva, A.A. Sivtcev, A.A. Malakhova, and P.O. Bogomolov

Subjects

0301 basic medicine, Karyotype, Cell Biology, General Medicine, Germ layer, Disease, Biology, medicine.disease, Peripheral blood mononuclear cell, Molecular biology, DNA sequencing, Wilson's disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, lcsh:Biology (General), Genotype, medicine, Induced pluripotent stem cell, lcsh:QH301-705.5, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Wilson’s disease is an inherited disorder associated with copper accumulation in the liver, brain and other vital organs. Wilson’s disease is caused by mutations in the ATP7B gene. Over 300 mutations of ATP7B have been described. Despite the disease is autosomal recessive, the patient whose PBMCs were reprogrammed in the study harbours heterozygous mutation c.3207C > A (p.H1069Q). Detailed analysis of the ATP7B complete gene sequencing data has not revealed other known disease associated mutation. The generated iPSC lines maintained the original genotype, expressed pluripotency markers, had normal karyotype and demonstrated the ability to differentiate into derivatives of the three germ layers.

Published

2020

30. [Evolutionary Aspects of Genomic Imprinting]

Author

E A, Sazhenova and I N, Lebedev

Subjects

Genomic Imprinting, Pregnancy, Mutation, Animals, Female, DNA Methylation

Abstract

Genomic imprinting is an epigenetic phenomenon that differentiates maternal and paternal copies of genes in the genome and causes monoallelic expression depending on parental origin. Imprinting is an evolutionary puzzle, as it bears the costs of diploidization without its advantages, namely, protection from recessive mutations. The aim of this review is to answer the question of why genomic imprinting arose and became fixed in the evolution of angiosperms, insects, marsupials, and placental mammals.

Published

2020

31. Generation of two iPSC lines (IMGTi001-A and IMGTi001-B) from human skin fibroblasts with ring chromosome 22

Author

Elena A. Kizilova, I. N. Lebedev, A.A. Khabarova, Yu.S. Yakovleva, A.G. Menzorov, S. A. Vasilyev, T.V. Nikitina, M.E. Lopatkina, A. A. Kashevarova, Oleg L. Serov, and M.M. Gridina

Subjects

0301 basic medicine, Induced Pluripotent Stem Cells, Ring chromosome, Germ layer, Embryoid body, Biology, 03 medical and health sciences, medicine, Humans, Ring Chromosomes, Induced pluripotent stem cell, Mitosis, lcsh:QH301-705.5, Skin, Karyotype, Cell Biology, General Medicine, Fibroblasts, medicine.disease, Molecular biology, 030104 developmental biology, lcsh:Biology (General), Cell culture, Child, Preschool, Female, Teratoma, Developmental Biology

Abstract

Skin fibroblasts from a patient with intellectual disability and ring chromosome 22 were reprogrammed into induced pluripotent stem cells (iPSCs) to establish a clonal stem cell lines, IMGTi001-A (iTAF5-29) and IMGTi001-B (iTAF5-32). Because of ring chromosome mitotic instability these cell lines show mosaic karyotypes with 46,XX,r(22) in >83% cells, 45,XX,-22 as minor class and sporadically cells with other karyotypes. Differentiation in derivatives of all three germ layers was shown in teratoma assay for IMGTi001-A, and in embryoid bodies for both cell lines. To our knowledge, human iPSC lines with ring chromosome are described for the first time.

Published

2018

32. Regulation of karyotype stability in human induced pluripotent stem cells

Author

I. N. Lebedev and T. V. Nikitina

Subjects

Karyotype, General Medicine, Human Induced Pluripotent Stem Cells, Biology, Cell biology

Published

2018

33. HUMAN CYTOGENETICS IN GENOME AND POSTGENOME ERA: FROM GENOME ARCHITECTURE TO NOVEL CHROMOSOMAL DISEASES

Author

I. N. Lebedev

Subjects

medicine.medical_specialty, Cytogenetics, medicine, General Medicine, Computational biology, Biology, Chromosomal diseases, Genome, Genome architecture

Published

2018

34. P718Genome-wide copy number profiling of atherosclerotic plaques

Author

I N Lebedev, Olga Barbarash, L A Tashireva, A.A. Sleptcov, M S Nazarenko, N A Skryabin, N N Burkov, V P Puzyrev, E. V. Denisov, N. V. Krakhmal, and A. Kazantsev

Subjects

Pathology, medicine.medical_specialty, Atheroma, Array-Based Comparative Genomic Hybridization, business.industry, Myotonic dystrophy type 2, medicine, Cardiology and Cardiovascular Medicine, medicine.disease, business, Laser capture microdissection

