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1. Whole tumor analysis reveals early origin of the TERT promoter mutation and intercellular heterogeneity in TERT expression

Author

Appin, Christina L, Hong, Chibo, Suwala, Abigail K, Hilz, Stephanie, Mathur, Radhika, Solomon, David A, Smirnov, Ivan V, Stevers, Nicholas O, Shai, Anny, Wang, Albert, Berger, Mitchel S, Chang, Susan M, Phillips, Joanna J, and Costello, Joseph F

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Cancer, Genetics, Cancer, Neurosciences, Brain Disorders, Human Genome, Rare Diseases, Cancer Genomics, Humans, Brain Neoplasms, Glioma, Glioblastoma, Oligodendroglioma, Mutation, Biomarkers, Tumor, Isocitrate Dehydrogenase, Telomerase, Proto-Oncogene Proteins, Cell Cycle Proteins, glioblastoma, oligodendroglioma, sequencing, TERT, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

BackgroundThe TERT promoter mutation (TPM) is acquired in most IDH-wildtype glioblastomas (GBM) and IDH-mutant oligodendrogliomas (OD) enabling tumor cell immortality. Previous studies on TPM clonality show conflicting results. This study was performed to determine whether TPM is clonal on a tumor-wide scale.MethodsWe investigated TPM clonality in relation to presumed early events in 19 IDH-wildtype GBM and 10 IDH-mutant OD using 3-dimensional comprehensive tumor sampling. We performed Sanger sequencing on 264 tumor samples and deep amplicon sequencing on 187 tumor samples. We obtained tumor purity and copy number estimates from whole exome sequencing. TERT expression was assessed by RNA-seq and RNAscope.ResultsWe detected TPM in 100% of tumor samples with quantifiable tumor purity (219 samples). Variant allele frequencies (VAF) of TPM correlate positively with chromosome 10 loss in GBM (R = 0.85), IDH1 mutation in OD (R = 0.87), and with tumor purity (R = 0.91 for GBM; R = 0.90 for OD). In comparison, oncogene amplification was tumor-wide for MDM4- and most EGFR-amplified cases but heterogeneous for MYCN and PDGFRA, and strikingly high in low-purity samples. TPM VAF was moderately correlated with TERT expression (R = 0.52 for GBM; R = 0.65 for OD). TERT expression was detected in a subset of cells, solely in TPM-positive samples, including samples equivocal for tumor.ConclusionsOn a tumor-wide scale, TPM is among the earliest events in glioma evolution. Intercellular heterogeneity of TERT expression, however, suggests dynamic regulation during tumor growth. TERT expression may be a tumor cell-specific biomarker.

Published
2024

2. Two-dimensional high-throughput on-cell screening of immunoglobulins against broad antigen repertoires

Author

Lomakin, Yakov A., Ovchinnikova, Leyla A., Terekhov, Stanislav S., Dzhelad, Samir S., Yaroshevich, Igor, Mamedov, Ilgar, Smirnova, Anastasia, Grigoreva, Tatiana, Eliseev, Igor E., Filimonova, Ioanna N., Mokrushina, Yuliana A., Abrikosova, Victoria, Rubtsova, Maria P., Kostin, Nikita N., Simonova, Maria A., Bobik, Tatiana V., Aleshenko, Natalia L., Alekhin, Alexander I., Boitsov, Vitali M., Zhang, Hongkai, Smirnov, Ivan V., Rubtsov, Yuri P., and Gabibov, Alexander G.

Published
2024
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3. Glioblastoma evolution and heterogeneity from a 3D whole-tumor perspective

Author

Mathur, Radhika, Wang, Qixuan, Schupp, Patrick G, Nikolic, Ana, Hilz, Stephanie, Hong, Chibo, Grishanina, Nadia R, Kwok, Darwin, Stevers, Nicholas O, Jin, Qiushi, Youngblood, Mark W, Stasiak, Lena Ann, Hou, Ye, Wang, Juan, Yamaguchi, Takafumi N, Lafontaine, Marisa, Shai, Anny, Smirnov, Ivan V, Solomon, David A, Chang, Susan M, Hervey-Jumper, Shawn L, Berger, Mitchel S, Lupo, Janine M, Okada, Hideho, Phillips, Joanna J, Boutros, Paul C, Gallo, Marco, Oldham, Michael C, Yue, Feng, and Costello, Joseph F

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Disorders, Cancer Genomics, Rare Diseases, Brain Cancer, Neurosciences, Genetics, Cancer, Human Genome, Precision Medicine, Humans, Brain Neoplasms, Epigenomics, Genomics, Glioblastoma, Single-Cell Analysis, Tumor Microenvironment, Models, Biological, Genetic Heterogeneity, brain tumors, chromatin accessibility, chromatin interactions, epigenomics, genomics, glioblastoma, intratumoral heterogeneity, microenvironment, spatial analysis, tumor evolution, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

Treatment failure for the lethal brain tumor glioblastoma (GBM) is attributed to intratumoral heterogeneity and tumor evolution. We utilized 3D neuronavigation during surgical resection to acquire samples representing the whole tumor mapped by 3D spatial coordinates. Integrative tissue and single-cell analysis revealed sources of genomic, epigenomic, and microenvironmental intratumoral heterogeneity and their spatial patterning. By distinguishing tumor-wide molecular features from those with regional specificity, we inferred GBM evolutionary trajectories from neurodevelopmental lineage origins and initiating events such as chromothripsis to emergence of genetic subclones and spatially restricted activation of differential tumor and microenvironmental programs in the core, periphery, and contrast-enhancing regions. Our work depicts GBM evolution and heterogeneity from a 3D whole-tumor perspective, highlights potential therapeutic targets that might circumvent heterogeneity-related failures, and establishes an interactive platform enabling 360° visualization and analysis of 3D spatial patterns for user-selected genes, programs, and other features across whole GBM tumors.

Published
2024

7. Cross-regulation of antibody responses against the SARS-CoV-2 Spike protein and commensal microbiota via molecular mimicry

Author

Bondareva, Marina, Budzinski, Lisa, Durek, Pawel, Witkowski, Mario, Angermair, Stefan, Ninnemann, Justus, Kreye, Jakob, Letz, Philine, Ferreira-Gomes, Marta, Semin, Iaroslav, Guerra, Gabriela Maria, Momsen Reincke, S., Sánchez-Sendin, Elisa, Yilmaz, Selin, Sempert, Toni, Heinz, Gitta Anne, Tizian, Caroline, Raftery, Martin, Schönrich, Günther, Matyushkina, Daria, Smirnov, Ivan V., Govorun, Vadim M., Schrezenmeier, Eva, Stefanski, Anna-Luisa, Dörner, Thomas, Zocche, Silvia, Viviano, Edoardo, Klement, Nele, Sehmsdorf, Katharina Johanna, Lunin, Alexander, Chang, Hyun-Dong, Drutskaya, Marina, Kozlovskaya, Liubov, Treskatsch, Sascha, Radbruch, Andreas, Diefenbach, Andreas, Prüss, Harald, Enghard, Philipp, Mashreghi, Mir-Farzin, and Kruglov, Andrey A.

