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1. Elevation of Donor-derived Cell-free DNA Before Biopsy-proven Rejection in Kidney Transplant.

Author

Bromberg, Jonathan, Bunnapradist, Suphamai, Samaniego-Picota, Milagros, Anand, Sanjiv, Stites, Erik, Gauthier, Philippe, Demko, Zachary, Prewett, Adam, Armer-Cabral, Madeleine, Marshall, Kyle, Kaur, Navchetan, Bloom, Michelle, Tabriziani, Hossein, Bhorade, Sangeeta, and Cooper, Matthew

Subjects
Humans, Kidney Transplantation, Graft Rejection, Cell-Free Nucleic Acids, Male, Female, Middle Aged, Retrospective Studies, Biopsy, Biomarkers, Adult, Tissue Donors, Kidney, Registries, Creatinine, Aged, Time Factors, Predictive Value of Tests, Prospective Studies
Abstract

BACKGROUND: Standard-of-care biomarkers for renal allograft rejection are lagging indicators, signaling existing organ injury. This precludes early intervention, when immunological cascades leading to rejection are most susceptible. Donor-derived cell-free DNA (dd-cfDNA) shows promise as an early indicator of rejection, allowing earlier and possibly more effective treatment. This analysis was designed to assess this promise using real-world dd-cfDNA testing evidence. METHODS: This retrospective analysis of the prospective, observational ProActive registry study (NCT04091984) assessed dd-cfDNA and serum creatinine levels before biopsy in 424 patients with ≥1 dd-cfDNA test (n = 1013) in the 6 mo before biopsy. RESULTS: Of 4667 enrolled patients, 1631 patients had ≥18 mo of follow-up data, of which 424 had a biopsy and were included in this analysis. Twenty-six biopsies showed antibody-mediated rejection (ABMR), 62 showed T cell-mediated rejection, and 336 showed nonrejection; each from a unique patient. dd-cfDNA fractions were significantly elevated 5 mo before ABMR biopsies, and 2 mo before T cell-mediated rejection biopsies, compared with nonrejection biopsies. In contrast, serum creatinine did not discriminate between rejection and nonrejection in advance, or concurrent with biopsy. Among patients with nonrejection biopsies, estimated glomerular filtration rate was significantly lower in cases with ≥2 increased dd-cfDNA results (≥1%), compared with those with 0 or 1 increased dd-cfDNA result. CONCLUSIONS: These data indicate that dd-cfDNA is an early indicator of biopsy-proven rejection, especially ABMR, suggesting a greater role for dd-cfDNA in surveillance to identify patients at high risk of ongoing or future rejection, thus requiring closer monitoring, biopsy, or other management changes.

Published
2024

2. A novel donor-derived cell-free DNA assay for the detection of acute rejection in heart transplantation

Author

Kim, Paul J, Olymbios, Michael, Siu, Alfonso, Pinzon, Omar Wever, Adler, Eric, Liang, Nathan, Swenerton, Ryan, Sternberg, Jonathan, Kaur, Navchetan, Ahmed, Ebad, Chen, Yen-An, Fehringer, Gordon, Demko, Zachary P, Billings, Paul R, and Stehlik, Josef

Subjects
Organ Transplantation, Cardiovascular, Transplantation, Clinical Research, Adult, Biomarkers, Cell-Free Nucleic Acids, Graft Rejection, Heart Transplantation, Humans, Tissue Donors, acute rejection, heart transplant, cell free DNA, endomyocardial biopsy, acute cellular rejection, antibody mediated rejection, graft dysfunction, Cardiorespiratory Medicine and Haematology, Surgery
Abstract

BackgroundEndomyocardial biopsy (EMB), the reference surveillance test for acute rejection (AR) in heart transplant (HTx) recipients, is invasive, costly, and shows significant interobserver variability. Recent studies indicate that donor-derived cell-free DNA (dd-cfDNA), obtained non-invasively from blood, is associated with AR and could reduce the frequency of EMB surveillance. The aim of this study was to examine the performance characteristics of a novel test for detecting AR in adult HTx recipients.MethodsPlasma samples with contemporaneous EMBs were obtained from HTx recipients. A clinically available SNP-based massively multiplexed-PCR dd-cfDNA assay was used to measure dd-cfDNA fraction. dd-cfDNA fractions were compared with EMB-defined rejection status and test performance was assessed by constructing ROC curves and calculating accuracy measures.ResultsA total of 811 samples from 223 patients with dd-cfDNA testing and contemporaneous EMB were eligible for the study. dd-cfDNA fraction was significantly higher in AR (median 0.58%, IQR, 0.13%-1.68%) compared to non-AR (median 0.04%, IQR, 0.01%-0.11%, pc < 0.001). ROC analysis produced an area under the curve (AUC-ROC) of 0.86 (95% CI, 0.77-0.96). Defining samples with dd-cfDNA fraction ≥0.15% as AR yielded 78.5% sensitivity (95% CI, 60.7%-96.3%) and 76.9% specificity (95% CI, 71.1%-82.7%). Positive and negative predictive values were 25.1% (95% CI, 18.8%-31.5%) and 97.3% (95% CI, 95.1%-99.5%) respectively, calculated using the cohort AR prevalence of 9.0% (95% CI, 5.3%-12.8%) with adjustment for repeat samples.ConclusionsThis novel dd-cfDNA test detects AR in HTx recipients with good accuracy and holds promise as a noninvasive test for AR in HTx recipients.