Abstract

Background Atherosclerotic plaque formation results from complex cellular interactions in the intima of arteries, which take place between resident cells of the vessel wall (smooth muscle cells (SMC) and endothelial cells) and cells of the immune system (macrophages (MF)). Less well known is the genomic alterations in cells involving in the atherosclerotic process as can be important in plaque progression and instability. Aim The main purpose of the study is to assess the spectrum of structural genomic alterations in the tissue of atherosclerotic artery wall and to evaluate of difference between structural variants (SV) in SMC and MF. Materials and methods Samples of atherosclerotic plaques of the internal carotid artery (ICA) was collected from patients during endarterectomy (n=100) and the atherosclerotic coronary arteries (ACA) was obtained by coronary artery bypass surgery (n=10, group: bpACA) and by autopsy (n=8, apACA). Specimens were stored in liquid nitrogen. White blood cells (WBC) derived from the same patients. Control group was the health persons with same age (WBC, n=100). The genomic imbalances in bpACA were assessed by array comparative genomic hybridization (array-CGH, CGH Microarray 2x400K). Identified SVs was verified by droplet-digital PCR using TaqMan-assays (reference assay is RNAse P) in bpACA and ICA groups.SMC and MF were immunostained (Anti-Human CD68 Antibody and Alpha-SMA Antibody) and collected by laser capture microdissection of fresh frozen apACA samples (30–40 cells of each per sample). Collected cells were lysed and DNA amplified by whole genome amplification technique along with WBC of the same person, then analyzed by array-CGH. Results We found 90 SV in atherosclerotic coronary arteries, 13% of them were no mentioned before in Database of Genomic Variants. We selected interested SVs that contains only one gene (ACACB, ABCC9, ERLIN1, SFMBT1, PRKRA, and SIRPB1). The loss in the 3p21.1 region (SFMBT1) was in 11.48% patients and 8.5% in control group. Among patients who had diabetes mellitus (DM2) had more frequently loss of SFMBT1 (16%) than patients without DM2 (8%). The frequency of gain 2q31.2 (PRKRA) was 6% in patients whereas in control group we identified it in only one person. The frequency of loss 20p13 (SIRPB1) was approx. 67% in both groups. Several aneuploidies were found in MF (9 trisomies and 3 monosomies) and SMCs (1 trisomy and 8 monosomies). In two patients, SMCs had a normal karyotype. The ratio of duplications and deletions in MF and SMCs was 1:0.8 and 1:7, respectively. In MF of 6 patients identified same duplication in chromosome region 9q34.13-q34.2, (arr[hg19] 9q34.13(9:134337452-135931774)x3) about 2Mb in size. Conclusion Our study indicates that genomic alterations are diverse in their structure and are widely represented in cells involved in the atherosclerotic process.

Published

2019

35. 46,XY,r(8)/45,XY,−8 Mosaicism as a Possible Mechanism of the Imprinted Birk-Barel Syndrome: A Case Study

Author

Elizaveta A. Fonova, Elena O. Belyaeva, I. N. Lebedev, N.A. Skryabin, T. V. Nikitina, Dmitry A Fedotov, Lyudmila P. Nazarenko, A. A. Kashevarova, Aleksei A Sivtsev, S. A. Vasilyev, M.E. Lopatkina, Larisa I Mikhailik, and Aleksei A. Zarubin

Subjects

Male, 0301 basic medicine, Microcephaly, Monosomy, lcsh:QH426-470, Karyotype, Ring chromosome, Nerve Tissue Proteins, Biology, KCNK9, Article, Craniofacial Abnormalities, Genomic Imprinting, 03 medical and health sciences, Potassium Channels, Tandem Pore Domain, 0302 clinical medicine, Intellectual Disability, Gene duplication, Genetics, medicine, Humans, Ring Chromosomes, Allele, ring chromosome 8, Genetics (clinical), Mosaicism, Membrane Proteins, medicine.disease, lcsh:Genetics, Phenotype, Birk-Barel syndrome, 030104 developmental biology, Child, Preschool, Karyotyping, Mutation, Muscle Hypotonia, Chromosome Deletion, imprinting, Genomic imprinting, invdupdel(8p), 030217 neurology & neurosurgery, Chromosomes, Human, Pair 8, SNP array