Published
2023
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10. Longer genotypically-estimated leukocyte telomere length is associated with increased meningioma risk

Author

Muskens, Ivo S, Hansen, Helen M, Smirnov, Ivan V, Molinaro, Annette M, Bondy, Melissa L, Schildkraut, Joellen M, Wrensch, Margaret, Wiemels, Joseph L, and Claus, Elizabeth B

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Disorders, Cancer, Brain Cancer, Human Genome, Rare Diseases, Neurosciences, Genetics, Case-Control Studies, Female, Follow-Up Studies, Genotype, Humans, Leukocytes, Male, Meningeal Neoplasms, Meningioma, Polymorphism, Single Nucleotide, Prognosis, Risk Factors, Telomere Homeostasis, Leukocyte telomere length, Mendelian randomization, Risk, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

PurposeTelomere length-associated SNPs have been associated with incidence and survival rates for malignant brain tumors such as glioma. Here, we study the influence of genetically determined lymphocyte telomere length (LTL) by comparing telomerase associated SNPs between the most common non-malignant brain tumor, i.e. meningioma, and healthy controls.Methods/patientsOne thousand fifty-three (1053) surgically treated meningioma patients and 4437 controls of Western European ancestry were included. Germline DNA was genotyped for 8 SNPs previously significantly associated with LTL. Genotypically-estimated LTL was then calculated by summing each SNP's genotypically-specified telomere length increase in base pairs (bp) for each person. Odds ratios for genotypically-estimated LTL in meningioma cases and controls were evaluated using logistic regression with the first two ancestral principal components and sex as covariates.ResultsThree out of the eight evaluated LTL SNPs were significantly associated with increased meningioma risk (rs10936599: OR 1.14, 95% CI 1.01-1.28, rs2736100: OR 1.13, 95% CI 1.03-1.25, rs9420907: OR 1.22, 95% CI 1.07-1.39). Only rs9420907 remained significant after correction for multiple testing. Average genotypically-estimated LTL was significantly longer for those with meningioma compared to controls [mean cases: 560.2 bp (standard error (SE): 4.05 bp), mean controls: 541.5 bp (SE: 2.02 bp), logistic regression p value = 2.13 × 10-5].ConclusionIncreased genotypically-estimated LTL was significantly associated with increased meningioma risk. A role for telomere length in the pathophysiology of meningioma is novel, and could lead to new insights on the etiology of meningioma.

Published
2019

13. Branched Linkers for Homogeneous Antibody-Drug Conjugates: How Long Is Long Enough?

Author

Gulyak, Evgeny L., Komarova, Olga A., Prokopenko, Yury A., Faizullina, Elina A., Malabuiok, Diana M., Ibragimova, Aigul R., Mokrushina, Yuliana A., Serova, Oxana V., Popova, Galina P., Zhitlov, Mikhail Y., Nikitin, Timofei D., Brylev, Vladimir A., Ustinov, Alexey V., Alferova, Vera A., Korshun, Vladimir A., Smirnov, Ivan V., Terekhov, Stanislav S., and Sapozhnikova, Ksenia A.

Abstract

Homogeneous antibody–drug conjugates (ADCs) exhibit significantly improved pharmacological properties compared to their heterogeneous counterparts. Site-specific conjugation of the payload to the IgG required for homogeneity can be achieved using enzymes. One example is microbial transglutaminase (MTGase), which can selectively perform transamidation on the Q295 residue of human Fc when N297 glycans are removed. As a result, two modifications can be introduced per IgG molecule; however, achieving higher drug-to-antibody ratios (DARs) requires the use of branched linkers. While several such linkers have been reported, little information is available on the relationship between linker structure and ADC properties. To address this gap, we synthesized two branched amino triazide linkers, differing by a PEG4 fragment inserted after the branching point, which were used to prepare two homogeneous trastuzumab-based DAR 6 ADCs (a "short" and a "long" one). This was achieved by a two-step process consisting of enzymatic linker conjugation followed by bioorthogonal coupling with a cleavable linker bearing monomethyl auristatin E (MMAE). Two other trastuzumab–MMAE conjugates were used as controls: a heterogeneous DAR 6 ADC, made using conventional thiol–maleimide chemistry, and a homogeneous DAR 2 ADC. We found that, while the four conjugates had identical affinity for HER2, their cytotoxicity differed significantly: the "long" homogeneous DAR 6 ADC was just as active as its heterogeneous counterpart, but the "short" DAR 6 ADC was an order of magnitude less potent, inferior even to the DAR 2 conjugate. Our findings indicate that the length of the branched linker critically affects the cytotoxic activity of ADCs, possibly due to steric hindrance influencing the rate of linker cleavage by lysosomal enzymes. [ABSTRACT FROM AUTHOR]

Published
2024
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15. Two HLA class II gene variants are independently associated with pediatric osteosarcoma risk

Author

Zhang, Chenan, Wiemels, Joseph L, Hansen, Helen M, Gonzalez-Maya, Julio, Endicott, Alyson A, de Smith, Adam J, Smirnov, Ivan V, Witte, John S, Morimoto, Libby M, Metayer, Catherine, and Walsh, Kyle M

Subjects
Epidemiology, Biomedical and Clinical Sciences, Health Sciences, Human Genome, Prevention, Pediatric, Cancer, Rare Diseases, Pediatric Cancer, Genetics, 2.1 Biological and endogenous factors, Adult, Bone Neoplasms, Case-Control Studies, Female, Follow-Up Studies, Genes, MHC Class II, Genetic Predisposition to Disease, Genotype, Humans, Male, Meta-Analysis as Topic, Osteosarcoma, Polymorphism, Single Nucleotide, Prognosis, Young Adult, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences
Abstract

Background: The genetic etiology of osteosarcoma remains poorly understood despite the publication of a genome-wide association study. Association between HLA genetic variants and risk of several cancers has been observed, but HLA variation is not well captured by standard SNP arrays.Methods: We genotyped 207 Californian pediatric osteosarcoma cases and 696 controls of European ancestry using a custom genome-wide array supplemented with approximately 6,000 additional probes across the MHC region. We subsequently imputed 4-digit classical HLA alleles using a reference panel of 5,225 individuals who underwent high-resolution HLA typing via next-generation sequencing. Case-control comparisons were adjusted for ancestry-informative principal components, and top associations from the discovery analysis underwent replication in an independent dataset of 657 cases and 1,183 controls.Results: Three highly correlated HLA class II variants (r 2 = 0.33-0.98) were associated with osteosarcoma risk in discovery analyses, including HLA-DRB1*0301 (OR = 0.52; P = 3.2 × 10-3), HLA-DQA1*0501 (OR = 0.74; P = 0.031), and HLA-DQB1*0201 (OR = 0.51; P = 2.7 × 10-3). Similar associations were observed in the replication data (P range = 0.011-0.037). Meta-analysis of the two datasets identified HLA-DRB1*0301 as the most significantly associated variant (ORmeta = 0.62; P meta = 1.5 × 10-4), reaching Bonferroni-corrected statistical significance. The meta-analysis also revealed a second significant independent signal at HLA-DQA1*01:01 (ORmeta = 1.33, P meta = 1.2 × 10-3), and a third suggestive association at HLA-DQB1*0302 (ORmeta = 0.73, P meta = 6.4 × 10-3).Conclusions: Multiple independent HLA class II alleles may influence osteosarcoma risk.Impact: Additional work is needed to extend our observations to other patient populations and to clarify the potential causal mechanisms underlying these associations. Understanding immunologic contributions to the etiology of osteosarcoma may inform rational therapeutic targets. Cancer Epidemiol Biomarkers Prev; 27(10); 1151-8. ©2018 AACR.