Abstract

Ring chromosome 8 (r(8)) is one of the least frequent ring chromosomes. Usually, maternal chromosome 8 forms a ring, which can be lost from cells due to mitotic instability. The 8q24 region contains the imprinted KCNK9 gene, which is expressed from the maternal allele. Heterozygous KCNK9 mutations are associated with the imprinting disorder Birk-Barel syndrome. Here, we report a 2.5-year-old boy with developmental delay, microcephaly, dysmorphic features, diffuse muscle hypotonia, feeding problems, motor alalia and noncoarse neurogenic type of disturbance of muscle electrogenesis, partially overlapping with Birk-Barel syndrome phenotype. Cytogenetic analysis of lymphocytes revealed his karyotype to be 46,XY,r(8)(p23q24.3)[27]/45,XY,&minus, 8[3]. A de novo 7.9 Mb terminal 8p23.3p23.1 deletion, a 27.1 Mb 8p23.1p11.22 duplication, and a 4.4 Mb intact segment with a normal copy number located between them, as well as a 154-kb maternal LINGO2 gene deletion (9p21.2) with unknown clinical significance were identified by aCGH + SNP array. These aberrations were confirmed by real-time PCR. According to FISH analysis, the 8p23.1-p11.22 duplication was inverted. The ring chromosome originated from maternal chromosome 8. Targeted massive parallel sequencing did not reveal the KCNK9 mutations associated with Birk-Barel syndrome. Our data allow to assume that autosomal monosomy with inactive allele of imprinted gene arising from the loss of a ring chromosome in some somatic cells may be an etiological mechanism of mosaic imprinting disorders, presumably with less severe phenotype.

Published

2020

36. MOLECULAR KARYOTYPING BY USING CELL-FREE DNA FROM HUMAN BLASTOCOELE FLUID, EMBRYOBLAST AND TROPHOBLAST CELLS

Author

D I, Zhigalina, N A, Skryabin, V G, Artyukhova, A V, Svetlakov, and I N, Lebedev

Subjects

Karyotyping, Abnormal Karyotype, Humans, Cell-Free Nucleic Acids, Trophoblasts

Abstract

In the present study, we have carried out a comparative analysis of molecular karyotypes of cell free DNA from blastocoele fluid, trophectoderm and inner cell mass of human blastocysts at the preimplantation stages of development, using the comparative genomic hybridization. Different types of chromosomal abnormalities distribution between trophectoderm, inner cell mass and blastocoele fluid were identified. It was first shown that the source of cell free DNA in the blastocoele fluid may arise from the cells of inner cell mass in addition to the trophectoderm cells, which are traditionally used in preimplantation genetic diagnosis of chromosomal aberrations. These results support the promising of blastocentesis as a new technology of preimplantation genetic diagnosis, which provides the possibility of integral analysis of chromosome abnormalities in different cells of the blastocyst.

Published

2018

37. Induced pluripotent stem cell line, ICAGi001-A, derived from human skin fibroblasts of a patient with 2p25.3 deletion and 2p25.3-p23.3 inverted duplication

Author

I. N. Lebedev, A. A. Kashevarova, A.A. Khabarova, N. P. Babushkina, Lyudmila P. Nazarenko, N. V. Shilova, T.V. Nikitina, N.B. Torkhova, Oleg L. Serov, Zh. G. Markova, M.E. Minzhenkova, N.A. Skryabin, T.A. Gayner, Inna E. Pristyazhnyuk, and A.R. Shorina

Subjects

0301 basic medicine, Induced Pluripotent Stem Cells, Chromosome Disorders, Human skin, Germ layer, Biology, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Humans, Induced pluripotent stem cell, lcsh:QH301-705.5, Skin, Inverted duplication, Chromosome, Cell Biology, General Medicine, Fibroblasts, In vitro, Cell biology, 030104 developmental biology, lcsh:Biology (General), Cell culture, Child, Preschool, Chromosomes, Human, Pair 2, Female, Stem cell line, Chromosome Deletion, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Skin fibroblasts from a patient with developmental delay and chromosome 2p25.3 deletion syndrome were reprogrammed into induced pluripotent stem cells (iPSCs) and the clonal stem cell line ICAGi001-A (iTAF9-11) was established. ICAGi001-A pluripotency was demonstrated in vitro by three germ layer differentiation capacity. This line is a good model for studying of the developmental delay and brain disorder.

Published

2019

38. Markers of human extraembryonal cells individual radiosensitivity in vitro

Author

Andrey Alexandrovich Belenko, S. A. Vasilyev, and I. N. Lebedev

Subjects

γh2ax foci, lcsh:QH426-470, DNA damage, DNA repair, dna repair, Biology, Biochemistry, extraembryonic fibroblasts, chemistry.chemical_compound, Genetics, medicine, Radiosensitivity, dna double-strand breaks, Fibroblast, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Ecology, individual radiosensitivity, Molecular biology, Embryonic stem cell, In vitro, lcsh:Genetics, medicine.anatomical_structure, chemistry, micronuclei, Micronucleus test, DNA

Abstract

Background: Genotoxic effects of ionizing radiation in early stages of human embryonic development can lead to fatal consequences. At the same time, the radiosensitivity of human embryonic and extraembryonic cells is still poorly studied. In this study, the analysis of DNA double-strand break repair effectiveness in human extraembryonal fibroblasts was carried out. Materials and methods. Extraembryonic human fibroblasts was irradiated by 1 Gy gamma-rays using Theratron Equinox (Cancer Research Institute, Tomsk). The level of DNA double strand breaks was assessed using γH2AX foci. Frequency of cytogenetic damage was assessed using micronucleus test conducted with FISH as a frequency of centromere-negative micronuclei. Results. No significant correlation was observed between both endogenous and residual levels of radiation-induced γH2AX foci and frequency of micronuclei after irradiation. It is suggested to be a result of the specificity of extraembryonal fibroblast radiation-induced response. The spontaneous frequency of centromere-negative micronuclei correlated with radiation-induced frequency of centromere-negative micronuclei. Conclusion. It was shown that human extraembryonal fibroblasts ability to repair radiation-induced DNA damage is likely to be reflected by the repair of spontaneous DNA double strand breaks.

Published

2015

39. Reproductive (epi)genetics

Author

C. Lynch, N. Tee, H. Rouse, A. Gordon, L. Sati, C. Zeiss, B. Soygur, I. Bassorgun, E. Goksu, R. Demir, J. McGrath, M. L. Groendahl, L. Thuesen, A. N. Andersen, A. Loft, J. Smitz, T. Adriaenssens, J. Vikesa, R. Borup, E. Mersy, N. Kisters, M. V. E. Macville, J. J. M. Engelen, S.-E. N. N. Consortium, P. P. C. A. Menheere, J. P. Geraedts, A. B. C. Coumans, S. G. M. Frints, T. Aledani, S. Assou, S. Traver, O. Ait-ahmed, H. Dechaud, S. Hamamah, E. Mizutani, N. Suzumori, C. Sugiyama, Y. Hattori, T. Sato, H. Ando, Y. Ozaki, M. Sugiura-Ogasawara, M. Wissing, S. G. Kristensen, C. Y. Andersen, A. L. Mikkelsen, T. Hoest, A. Velthut-Meikas, J. Simm, M. Metsis, A. Salumets, S. Palini, L. Galluzzi, S. De Stefani, M. Primiterra, D. Wells, M. Magnani, C. Bulletti, P. H. Vogt, P. Frank-Herrmann, U. Bender, T. Strowitzki, B. Besikoglu, P. Heidemann, L. Wunsch, M. Bettendorf, L. Jelinkova, S. Vilimova, M. Kosarova, P. Sebek, E. Volemanova, M. Kruzelova, J. Civisova, L. Svobodova, V. Sobotka, T. Mardesic, C. van de