Published
2018

16. Genetic determinants of childhood and adult height associated with osteosarcoma risk

Author

Zhang, Chenan, Morimoto, Libby M, de Smith, Adam J, Hansen, Helen M, Gonzalez‐Maya, Julio, Endicott, Alyson A, Smirnov, Ivan V, Metayer, Catherine, Wei, Qingyi, Eward, William C, Wiemels, Joseph L, and Walsh, Kyle M

Subjects
Epidemiology, Biomedical and Clinical Sciences, Health Sciences, Rare Diseases, Pediatric, Pediatric Cancer, Genetics, Human Genome, Cancer, Adult, Body Height, Bone Neoplasms, California, Case-Control Studies, Child, Child Development, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Infant, Newborn, Male, Multifactorial Inheritance, Neonatal Screening, Osteosarcoma, Polymorphism, Single Nucleotide, Registries, Risk Factors, White People, Young Adult, height, Mendelian randomization, osteosarcoma, pediatric cancer, polygenic score, Oncology and Carcinogenesis, Public Health and Health Services, Oncology & Carcinogenesis, Oncology and carcinogenesis, Public health
Abstract

BackgroundAlthough increased height has been associated with osteosarcoma risk in previous epidemiologic studies, to the authors' knowledge the relative contribution of stature during different developmental timepoints remains unclear. Furthermore, the question of how genetic determinants of height impact osteosarcoma etiology remains unexplored. Genetic variants associated with stature in previous genome-wide association studies may be biomarkers of osteosarcoma risk.MethodsThe authors tested the associations between osteosarcoma risk and polygenic scores for adult height (416 variants), childhood height (6 variants), and birth length (5 variants) in 864 osteosarcoma cases and 1879 controls of European ancestry.ResultsEach standard deviation increase in the polygenic score for adult height, corresponding to a 1.7-cm increase in stature, was found to be associated with a 1.10-fold increase in the risk of osteosarcoma (95% confidence interval [95% CI], 1.01-1.19; P =.027). Each standard deviation increase in the polygenic score for childhood height, corresponding to a 0.5-cm increase in stature, was associated with a 1.10-fold increase in the risk of osteosarcoma (95% CI, 1.01-1.20; P =.023). The polygenic score for birth length was not found to be associated with osteosarcoma risk (P =.11). When adult and childhood height scores were modeled together, they were found to be independently associated with osteosarcoma risk (P =.037 and P = .043, respectively). An expression quantitative trait locus for cartilage intermediate layer protein 2 (CILP2), rs8103992, was significantly associated with osteosarcoma risk after adjustment for multiple comparisons (odds ratio, 1.35; 95% CI, 1.16-1.56 [P = 7.93×10-5 and Padjusted =.034]).ConclusionsA genetic propensity for taller adult and childhood height attainments contributed independently to osteosarcoma risk in the current study data. These results suggest that the biological pathways affecting normal bone growth may be involved in osteosarcoma etiology.

Published
2018

17. Genomic analysis of the origins and evolution of multicentric diffuse lower-grade gliomas

Author

Hayes, Josie, Yu, Yao, Jalbert, Llewellyn E, Mazor, Tali, Jones, Lindsey E, Wood, Matthew D, Walsh, Kyle M, Bengtsson, Henrik, Hong, Chibo, Oberndorfer, Stefan, Roetzer, Thomas, Smirnov, Ivan V, Clarke, Jennifer L, Aghi, Manish K, Chang, Susan M, Nelson, Sarah J, Woehrer, Adelheid, Phillips, Joanna J, Solomon, David A, and Costello, Joseph F

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Genetics, Brain Cancer, Cancer Genomics, Human Genome, Biotechnology, Neurosciences, Cancer, Rare Diseases, Clinical Research, Brain Disorders, Orphan Drug, 2.1 Biological and endogenous factors, Adult, Biomarkers, Tumor, Brain Neoplasms, Clonal Evolution, Female, Genomics, Glioma, Humans, Male, Middle Aged, Mutation, Neoplasm Grading, Phylogeny, Young Adult, astrocytoma, bilateral, IDH1, multicentric, oligodendroglioma, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

BackgroundRare multicentric lower-grade gliomas (LGGs) represent a unique opportunity to study the heterogeneity among distinct tumor foci in a single patient and to infer their origins and parallel patterns of evolution.MethodsIn this study, we integrate clinical features, histology, and immunohistochemistry for 4 patients with multicentric LGG, arising both synchronously and metachronously. For 3 patients we analyze the phylogeny of the lesions using exome sequencing, including one case with a total of 8 samples from the 2 lesions.ResultsOne patient was diagnosed with multicentric isocitrate dehydrogenase 1 (IDH1) mutated diffuse astrocytomas harboring distinct IDH1 mutations, R132H and R132C; the latter mutation has been associated with Li-Fraumeni syndrome, which was subsequently confirmed in the patient's germline DNA and shown in additional cases with The Cancer Genome Atlas data. In another patient, phylogenetic analysis of synchronously arising grade II and grade III diffuse astrocytomas demonstrated a single shared mutation, IDH1 R132H, and revealed convergent evolution via non-overlapping mutations in ATRX and TP53. In 2 cases, there was divergent evolution of IDH1-mutated and 1p/19q-codeleted oligodendroglioma and IDH1-mutated and 1p/19q-intact diffuse astrocytoma, occurring synchronously in one case and metachronously in a second.ConclusionsEach tumor in multicentric LGG cases may arise independently or may diverge very early in their development, presenting as genetically and histologically distinct tumors. Comprehensive sampling of these lesions can therefore significantly alter diagnosis and management. Additionally, somatic IDH1 R132C mutation in either multicentric or solitary LGG identifies unsuspected germline TP53 mutation, validating the limited number of published cases.

Published
2018

19. Liquid drop of DNA libraries reveals total genome information

Author

Terekhov, Stanislav S., Eliseev, Igor E., Ovchinnikova, Leyla A., Kabilov, Marsel R., Prjibelski, Andrey D., Tupikin, Alexey E., Smirnov, Ivan V., Belogurov, Alexey A., Severinov, Konstantin V., Lomakin, Yakov A., Altman, Sidney, and Gabibov, Alexander G.

Published
2020

20. Multiscale computation delivers organophosphorus reactivity and stereoselectivity to immunoglobulin scavengers

Author

Mokrushina, Yuliana A., Golovin, Andrey V., Smirnov, Ivan V., Chatziefthimiou, Spyros D., Stepanova, Anastasia V., Bobik, Tatyana V., Zalevsky, Arthur O., Zlobin, Alexander S., Konovalov, Kirill A., Terekhov, Stanislav S., Stepanov, Alexey V., Pipiya, Sofiya O., Shamborant, Olga G., Round, Ekaterina, Belogurov, Alexey A., Bourenkov, Gleb, Makarov, Alexander A., Wilmanns, Matthias, Xie, Jia, Blackburn, G. Michael, Gabibov, Alexander G., and Lerner, Richard A.

Published
2020

22. Comprehensive Analysis of Hypermutation in Human Cancer

Author

Campbell, Brittany B, Light, Nicholas, Fabrizio, David, Zatzman, Matthew, Fuligni, Fabio, de Borja, Richard, Davidson, Scott, Edwards, Melissa, Elvin, Julia A, Hodel, Karl P, Zahurancik, Walter J, Suo, Zucai, Lipman, Tatiana, Wimmer, Katharina, Kratz, Christian P, Bowers, Daniel C, Laetsch, Theodore W, Dunn, Gavin P, Johanns, Tanner M, Grimmer, Matthew R, Smirnov, Ivan V, Larouche, Valérie, Samuel, David, Bronsema, Annika, Osborn, Michael, Stearns, Duncan, Raman, Pichai, Cole, Kristina A, Storm, Phillip B, Yalon, Michal, Opocher, Enrico, Mason, Gary, Thomas, Gregory A, Sabel, Magnus, George, Ben, Ziegler, David S, Lindhorst, Scott, Issai, Vanan Magimairajan, Constantini, Shlomi, Toledano, Helen, Elhasid, Ronit, Farah, Roula, Dvir, Rina, Dirks, Peter, Huang, Annie, Galati, Melissa A, Chung, Jiil, Ramaswamy, Vijay, Irwin, Meredith S, Aronson, Melyssa, Durno, Carol, Taylor, Michael D, Rechavi, Gideon, Maris, John M, Bouffet, Eric, Hawkins, Cynthia, Costello, Joseph F, Meyn, M Stephen, Pursell, Zachary F, Malkin, David, Tabori, Uri, and Shlien, Adam

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Oncology and Carcinogenesis, Cancer, Rare Diseases, Cancer Genomics, Human Genome, 2.1 Biological and endogenous factors, Good Health and Well Being, Adult, Child, Cluster Analysis, DNA Polymerase II, DNA Polymerase III, DNA Replication, Humans, Mutation, Neoplasms, Poly-ADP-Ribose Binding Proteins, DNA repair, DNA replication, cancer genomics, cancer predisposition, hypermutation, immune checkpoint inhibitors, mismatch repair, mutator, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences
Abstract

We present an extensive assessment of mutation burden through sequencing analysis of >81,000 tumors from pediatric and adult patients, including tumors with hypermutation caused by chemotherapy, carcinogens, or germline alterations. Hypermutation was detected in tumor types not previously associated with high mutation burden. Replication repair deficiency was a major contributing factor. We uncovered new driver mutations in the replication-repair-associated DNA polymerases and a distinct impact of microsatellite instability and replication repair deficiency on the scale of mutation load. Unbiased clustering, based on mutational context, revealed clinically relevant subgroups regardless of the tumors' tissue of origin, highlighting similarities in evolutionary dynamics leading to hypermutation. Mutagens, such as UV light, were implicated in unexpected cancers, including sarcomas and lung tumors. The order of mutational signatures identified previous treatment and germline replication repair deficiency, which improved management of patients and families. These data will inform tumor classification, genetic testing, and clinical trial design.

Published
2017

23. Non-additive and epistatic effects of HLA polymorphisms contributing to risk of adult glioma

Author

Zhang, Chenan, de Smith, Adam J, Smirnov, Ivan V, Wiencke, John K, Wiemels, Joseph L, Witte, John S, and Walsh, Kyle M

Subjects
Biomedical and Clinical Sciences, Neurosciences, Oncology and Carcinogenesis, Genetics, Human Genome, Cancer, Rare Diseases, Health Disparities, Minority Health, 2.1 Biological and endogenous factors, Brain Neoplasms, Case-Control Studies, Female, Genetic Association Studies, Genetic Predisposition to Disease, Glioma, HLA Antigens, Haplotypes, Heterozygote, Homozygote, Humans, Male, Middle Aged, Models, Genetic, Polymorphism, Single Nucleotide, White People, Brain tumor, HLA, MHC, Non-additive effects, Epistasis, Interactions, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

Although genome-wide association studies have identified several susceptibility loci for adult glioma, little is known regarding the potential contribution of genetic variation in the human leukocyte antigen (HLA) region to glioma risk. HLA associations have been reported for various malignancies, with many studies investigating selected candidate HLA polymorphisms. However, no systematic analysis has been conducted in glioma patients, and no investigation into potential non-additive effects has been described. We conducted comprehensive genetic analyses of HLA variants among 1746 adult glioma patients and 2312 controls of European-ancestry from the GliomaScan Consortium. Genotype data were generated with the Illumina 660-Quad array, and we imputed HLA alleles using a reference panel of 5225 individuals in the Type 1 Diabetes Genetics Consortium who underwent high-resolution HLA typing via next-generation sequencing. Case-control comparisons were adjusted for population stratification using ancestry-informative principal components. Because alleles in different loci across the HLA region are linked, we created multigene haplotypes consisting of the genes DRB1, DQA1, and DQB1. Although none of the haplotypes were associated with glioma in additive models, inclusion of a dominance term significantly improved the model for multigene haplotype HLA-DRB1*1501-DQA1*0102-DQB1*0602 (P = 0.002). Heterozygous carriers of the haplotype had an increased risk of glioma [odds ratio (OR) 1.23; 95% confidence interval (CI) 1.01-1.49], while homozygous carriers were at decreased risk compared with non-carriers (OR 0.64; 95% CI 0.40-1.01). Our results suggest that the DRB1*1501-DQA1*0102-DQB1*0602 haplotype may contribute to the risk of glioma in a non-additive manner, with the positive dominance effect partly explained by an epistatic interaction with HLA-DRB1*0401-DQA1*0301-DQB1*0301.

Published
2017

24. Clonal expansion and epigenetic reprogramming following deletion or amplification of mutant IDH1

Author

Mazor, Tali, Chesnelong, Charles, Pankov, Aleksandr, Jalbert, Llewellyn E, Hong, Chibo, Hayes, Josie, Smirnov, Ivan V, Marshall, Roxanne, Souza, Camila F, Shen, Yaoqing, Viswanath, Pavithra, Noushmehr, Houtan, Ronen, Sabrina M, Jones, Steven JM, Marra, Marco A, Cairncross, J Gregory, Perry, Arie, Nelson, Sarah J, Chang, Susan M, Bollen, Andrew W, Molinaro, Annette M, Bengtsson, Henrik, Olshen, Adam B, Weiss, Samuel, Phillips, Joanna J, Luchman, H Artee, and Costello, Joseph F

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Disorders, Brain Cancer, Rare Diseases, Cancer, Cancer Genomics, Human Genome, Genetics, 2.1 Biological and endogenous factors, Brain Neoplasms, DNA Copy Number Variations, DNA Methylation, Epigenomics, Gene Amplification, Gene Expression Profiling, Glioma, Glutarates, Humans, Isocitrate Dehydrogenase, Mutation, Neoplasm Recurrence, Local, Sequence Deletion, Tumor Cells, Cultured, IDH1, DNA methylation, 2HG, glioma, copy number
Abstract

IDH1 mutation is the earliest genetic alteration in low-grade gliomas (LGGs), but its role in tumor recurrence is unclear. Mutant IDH1 drives overproduction of the oncometabolite d-2-hydroxyglutarate (2HG) and a CpG island (CGI) hypermethylation phenotype (G-CIMP). To investigate the role of mutant IDH1 at recurrence, we performed a longitudinal analysis of 50 IDH1 mutant LGGs. We discovered six cases with copy number alterations (CNAs) at the IDH1 locus at recurrence. Deletion or amplification of IDH1 was followed by clonal expansion and recurrence at a higher grade. Successful cultures derived from IDH1 mutant, but not IDH1 wild type, gliomas systematically deleted IDH1 in vitro and in vivo, further suggestive of selection against the heterozygous mutant state as tumors progress. Tumors and cultures with IDH1 CNA had decreased 2HG, maintenance of G-CIMP, and DNA methylation reprogramming outside CGI. Thus, while IDH1 mutation initiates gliomagenesis, in some patients mutant IDH1 and 2HG are not required for later clonal expansions.

Published
2017

25. Method for Detecting Text Markers of Depression and Depressiveness

Author

Smirnov, Ivan V., Ushakova, Anastasiya V., Chudova, Natalya V., Goos, Gerhard, Founding Editor, Hartmanis, Juris, Founding Editor, Bertino, Elisa, Editorial Board Member, Gao, Wen, Editorial Board Member, Steffen, Bernhard, Editorial Board Member, Woeginger, Gerhard, Editorial Board Member, Yung, Moti, Editorial Board Member, Kuznetsov, Sergei O., editor, Panov, Aleksandr I., editor, and Yakovlev, Konstantin S., editor

Published
2020
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29. Genetic Variation Associated with Longer Telomere Length Increases Risk of Chronic Lymphocytic Leukemia

Author

Ojha, Juhi, Codd, Veryan, Nelson, Christopher P, Samani, Nilesh J, Smirnov, Ivan V, Madsen, Nils R, Hansen, Helen M, de Smith, Adam J, Bracci, Paige M, Wiencke, John K, Wrensch, Margaret R, Wiemels, Joseph L, and Walsh, Kyle M