Werken, M. A. Santos, C. Eleveld, J. S. E. Laven, E. B. Baart, L. Y. Pylyp, L. A. Spinenko, V. D. Zukin, J. Perez-Sanz, R. Matorras, J. Arluzea, J. Bilbao, N. Gonzalez-Santiago, N. Yeh, A. Koff, A. Barlas, Y. Romin, K. Manova-Todorova, C. D. l. Hoz, A. L. Mauri, A. M. Nascimento, L. D. Vagnini, C. G. Petersen, J. Ricci, F. C. Massaro, M. Cavagna, A. Pontes, J. B. A. Oliveira, R. L. R. Baruffi, J. G. Franco, E. X. Wu, S. Ma, M. Parriego, M. Sole, M. Boada, B. Coroleu, A. Veiga, G. Kakourou, M. Poulou, C. Vrettou, A. Destouni, J. Traeger-Synodinos, E. Kanavakis, A. N. Yatsenko, A. P. Georgiadis, M. M. McGuire, M. Zorrilla, K. D. Bunce, D. Peters, A. Rajkovic, M. Olszewska, M. Kurpisz, A. Z. A. Gilbertson, C. S. Ottolini, M. C. Summers, K. Sage, A. H. Handyside, A. R. Thornhill, D. K. Griffin, M. K. Chung, J. W. Kim, J. H. Lee, H. J. Jeong, M. H. Kim, M. J. Ryu, S. J. Park, H. Y. Kang, H. S. Lee, B. Zimmermann, M. Banjevic, M. Hill, P. Lacroute, M. Dodd, S. Sigurjonsson, P. Lau, D. Prosen, N. Chopra, A. Ryan, M. Hall, S. McAdoo, Z. Demko, B. Levy, M. Rabinowitz, A. Vereczeky, Z. S. Kosa, S. Savay, M. Csenki, L. Nanassy, B. Dudas, Z. S. Domotor, D. Debreceni, A. Rossi, J. R. Alegretti, J. Cuzzi, M. Bonavita, M. Tanada, P. Matunaga, P. Fettback, M. B. Rosa, V. Maia, P. Hassun, E. L. A. Motta, M. Piccolomini, C. Gomes, B. Barros, M. Nicoliello, T. Criscuolo, E. Miyadahira, D. Montjean, M. Benkhalifa, I. Berthaut, J. F. Griveau, K. Morcel, A. Bashamboo, K. McElreavey, C. Ravel, C. Rubio, L. Rodrigo, E. Mateu, A. Mercader, V. Peinado, P. Buendia, M. Milan, A. Delgado, N. Al-Asmar, L. Escrich, I. Campos-Galindo, S. Garcia-Herrero, M. E. Poo, P. Mir, C. Simon, A. Reyes-Engel, M. Cortes-Rodriguez, A. Lendinez, B. Perez-Nevot, A. R. Palomares, M. R. Galdon, A. Ruberti, M. G. Minasi, A. Biricik, A. Colasante, D. Zavaglia, E. Iammarrone, F. Fiorentino, E. Greco, N. Demir, S. Ozturk, B. Sozen, R. Morales, B. Lledo, J. A. Ortiz, J. Ten, J. Llacer, R. Bernabeu, M. Nagayoshi, A. Tanaka, I. Tanaka, H. Kusunoki, S. Watanabe, S. G. Temel, C. Beyazyurek, G. C. Ekmekci, F. Aybar, C. Cinar, S. Kahraman, S. Nordqvist, K. Karehed, H. Akerud, M. Gultomruk, P. Tulay, N. Findikli, E. Yagmur, G. Karlikaya, U. Ulug, M. Bahceci, M. F. Bargallo, M. R. Arevalo, M. M. Salat, I. V. Barbat, J. T. Lopez, M. E. Algam, A. B. Boluda, G. C. de Oya, E. N. Tolmacheva, A. A. Kashevarova, N. A. Skryabin, I. N. Lebedev, E. Semaco, A. Belo, M. Riboldi, L. Luz, N. Nobrega, R. Mazetto, J. A. Alegretti, M. Bibancos, P. Serafini, J. Neupane, M. Vandewoestyne, B. Heindryckx, T. Deroo, Y. Lu, S. Ghimire, S. Lierman, C. Qian, D. Deforce, P. De Sutter, T. Viloria, J. M. Martinez-Jabaloyas, M. Gil-Salom, A. Capalbo, N. Treff, D. Cimadomo, X. Tao, K. Ferry, F. M. Ubaldi, L. Rienzi, R. T. Scott, N. Katzorke, H. P. Vogt, A. Hehr, C. Gassner, B. Paulmann, Z. Kowalzyk, M. Klatt, S. Krauss, D. Seifert, B. Seifert, U. Hehr, M. Lobascio, M. T. Varricchio, P. Rubino, S. Bono, R. P. Cotarelo, L. Spizzichino, A. Colicchia, P. Giannini, M. Suhorutshenko, and K. Rosenstein-Tamm