Subjects
Biomedical and Clinical Sciences, Cancer, Genetics, Lymphoma, Rare Diseases, Hematology, Lymphatic Research, Human Genome, 2.1 Biological and endogenous factors, Adult, Aged, Biomarkers, Tumor, Case-Control Studies, Female, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Humans, Leukemia, Lymphocytic, Chronic, B-Cell, Leukocytes, Male, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Telomere Homeostasis, ENGAGE Consortium Telomere Group, Medical and Health Sciences, Epidemiology, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundChronic lymphocytic leukemia (CLL) is the most common leukemia in the Western world. Shorter mean telomere length in leukemic cells has been associated with more aggressive disease. Germline polymorphisms in telomere maintenance genes affect telomere length and may contribute to CLL susceptibility.MethodsWe collected genome-wide data from two groups of patients with CLL (N = 273) and two control populations (N = 5,725). In ancestry-adjusted case-control comparisons, we analyzed eight SNPs in genes definitively associated with inter-individual variation in leukocyte telomere length (LTL) in prior genome-wide association studies: ACYP2, TERC, NAF1, TERT, OBFC1, CTC1, ZNF208, and RTEL1 RESULTS: Three of the eight LTL-associated SNPs were associated with CLL risk at P < 0.05, including those near: TERC [OR, 1.46; 95% confidence interval (CI), 1.15-1.86; P = 1.8 × 10(-3)], TERT (OR = 1.23; 95% CI, 1.02-1.48; P = 0.030), and OBFC1 (OR, 1.36; 95% CI, 1.08-1.71; P = 9.6 × 10(-3)). Using a weighted linear combination of the eight LTL-associated SNPs, we observed that CLL patients were predisposed to longer LTL than controls in both case-control sets (P = 9.4 × 10(-4) and 0.032, respectively). CLL risk increased monotonically with increasing quintiles of the weighted linear combination.ConclusionsGenetic variants in TERC, TERT, and OBFC1 are associated with both longer LTL and increased CLL risk. Because the human CST complex competes with shelterin for telomeric DNA, future work should explore the role of OBFC1 and other CST complex genes in leukemogenesis.ImpactA genetic predisposition to longer telomere length is associated with an increased risk of CLL, suggesting that the role of telomere length in CLL etiology may be distinct from its role in disease progression. Cancer Epidemiol Biomarkers Prev; 25(7); 1043-9. ©2016 AACR.

Published
2016

30. Common genetic variants associated with telomere length confer risk for neuroblastoma and other childhood cancers

Author

Walsh, Kyle M, Whitehead, Todd P, de Smith, Adam J, Smirnov, Ivan V, Park, Minsun, Endicott, Alyson A, Francis, Stephen S, Codd, Veryan, Group, ENGAGE Consortium Telomere, Samani, Nilesh J, Metayer, Catherine, and Wiemels, Joseph L

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Human Genome, Pediatric, Orphan Drug, Prevention, Neuroblastoma, Cancer, Cancer Genomics, Neurosciences, Hematology, Childhood Leukemia, Pediatric Cancer, Rare Diseases, 2.1 Biological and endogenous factors, Adolescent, Bone Neoplasms, Case-Control Studies, Child, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Leukocytes, Osteosarcoma, Polymorphism, Single Nucleotide, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Proteins, Telomere Homeostasis, Young Adult, ENGAGE Consortium Telomere Group, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

Aberrant telomere lengthening is an important feature of cancer cells in adults and children. In addition to somatic mutations, germline polymorphisms in telomere maintenance genes impact telomere length. Whether these telomere-associated polymorphisms affect risk of childhood malignancies remains largely unexplored. We collected genome-wide data from three groups with pediatric malignancies [neuroblastoma (N = 1516), acute lymphoblastic leukemia (ALL) (N = 958) and osteosarcoma (N = 660)] and three control populations (N = 6892). Using case-control comparisons, we analyzed eight single nucleotide polymorphisms (SNPs) in genes definitively associated with interindividual variation in leukocyte telomere length (LTL) in prior genome-wide association studies: ACYP2, TERC, NAF1, TERT, OBFC1, CTC1, ZNF208 and RTEL1 Six of these SNPs were associated (P < 0.05) with neuroblastoma risk, one with leukemia risk and one with osteosarcoma risk. The allele associated with longer LTL increased cancer risk for all these significantly associated SNPs. Using a weighted linear combination of the eight LTL-associated SNPs, we observed that neuroblastoma patients were predisposed to longer LTL than controls, with each standard deviation increase in genotypically estimated LTL associated with a 1.15-fold increased odds of neuroblastoma (95%CI = 1.09-1.22; P = 7.9×10(-7)). This effect was more pronounced in adolescent-onset neuroblastoma patients (OR = 1.46; 95%CI = 1.03-2.08). A one standard deviation increase in genotypically estimated LTL was more weakly associated with osteosarcoma risk (OR = 1.10; 95%CI = 1.01-1.19; P = 0.017) and leukemia risk (OR = 1.07; 95%CI = 1.00-1.14; P = 0.044), specifically for leukemia patients who relapsed (OR = 1.19; 95%CI = 1.01-1.40; P = 0.043). These results indicate that genetic predisposition to longer LTL is a newly identified risk factor for neuroblastoma and potentially for other cancers of childhood.

Published
2016

31. Longer genotypically-estimated leukocyte telomere length is associated with increased adult glioma risk

Author

Walsh, Kyle M, Codd, Veryan, Rice, Terri, Nelson, Christopher P, Smirnov, Ivan V, McCoy, Lucie S, Hansen, Helen M, Elhauge, Edward, Ojha, Juhi, Francis, Stephen S, Madsen, Nils R, Bracci, Paige M, Pico, Alexander R, Molinaro, Annette M, Tihan, Tarik, Berger, Mitchel S, Chang, Susan M, Prados, Michael D, Jenkins, Robert B, Wiemels, Joseph L, Group, ENGAGE Consortium Telomere, Samani, Nilesh J, Wiencke, John K, and Wrensch, Margaret R

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Neurosciences, Rare Diseases, Prevention, Human Genome, Brain Cancer, Brain Disorders, Genetics, Cancer, Cancer Genomics, 2.1 Biological and endogenous factors, Generic health relevance, Adult, Brain Neoplasms, Case-Control Studies, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Genotype, Glioma, Humans, Leukocytes, Male, Models, Statistical, Polymorphism, Single Nucleotide, Risk Factors, Telomere, single nucleotide polymorphism, telomerase, telomere, CST complex, glioma, ENGAGE Consortium Telomere Group, Oncology and carcinogenesis
Abstract

Telomere maintenance has emerged as an important molecular feature with impacts on adult glioma susceptibility and prognosis. Whether longer or shorter leukocyte telomere length (LTL) is associated with glioma risk remains elusive and is often confounded by the effects of age and patient treatment. We sought to determine if genotypically-estimated LTL is associated with glioma risk and if inherited single nucleotide polymorphisms (SNPs) that are associated with LTL are glioma risk factors. Using a Mendelian randomization approach, we assessed differences in genotypically-estimated relative LTL in two independent glioma case-control datasets from the UCSF Adult Glioma Study (652 patients and 3735 controls) and The Cancer Genome Atlas (478 non-overlapping patients and 2559 controls). LTL estimates were based on a weighted linear combination of subject genotype at eight SNPs, previously associated with LTL in the ENGAGE Consortium Telomere Project. Mean estimated LTL was 31bp (5.7%) longer in glioma patients than controls in discovery analyses (P = 7.82x10-8) and 27bp (5.0%) longer in glioma patients than controls in replication analyses (1.48x10-3). Glioma risk increased monotonically with each increasing septile of LTL (O.R.=1.12; P = 3.83x10-12). Four LTL-associated SNPs were significantly associated with glioma risk in pooled analyses, including those in the telomerase component genes TERC (O.R.=1.14; 95% C.I.=1.03-1.28) and TERT (O.R.=1.39; 95% C.I.=1.27-1.52), and those in the CST complex genes OBFC1 (O.R.=1.18; 95% C.I.=1.05-1.33) and CTC1 (O.R.=1.14; 95% C.I.=1.02-1.28). Future work is needed to characterize the role of the CST complex in gliomagenesis and further elucidate the complex balance between ageing, telomere length, and molecular carcinogenesis.

Published
2015

32. A Heritable Missense Polymorphism in CDKN2A Confers Strong Risk of Childhood Acute Lymphoblastic Leukemia and Is Preferentially Selected during Clonal Evolution

Author

Walsh, Kyle M, de Smith, Adam J, Hansen, Helen M, Smirnov, Ivan V, Gonseth, Semira, Endicott, Alyson A, Xiao, Jianqiao, Rice, Terri, Fu, Cecilia H, McCoy, Lucie S, Lachance, Daniel H, Eckel-Passow, Jeanette E, Wiencke, John K, Jenkins, Robert B, Wrensch, Margaret R, Ma, Xiaomei, Metayer, Catherine, and Wiemels, Joseph L

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Cancer, Cancer Genomics, Human Genome, Orphan Drug, Pediatric Cancer, Hematology, Pediatric, Prevention, Rare Diseases, Childhood Leukemia, 2.1 Biological and endogenous factors, Case-Control Studies, Child, Evolution, Molecular, Female, Genes, p16, Genetic Predisposition to Disease, Genome-Wide Association Study, Genotype, Humans, Male, Polymorphism, Single Nucleotide, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Genome-wide association studies (GWAS) have identified SNPs in six genes that are associated with childhood acute lymphoblastic leukemia (ALL). A lead SNP was found to occur on chromosome 9p21.3, a region that is deleted in 30% of childhood ALLs, suggesting the presence of causal polymorphisms linked to ALL risk. We used SNP genotyping and imputation-based fine-mapping of a multiethnic ALL case-control population (Ncases = 1,464, Ncontrols = 3,279) to identify variants of large effect within 9p21.3. We identified a CDKN2A missense variant (rs3731249) with 2% allele frequency in controls that confers three-fold increased risk of ALL in children of European ancestry (OR, 2.99; P = 1.51 × 10(-9)) and Hispanic children (OR, 2.77; P = 3.78 × 10(-4)). Moreover, of 17 patients whose tumors displayed allelic imbalance at CDKN2A, 14 preferentially retained the risk allele and lost the protective allele (PBinomial = 0.006), suggesting that the risk allele provides a selective advantage during tumor growth. Notably, the CDKN2A variant was not significantly associated with melanoma, glioblastoma, or pancreatic cancer risk, implying that this polymorphism specifically confers ALL risk but not general cancer risk. Taken together, our findings demonstrate that coding polymorphisms of large effect can underlie GWAS "hits" and that inherited polymorphisms may undergo directional selection during clonal expansion of tumors.

Published
2015

33. DNA Methylation and Somatic Mutations Converge on the Cell Cycle and Define Similar Evolutionary Histories in Brain Tumors

Author

Mazor, Tali, Pankov, Aleksandr, Johnson, Brett E, Hong, Chibo, Hamilton, Emily G, Bell, Robert JA, Smirnov, Ivan V, Reis, Gerald F, Phillips, Joanna J, Barnes, Michael J, Idbaih, Ahmed, Alentorn, Agusti, Kloezeman, Jenneke J, Lamfers, Martine LM, Bollen, Andrew W, Taylor, Barry S, Molinaro, Annette M, Olshen, Adam B, Chang, Susan M, Song, Jun S, and Costello, Joseph F

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Brain Cancer, Rare Diseases, Cancer Genomics, Neurosciences, Cancer, Human Genome, Brain Disorders, Brain Neoplasms, DNA Methylation, Epigenesis, Genetic, G1 Phase Cell Cycle Checkpoints, Gene Expression Regulation, Neoplastic, Glioblastoma, Glioma, Humans, Mutation, Phylogeny, Promoter Regions, Genetic, Transcription, Genetic, Up-Regulation, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

The evolutionary history of tumor cell populations can be reconstructed from patterns of genetic alterations. In contrast to stable genetic events, epigenetic states are reversible and sensitive to the microenvironment, prompting the question whether epigenetic information can similarly be used to discover tumor phylogeny. We examined the spatial and temporal dynamics of DNA methylation in a cohort of low-grade gliomas and their patient-matched recurrences. Genes transcriptionally upregulated through promoter hypomethylation during malignant progression to high-grade glioblastoma were enriched in cell cycle function, evolving in parallel with genetic alterations that deregulate the G1/S cell cycle checkpoint. Moreover, phyloepigenetic relationships robustly recapitulated phylogenetic patterns inferred from somatic mutations. These findings highlight widespread co-dependency of genetic and epigenetic events throughout brain tumor evolution.

Published
2015

34. Glioma Groups Based on 1p/19q, IDH, and TERT Promoter Mutations in Tumors

Author

Eckel-Passow, Jeanette E, Lachance, Daniel H, Molinaro, Annette M, Walsh, Kyle M, Decker, Paul A, Sicotte, Hugues, Pekmezci, Melike, Rice, Terri, Kosel, Matt L, Smirnov, Ivan V, Sarkar, Gobinda, Caron, Alissa A, Kollmeyer, Thomas M, Praska, Corinne E, Chada, Anisha R, Halder, Chandralekha, Hansen, Helen M, McCoy, Lucie S, Bracci, Paige M, Marshall, Roxanne, Zheng, Shichun, Reis, Gerald F, Pico, Alexander R, O'Neill, Brian P, Buckner, Jan C, Giannini, Caterina, Huse, Jason T, Perry, Arie, Tihan, Tarik, Berger, Mitchell S, Chang, Susan M, Prados, Michael D, Wiemels, Joseph, Wiencke, John K, Wrensch, Margaret R, and Jenkins, Robert B

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Genetics, Clinical Research, Brain Disorders, Neurosciences, Brain Cancer, Rare Diseases, Cancer, 2.1 Biological and endogenous factors, 6.1 Pharmaceuticals, Adult, Age of Onset, Biomarkers, Tumor, Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 19, DNA Mutational Analysis, DNA, Neoplasm, Female, Germ-Line Mutation, Glioma, Humans, Isocitrate Dehydrogenase, Kaplan-Meier Estimate, Male, Middle Aged, Mutation, Neoplasm Grading, Promoter Regions, Genetic, Proportional Hazards Models, Telomerase, Medical and Health Sciences, General & Internal Medicine, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundThe prediction of clinical behavior, response to therapy, and outcome of infiltrative glioma is challenging. On the basis of previous studies of tumor biology, we defined five glioma molecular groups with the use of three alterations: mutations in the TERT promoter, mutations in IDH, and codeletion of chromosome arms 1p and 19q (1p/19q codeletion). We tested the hypothesis that within groups based on these features, tumors would have similar clinical variables, acquired somatic alterations, and germline variants.MethodsWe scored tumors as negative or positive for each of these markers in 1087 gliomas and compared acquired alterations and patient characteristics among the five primary molecular groups. Using 11,590 controls, we assessed associations between these groups and known glioma germline variants.ResultsAmong 615 grade II or III gliomas, 29% had all three alterations (i.e., were triple-positive), 5% had TERT and IDH mutations, 45% had only IDH mutations, 7% were triple-negative, and 10% had only TERT mutations; 5% had other combinations. Among 472 grade IV gliomas, less than 1% were triple-positive, 2% had TERT and IDH mutations, 7% had only IDH mutations, 17% were triple-negative, and 74% had only TERT mutations. The mean age at diagnosis was lowest (37 years) among patients who had gliomas with only IDH mutations and was highest (59 years) among patients who had gliomas with only TERT mutations. The molecular groups were independently associated with overall survival among patients with grade II or III gliomas but not among patients with grade IV gliomas. The molecular groups were associated with specific germline variants.ConclusionsGliomas were classified into five principal groups on the basis of three tumor markers. The groups had different ages at onset, overall survival, and associations with germline variants, which implies that they are characterized by distinct mechanisms of pathogenesis. (Funded by the National Institutes of Health and others.).