Subjects

Genetics, Reproductive Medicine, Rehabilitation, Obstetrics and Gynecology, Biology

Published

2013

40. Early pregnancy

Author

A. Zeadna, H. Holzer, W. Y. Son, E. Demirtas, S. Reinblatt, M. H. Dahan, V. Colleselli, E. D'Costa, L. Wildt, B. Seeber, A. A. Kashevarova, N. A. Skryabin, T. V. Nikitina, I. N. Lebedev, P. P. Bordignon, A. Mugione, V. S. Vanni, P. Vigano, E. Papaleo, M. Candiani, E. Somigliana, G. Amodio, S. Gregori, Y. H. Guo, R. Li, L. L. Wang, S. L. Chen, X. Chen, W. Guo, D. S. Ye, Y. D. Liu, M. M. Renzini, M. Dal Canto, G. Coticchio, R. Comi, C. Brigante, I. Caliari, F. Brambillasca, M. Merola, M. Lain, D. Turchi, G. Karagouga, M. Sottocornola, R. Fadini, M. Z. Wekker, F. Mol, M. van Wely, W. M. Ankum, B. W. Mol, F. van der Veen, P. J. Hajenius, N. M. van Mello, C. Verlengia, E. Alviggi, M. R. Rampini, P. Alfano, I. Pergolini, D. Marconi, N. Iacobelli, M. C. Muzi, G. Gelli, C. Alviggi, A. Colicchia, L. Herraiz-Nicuesa, M. Tejera-Alhambra, A. Garcia-Segovia, R. Ramos-Medina, B. Alonso, J. Gil-Pulido, L. Martin, M. Caballero, M. Rodriguez-Mahou, S. Sanchez-Ramon, P. G. de Jong, S. P. Kaandorp, M. Di Nisio, M. Goddijn, S. Middeldorp, B. Lledo, A. Turienzo, J. A. Ortiz, R. Morales, J. Ten, J. Llacer, R. Bernabeu, J. Gil, J. A. Leon, A. Seyfferth, A. Aguaron, J. Alonso, E. C. de Albornoz, J. Carbone, P. Caballero, E. Fernandez-Cruz, L. Ortiz-Quintana, Y. Y. Lou, F. Jin, Y. M. Zheng, L. J. Li, F. Le, L. Y. Wang, S. Y. Liu, P. P. Pan, C. X. Hu, A. Akoum, A. Bourdiec, R. Shao, C. V. Rao, F. Scarpellini, M. Sbracia, N. Jancar, E. V. Bokal, H. Ban-Frangez, S. Drobnic, S. Korosec, B. Pinter, V. Salamun, M. Yamaguchi, R. Honda, K. Uchino, T. Ohba, H. Katabuchi, O. Leylek, B. Tiras, A. Y. S. E. Saltik, C. Halicigil, N. Kavci, A. Wiser, A. Gilbert, R. Nahum, R. Orvieto, J. Hass, A. Hourvitz, A. Weissman, G. Younes, M. Dirnfeld, A. Hershko, A. Shulma, E. Shalom-Paz, T. Tulandi, S. M. O'Neill, E. Agerbo, L. C. Kenny, T. B. Henriksen, P. M. Kearney, R. A. Greene, P. B. Mortensen, A. S. Khashan, V. S. Talaulikar, B. E. Bax, I. Manyonda, and N. Van Mello

Subjects

Reproductive Medicine, Rehabilitation, Obstetrics and Gynecology

Published

2013

41. [Estimation of association of CNTN6 copy number variation with idiopathic intellectual disability]

Author

M E, Lopatkina, A A, Kashevarova, and I N, Lebedev

Subjects

Adult, Male, Adolescent, INDEL Mutation, Contactins, Child, Preschool, Intellectual Disability, Gene Dosage, Humans, Female, Middle Aged, Child, Aged

Abstract

Analysis of the prevalence of copy number variations of the CNTN6 gene, recently selected as a new candidate gene for intellectual disorders, was performed. Real-time PCR did not detect any change in the number of CNTN6 gene copies in a group of 200 patients with impaired intellectual development. However, taking into account our data from the previous aCGH analysis and published data, the overall frequency of microdeletions and microduplications of CNTN6 was estimated as 1: 265 (0.4%). The common phenotypic features of 40 patients with microdeletions and microduplications of CNTN6 appeared to be the autism spectrum disorders, developmental delay, intellectual disability, seizures, cognitive impairment, cardiological defects, and behavioral problems.

Published

2016

42. [Preimplantation Genetic Diagnosis by Blastocentesis: Problems and Perspectives]

Author

D I, Zhigalina, N A, Skryabin, V G, Artyukhova, A V, Svetlakov, and I N, Lebedev

Subjects

Blastocyst, Mosaicism, Pregnancy, Karyotyping, Humans, Female, DNA, Genetic Testing, Preimplantation Diagnosis

Abstract

The discovery of cell-free DNA in blastocoele fluid opens new perspectives for the development of preimplantation genetic diagnosis of human chromosomal and genetic diseases. In this review we analyzed the results of the first studies, which made it possible to evaluate the effectiveness of the application of a new source of biological material and showed a high degree of agreement between the results of molecular karyotyping with cell-free DNA and blastocyst cells. The results suggest the possibility of developing a noninvasive method of preimplantation genetic diagnosis, which may open a new round of progress in the field of assisted reproductive technologies and the genetics of early stages of human ontogenesis.

Published

2016

43. [Genomic architecture of human chromosomal diseases]

Author

A A, Kashevarova and I N, Lebedev

Subjects

Chromosome Aberrations, DNA Copy Number Variations, Chromosomes, Human, Humans, Chromosome Disorders

Abstract

The genomic architecture predisposed to the emergence of DNA copy number variation causing a new class of human chromosomal diseases—reciprocal microdeletion and microduplication syndromes— is reviewed in the paper. The molecular mechanisms of such chromosomal abnormalities are described. The problems of the interpretation of their clinical significance and genotype-phenotype correlations are discussed. The classification of phenotypes due to reciprocal chromosomal microdeletions and microduplications is shown. Published by 2015, reciprocal mutations associated with inherited and congenital human pathology and involving 58 chromosomal regions are summarized.