Published
2015

35. Gausemycin Antibiotic Family Acts via Ca2+-Dependent Membrane Targeting

Author

Kravchenko, Tatyana V., primary, Paramonov, Alexander S., additional, Kudzhaev, Arsen M., additional, Efimova, Svetlana S., additional, Khorev, Alexey S., additional, Kudryakova, Gulnara Kh., additional, Ivanov, Igor A., additional, Chistov, Alexey A., additional, Baranova, Anna A., additional, Krasilnikov, Maxim S., additional, Lapchinskaya, Olda A., additional, Tyurin, Anton P., additional, Ostroumova, Olga S., additional, Smirnov, Ivan V., additional, Terekhov, Stanislav S., additional, Dontsova, Olga A., additional, Shenkarev, Zakhar O., additional, Alferova, Vera A., additional, and Korshun, Vladimir A., additional

Published
2024
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36. Variants near TERT and TERC influencing telomere length are associated with high-grade glioma risk

Author

Walsh, Kyle M, Codd, Veryan, Smirnov, Ivan V, Rice, Terri, Decker, Paul A, Hansen, Helen M, Kollmeyer, Thomas, Kosel, Matthew L, Molinaro, Annette M, McCoy, Lucie S, Bracci, Paige M, Cabriga, Belinda S, Pekmezci, Melike, Zheng, Shichun, Wiemels, Joseph L, Pico, Alexander R, Tihan, Tarik, Berger, Mitchell S, Chang, Susan M, Prados, Michael D, Lachance, Daniel H, O'Neill, Brian Patrick, Sicotte, Hugues, Eckel-Passow, Jeanette E, van der Harst, Pim, Wiencke, John K, Samani, Nilesh J, Jenkins, Robert B, and Wrensch, Margaret R

Subjects
Agricultural, Veterinary and Food Sciences, Biological Sciences, Bioinformatics and Computational Biology, Genetics, Agricultural Biotechnology, Aging, Cancer, Brain Disorders, Brain Cancer, Prevention, Rare Diseases, Neurosciences, Adult, Case-Control Studies, Genome-Wide Association Study, Genotype, Glioma, Humans, Leukocytes, Neoplasm Grading, Polymorphism, Single Nucleotide, Prognosis, RNA, Risk Factors, Telomerase, Telomere, ENGAGE Consortium Telomere Group, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology
Abstract

Glioma, the most common central nervous system cancer in adults, has poor prognosis. Here we identify a new SNP associated with glioma risk, rs1920116 (near TERC), that reached genome-wide significance (Pcombined = 8.3 × 10(-9)) in a meta-analysis of genome-wide association studies (GWAS) of high-grade glioma and replication data (1,644 cases and 7,736 controls). This region has previously been associated with mean leukocyte telomere length (LTL). We therefore examined the relationship between LTL and both this new risk locus and other previously established risk loci for glioma using data from a recent GWAS of LTL (n = 37,684 individuals). Alleles associated with glioma risk near TERC and TERT were strongly associated with longer LTL (P = 5.5 × 10(-20) and 4.4 × 10(-19), respectively). In contrast, risk-associated alleles near RTEL1 were inconsistently associated with LTL, suggesting the presence of distinct causal alleles. No other risk loci for glioma were associated with LTL. The identification of risk alleles for glioma near TERC and TERT that also associate with telomere length implicates telomerase in gliomagenesis.

Published
2014

37. Molecular Basis of Influence of A501X Mutations in Penicillin-Binding Protein 2 of Neisseria gonorrhoeae Strain 35/02 on Ceftriaxone Resistance.

Author

Krivitskaya, Alexandra V., Kuryshkina, Maria S., Eremina, Maria Y., Smirnov, Ivan V., and Khrenova, Maria G.

Subjects
PENICILLIN-binding proteins, NEISSERIA gonorrhoeae, ACTIVATION energy, SCISSION (Chemistry), MOLECULAR dynamics
Abstract

The increase in the resistance of mutant strains of Neisseria gonorrhoeae to the antibiotic ceftriaxone is pronounced in the decrease in the second-order acylation rate constant, k2/KS, by penicillin-binding protein 2 (PBP2). These changes can be caused by both the decrease in the acylation rate constant, k2, and the weakening of the binding affinity, i.e., an increase in the substrate constant, KS. A501X mutations in PBP2 affect second-order acylation rate constants. The PBP2A501V variant exhibits a higher k2/KS value, whereas for PBP2A501R and PBP2A501P variants, these values are lower. We performed molecular dynamic simulations with both classical and QM/MM potentials to model both acylation energy profiles and conformational dynamics of four PBP2 variants to explain the origin of k2/KS changes. The acylation reaction occurs in two elementary steps, specifically, a nucleophilic attack by the oxygen atom of the Ser310 residue and C–N bond cleavage in the β-lactam ring accompanied by the elimination of the leaving group of ceftriaxone. The energy barrier of the first step increases for PBP2 variants with a decrease in the observed k2/KS value. Submicrosecond classic molecular dynamic trajectories with subsequent cluster analysis reveal that the conformation of the β3–β4 loop switches from open to closed and its flexibility decreases for PBP2 variants with a lower k2/KS value. Thus, the experimentally observed decrease in the k2/KS in A501X variants of PBP2 occurs due to both the decrease in the acylation rate constant, k2, and the increase in KS. [ABSTRACT FROM AUTHOR]

Published
2024
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39. Whole tumor analysis reveals early origin of the TERT promoter mutation and intercellular heterogeneity in TERT expression

Author

Appin, Christina L, primary, Hong, Chibo, additional, Suwala, Abigail K, additional, Hilz, Stephanie, additional, Mathur, Radhika, additional, Solomon, David A, additional, Smirnov, Ivan V, additional, Stevers, Nicholas O, additional, Shai, Anny, additional, Wang, Albert, additional, Berger, Mitchel S, additional, Chang, Susan M, additional, Phillips, Joanna J, additional, and Costello, Joseph F, additional

Published
2023
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41. Genetically encodable bioluminescent system from fungi

Author

Kotlobay, Alexey A., Sarkisyan, Karen S., Mokrushina, Yuliana A., Marcet-Houben, Marina, Serebrovskaya, Ekaterina O., Markina, Nadezhda M., Somermeyer, Louisa Gonzalez, Gorokhovatsky, Andrey Y., Vvedensky, Andrey, Purtov, Konstantin V., Petushkov, Valentin N., Rodionova, Natalja S., Chepurnyh, Tatiana V., Fakhranurova, Liliia I., Guglya, Elena B., Ziganshin, Rustam, Tsarkova, Aleksandra S., Kaskova, Zinaida M., Shender, Victoria, Abakumov, Maxim, Abakumova, Tatiana O., Povolotskaya, Inna S., Eroshkin, Fedor M., Zaraisky, Andrey G., Mishin, Alexander S., Dolgov, Sergey V., Mitiouchkina, Tatiana Y., Kopantzev, Eugene P., Waldenmaier, Hans E., Oliveira, Anderson G., Oba, Yuichi, Barsova, Ekaterina, Bogdanova, Ekaterina A., Gabaldón, Toni, Stevani, Cassius V., Lukyanov, Sergey, Smirnov, Ivan V., Gitelson, Josef I., Kondrashov, Fyodor A., and Yampolsky, Ilia V.