Published

2016

44. [SKEWED X-CHROMOSOME INACTIVATION IN HUMAN MISCARRIAGES]

Author

E N, Tolmacheva, S A, Vasilyev, E A, Sazhenova, D I, Zhigalina, E I, Grigorovich, T V, Nikitina, A A, Melnikov, E S, Zhabina, T V, Ivanova, I D, Evtushenko, and I N, Lebedev

Subjects

Abortion, Spontaneous, Male, Abortion, Habitual, Chromosomes, Human, X, Pregnancy, X Chromosome Inactivation, Humans, Female, Embryo, Mammalian

Abstract

Sex ratio in first trimester of pregnancy is skewed due to preferential elimination of female embryos. It could be resulted from aberrant X-chromosome inactivation. X-chromosome inactivation was analyzed in extraembryonic tissues of miscarriages and induced abortions with 46, XX karyotype. In chorion cytotrophoblast of both miscarriages and induced abortions observed either random or skewed X-chromosome inactivation. In extraembryonic mesoderm of the control group, random inactivation was observed, whereas 15% of miscarriages had skewed X-chromosome inactivation. The highest frequency of skewed inactivation of one of the parental homologues was observed in the groups of blighted ovum pregnancy and embryos from women with recurrent pregnancy loss. It was suggested that in these cases compartmentalization of cells in the blastocyst probably leads to predominance of cell with mutant active X-chromosome among the cells of inner cell mass carrying the aberrations that are incompatible with normal embryonic development.

Published

2016

45. [ROLE OF CONTACTINS IN NEUROGENESIS IN HUMAN AND ANIMALS]

Author

N M, Matveeva, A A, Kashevarova, I N, Lebedev, and O L, Serov

Subjects

Neuronal Plasticity, Neurogenesis, Gene Expression Regulation, Developmental, Neurodegenerative Diseases, Cell Communication, Synaptic Transmission, Axons, Cell Movement, Contactins, Memory, Mutation, Cell Adhesion, Neurites, Animals, Humans

Abstract

Development of central and peripheral nervous system is one of the most complicated processes of embryogenesis. Dendritogenesis is an important component of this process because properties of dendritic branching define input and output signals received by neuron. Moreover, communications between neurons require transition of signal from dendrite of one neuron to axon of another, and this process of signal transduction underlies mechanisms of synaptic plasticity and memory formation. The neural cell adhesion molecules of the immunoglobulin superfamily involved in the control of dendritogenesis. In current review we focus our attention on 6 members of this adhesion molecules family: contactins 1-6. The contactins are proteins that control key events of neurogenesis: adhesion and migration of neuronal cells, orientation of growth of neurites and axons myelination. Functions of contactins are actively studied using model animals that express contactins in central and peripheral nervous system with almost similar to human pattern. Mutations of contactin-encoding genes result in abnormalities of neurogenesis process and development of multiple neurological disorders. Review is devoted to the role of contactin proteins in neurogenesis and nervous system disorders.

Published

2016

46. [Molecular Karyotyping of Cell-Free DNA from Blastocoele Fluid as a Basis for Noninvasive Preimplantation Genetic Screening of Aneuploidy]

Author

N A, Skryabin, I N, Lebedev, V G, Artukhova, D I, Zhigalina, I A, Stepanov, G V, Krivoschekova, and A V, Svetlakov

Subjects

Blastocyst, Karyotyping, Animals, DNA, Genetic Testing, Horses, Aneuploidy, Preimplantation Diagnosis

Abstract

The discovery of DNA fragments in the blastocoele fluid is promising for the development of new noninvasive methods for the preimplantation genetic diagnosis of chromosomal diseases. However, to date there are no data confirming the concordance between the molecular karyotype of cell-free DNA from blastocoele fluid and the blastocyst cells per se. This paper reports on this concordance according to the results of molecular-cytogenetic analysis of the chromosomal set with the use of comparative genomic hybridization.

Published

2016

47. SELECTED ORAL COMMUNICATION SESSION, SESSION 36: ANEUPLOIDY, Tuesday 5 July 2011 10:00 - 11:30

Author

E. N. Tolmacheva, A. Barker, C. Gimenez, Kumiko Oseto, Hans Jakob Ingerslev, P. Brezina, Kirstine Kirkegaard, E. Garcia-Guixé, Makoto Nakanishi, L. Du, Chisato Yamada-Namikawa, Mayumi Sugiura-Ogasawara, Nobuhiro Suzumori, J. Hindkjær, Amanda Souza Setti, N. N. Sukhanova, William G. Kearns, F.F. Pasqualetto, Assumpto Iaconelli, Daniela Paes de Almeida Ferreira Braga, K.H.D. Nguyen, M. Sandalinas, R. Ross, Eita Mizutani, Edson Borges, A. Jimenez-Macedo, Yasuhiko Ozaki, Kevin S. Richter, R.M. Anchan, C. Arjona, R.C.S. Figueira, A.A. Kashevarova, I. N. Lebedev, and A.T. Benner