Published
2018

42. Ultrahigh-throughput functional profiling of microbiota communities

Author

Terekhov, Stanislav S., Smirnov, Ivan V., Malakhova, Maja V., Samoilov, Andrei E., Manolov, Alexander I., Nazarov, Anton S., Danilov, Dmitry V., Dubiley, Svetlana A., Osterman, Ilya A., Rubtsova, Maria P., Kostryukova, Elena S., Ziganshin, Rustam H., Kornienko, Maria A., Vanyushkina, Anna A., Bukato, Olga N., Ilina, Elena N., Vlasov, Valentin V., Severinov, Konstantin V., Gabibov, Alexander G., and Altman, Sidney

Published
2018

43. Mutational Analysis Reveals the Origin and Therapy-Driven Evolution of Recurrent Glioma

Author

Johnson, Brett E, Mazor, Tali, Hong, Chibo, Barnes, Michael, Aihara, Koki, McLean, Cory Y, Fouse, Shaun D, Yamamoto, Shogo, Ueda, Hiroki, Tatsuno, Kenji, Asthana, Saurabh, Jalbert, Llewellyn E, Nelson, Sarah J, Bollen, Andrew W, Gustafson, W Clay, Charron, Elise, Weiss, William A, Smirnov, Ivan V, Song, Jun S, Olshen, Adam B, Cha, Soonmee, Zhao, Yongjun, Moore, Richard A, Mungall, Andrew J, Jones, Steven JM, Hirst, Martin, Marra, Marco A, Saito, Nobuhito, Aburatani, Hiroyuki, Mukasa, Akitake, Berger, Mitchel S, Chang, Susan M, Taylor, Barry S, and Costello, Joseph F

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Human Genome, Brain Cancer, Neurosciences, Brain Disorders, Orphan Drug, Genetics, Cancer, Rare Diseases, Cancer Genomics, Good Health and Well Being, Antineoplastic Agents, Alkylating, Brain, Brain Neoplasms, DNA Helicases, DNA Mutational Analysis, Dacarbazine, Glioma, Humans, Mutagenesis, Neoplasm Grading, Neoplasm Recurrence, Local, Nuclear Proteins, Proto-Oncogene Proteins B-raf, Proto-Oncogene Proteins c-akt, TOR Serine-Threonine Kinases, Temozolomide, Transcription Factors, Tumor Suppressor Protein p53, X-linked Nuclear Protein, General Science & Technology
Abstract

Tumor recurrence is a leading cause of cancer mortality. Therapies for recurrent disease may fail, at least in part, because the genomic alterations driving the growth of recurrences are distinct from those in the initial tumor. To explore this hypothesis, we sequenced the exomes of 23 initial low-grade gliomas and recurrent tumors resected from the same patients. In 43% of cases, at least half of the mutations in the initial tumor were undetected at recurrence, including driver mutations in TP53, ATRX, SMARCA4, and BRAF; this suggests that recurrent tumors are often seeded by cells derived from the initial tumor at a very early stage of their evolution. Notably, tumors from 6 of 10 patients treated with the chemotherapeutic drug temozolomide (TMZ) followed an alternative evolutionary path to high-grade glioma. At recurrence, these tumors were hypermutated and harbored driver mutations in the RB (retinoblastoma) and Akt-mTOR (mammalian target of rapamycin) pathways that bore the signature of TMZ-induced mutagenesis.

Published
2014

44. Mn-catalyzed syngas-assisted reductive Knoevenagel condensation.

Author

Smirnov, Ivan V., Afanasyev, Oleg I., Biriukov, Klim O., Godovikova, Maria I., and Chusov, Denis A.

Subjects
*CHEMICAL reactions, *PHARMACEUTICAL chemistry, *REDUCING agents, *BIOCHEMICAL substrates, *SYNTHESIS gas
Abstract

[Display omitted] Arene manganese π-complex was applied as a catalyst for the reductive Knoevenagel condensation. Syngas was used as a selective synergistic reducing agent providing the possibility to use 3d metal-based catalyst in such process. Demonstrated substrate scope indicates a high potential for this reaction in a medicinal chemistry. [ABSTRACT FROM AUTHOR]

Published
2024
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46. Microfluidic droplet platform for ultrahigh-throughput single-cell screening of biodiversity

Author

Terekhov, Stanislav S., Smirnov, Ivan V., Stepanova, Anastasiya V., Bobik, Tatyana V., Mokrushina, Yuliana A., Ponomarenko, Natalia A., Belogurov, Alexey A., Rubtsova, Maria P., Kartseva, Olga V., Gomzikova, Marina O., Moskovtsev, Alexey A., Bukatin, Anton S., Dubina, Michael V., Kostryukova, Elena S., Babenko, Vladislav V., Vakhitova, Maria T., Manolov, Alexander I., Malakhova, Maja V., Kornienko, Maria A., Tyakht, Alexander V., Vanyushkina, Anna A., Ilina, Elena N., Masson, Patrick, Gabibov, Alexander G., and Altman, Sidney

Published
2017

47. SNPLogic: an interactive single nucleotide polymorphism selection, annotation, and prioritization system

Author

Pico, Alexander R, Smirnov, Ivan V, Chang, Jeffrey S, Yeh, Ru-Fang, Wiemels, Joseph L, Wiencke, John K, Tihan, Tarik, Conklin, Bruce R, and Wrensch, Margaret

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Genetics, Networking and Information Technology R&D (NITRD), Human Genome, 1.5 Resources and infrastructure (underpinning), Generic health relevance, Databases, Nucleic Acid, Disease, Gene Frequency, Genes, Genotype, Humans, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide, User-Computer Interface, Environmental Sciences, Information and Computing Sciences, Developmental Biology, Biological sciences, Chemical sciences, Environmental sciences
Abstract

SNPLogic (http://www.snplogic.org) brings together single nucleotide polymorphism (SNP) information from numerous sources to provide a comprehensive SNP selection, annotation and prioritization system for design and analysis of genotyping projects. SNPLogic integrates information about the genetic context of SNPs (gene, chromosomal region, functional location, haplotypes tags and overlap with transcription factor binding sites, splicing sites, miRNAs and evolutionarily conserved regions), genotypic data (allele frequencies per population and validation method), coverage of commercial arrays (ParAllele, Affymetrix and Illumina), functional predictions (modeled on structure and sequence) and connections or established associations (biological pathways, gene ontology terms and OMIM disease terms). The SNPLogic web interface facilitates construction and annotation of user-defined SNP lists that can be saved, shared and exported. Thus, SNPLogic can be used to identify and prioritize candidate SNPs, assess custom and commercial arrays panels and annotate new SNP data with publicly available information. We have found integration of SNP annotation in the context of pathway information and functional prediction scores to be a powerful approach to the analysis and interpretation of SNP-disease association data.

Published
2009

48. Air-Stable Arene Manganese Complexes as Catalysts for the Syngas-Assisted Direct Reductive Amination, Cyanation of Aldehyde, and CO2Fixation by Epoxide with High Functional Groups Tolerance

Author

Smirnov, Ivan V., Biriukov, Klim O., Shvydkiy, Nikita V., Perekalin, Dmitry S., Afanasyev, Oleg I., and Chusov, Denis

Abstract

Manganese complexes [(arene)Mn(CO)3]+were prepared in one step from arenes and Mn(CO)5Br. They were found to be efficient catalysts in the carbonyl cyanation with TMSCN, CO2fixation by epoxides, and direct reductive amination in the presence of syngas. The amination reaction tolerated various reducible functional groups. The synergy of carbon monoxide and hydrogen in syngas provides high efficiency of the catalytic system. The developed protocols do not require an inert atmosphere, and the catalysts can be handled in air.

Published
2024
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