Subjects

medicine.medical_specialty, Reproductive Medicine, business.industry, Rehabilitation, medicine, Obstetrics and Gynecology, Aneuploidy, Medical physics, Session (computer science), business, medicine.disease

Published

2011

48. Spontaneous aneuploidy level in blood cells of fertile females

Author

N. V. Zotova, AV Svetlakov, E. Markova, and I. N. Lebedev

Subjects

Fish technique, Hybridization probe, Aneuploidy, Reproductive age, Cell Biology, Biology, medicine.disease, Molecular biology, Andrology, Middle level, medicine, %22">Fish , Mutation detection, Multicolor fish

Abstract

In this study, we presented results of molecular cytogenetic assay of blood cells of fertile women of reproductive age. Cultivated and uncultivated cells and two sets of FISH probes with direct and indirect labeling were used. The middle level of aneuploidy for four chromosomes and statistical limits for aneuploidy detection were estimated. Aneuploidy determined with direct multicolor FISH in cultivated lymphocytes varied from 0.1 to 1.3%. The middle level of aneuploidy for all four chromosomes (13, 18, 21, and X) was 1.39%. The limit of mutation detection was 3.4%. We found differences in results with direct and indirect labeling. It was shown that the cultivation process influenced the level of aneuploidy. The absolute error in FISH technique was 0.13% and the relative error was 4.08%.

Published

2009

49. [Background Level of γH2AX Foci in Human Cells as a Factor of Individual Radiosensitivity]

Author

S A, Vasilyev, A I, Velichevskaya, T V, Vishnevskaya, A A, Belenko, O V, Gribova, M B, Plaksin, Zh A, Startseva, and I N, Lebedev

Subjects

Adult, Male, Micronucleus Tests, DNA Repair, Middle Aged, Radiation Tolerance, Histones, Young Adult, Gamma Rays, Humans, DNA Breaks, Double-Stranded, Lymphocytes, Cells, Cultured, Micronuclei, Chromosome-Defective, Aged

Abstract

The paper analyzes the effects of spontaneous level of yH2AX and 53BP1 foci on a frequency of radiation-induced centromere-negative and centromere-positive micronuclei in peripheral blood lymphocytes of 54 healthy individuals after exposure to 2 Gy of ionizing radiation in vitro. An inverse correlation was found between the level of spontaneous yH2AX foci and the frequency of centromere-negative micronuclei after irradiation. The corresponding correlations between the spontaneous level of protein 53BP1 foci and the frequency of centromere-negative micronuclei were not statistically significant. In addition, cells of the individuals with a high frequency of radiation-induced micronuclei were also characterized by a low proliferative activity. It was suggested that DNA double strand break repair works less efficiently in cells of the individuals with low levels of spontaneous yH2AX foci, and a greater number of DNA double strand breaks after exposure to ionizing radiation remains unrepaired, thus leading to a cell cycle block and an increase of the frequency of centromere-negative micronuclei.

Published

2015

50. [Methylation status of line-1 retrotransposon in chromosomal mosaicism during the early stages of human embryonic development]

Author

S A, Vasil'ev, E N, Tolmacheva, A A, Kashevarova, E A, Sazhenova, and I N, Lebedev

Subjects

Abortion, Spontaneous, Chromosome Aberrations, Long Interspersed Nucleotide Elements, Base Sequence, Mosaicism, Pregnancy, Embryonic Development, Humans, Female, DNA Methylation, Aneuploidy

Abstract

Early stages of human embryonic development are characterized by spatio-temporal coincidence of events of total epigenetic genome reprogramming and elevated level of mosaic forms of numerical chromosome abnormalities. It is possible that the abnormal reprogramming of various regions of the genome can lead to violations of local epigenetic chromatin organization and gene expression, affecting the correct chromosome segregation during mitosis. In this study, a comparative analysis of the methylation index of LINE-1 retrotransposon, which is largely reflecting the methylation profile of the genome, is performed in placental tissues of spontaneous abortions with complete and mosaic forms of aneuploidy, and with a normal karyotype, as well as in the control group of induced abortions of the first trimester of pregnancy. It was shown that extraembryonic mesoderm and chorionic cytotrophoblast of spontaneous abortions with chromosomal mosaicism are characterized by the highest index of LINE-1 methylation among all groups studied. At the same time excessive hypomethylation of transposable genetic element recorded in spontaneous abortions with normal karyotype. It is suggested that violations of parental genomes demethylation during epigenetic reprogramming at preimplantation stages of development may be associated with an increased frequency of mitotic errors in chromosome segregation, leading to the formation of a mosaic karyotype.

Published

2015