Published
2022

4. Distinct Molecular Processes Mediate Donor-derived Cell-free DNA Release From Kidney Transplants in Different Disease States

Author

Gauthier, Patrick T., Madill-Thomsen, Katelynn S., Demko, Zachary, Prewett, Adam, Gauthier, Philippe, Halloran, Philip F., Fryc, Justyna, Naumnik, Beata, Bromberg, Jonathan, Weir, Matt, Costa, Nadiesa, Brennan, Daniel, Kant, Sam, Viswanathan, Vignesh, Samaniego-Picota, Milagros, Francis, Iman, Patel, Anita, Dębska-Ślizień, Alicja, Konopa, Joanna, Chamienia, Andrzej, Więcek, Andrzej, Piecha, Grzegorz, Veceric-Haler, Željka, Arnol, Miha, Kojc, Nika, Glyda, Maciej, Smykal-Jankowiak, Katarzyna, Viklicky, Ondrej, Hruba, Petra, Bloudíčkova, Silvie Rajnochová, Slatinská, Janka, Miglinas, Marius, Myślak, Marek, Mazurkiewicz, Joanna, Gryczman, Marta, Domański, Leszek, Kamel, Mahmoud, Perkowska-Ptasińska, Agnieszka, Dęborska-Materkowska, Dominika, Ciszek, Michal, Durlik, Magdalena, Grenda, Ryszard, Banasik, Miroslaw, Knotek, Mladen, Vucur, Ksenija, Jurekovic, Zeljka, Müller, Thomas, Schachtner, Thomas, Malone, Andrew, Alhamad, Tarek, Jittirat, Arksarapuk, Poggio, Emilio, Fatica, Richard, Zaky, Ziad, Chow, Kevin, Hughes, Peter, Anand, Sanjiv, Gupta, Gaurav, Kamal, Layla, Kumar, Dhiren, Moinuddin, Irfan, and Bobba., Sindhura

Published
2024
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6. The Clinical Utility of Genetic Testing in the Diagnosis and Management of Adults with Chronic Kidney Disease

Author

Dahl, Neera K., Bloom, Michelle S., Chebib, Fouad T., Clark, Dinah, Westemeyer, Maggie, Jandeska, Sara, Zhang, Zhiji, Milo-Rasouly, Hila, Kolupaeva, Victoria, Marasa, Maddalena, Broumand, Varshasb, Fatica, Richard A., Raj, Dominic S., Demko, Zachary P., Marshall, Kyle, Punj, Sumit, Tabriziani, Hossein, Bhorade, Sangeeta, and Gharavi, Ali G.

Published
2023
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7. Performance of prenatal cfDNA screening for sex chromosomes

Author

Martin, Kimberly, Dar, Pe’er, MacPherson, Cora, Egbert, Melissa, Demko, Zachary, Parmar, Sheetal, Hashimoto, Katelyn, Haeri, Sina, Malone, Fergal, Wapner, Ronald J., Roman, Ashley S., Khalil, Asma, Faro, Revital, Madankumar, Rajeevi, Strong, Noel, Silver, Robert M., Vohra, Nidhi, Hyett, Jon, Rabinowitz, Matt, Kao, Charlly, Hakonarson, Hakon, Jacobsson, Bo, and Norton, Mary E.

Published
2023
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8. Cell‐free DNA fetal fraction in twin gestations in single‐nucleotide polymorphism‐based noninvasive prenatal screening

Author

Hedriana, Herman, Martin, Kimberly, Saltzman, Daniel, Billings, Paul, Demko, Zachary, and Benn, Peter

Subjects
Reproductive Medicine, Biomedical and Clinical Sciences, Genetics, Pediatric, Perinatal Period - Conditions Originating in Perinatal Period, Clinical Research, Reproductive health and childbirth, Adult, Aneuploidy, Cell-Free Nucleic Acids, Female, Humans, Noninvasive Prenatal Testing, Pregnancy, Pregnancy, Twin, Twins, Dizygotic, Twins, Monozygotic, Clinical Sciences, Paediatrics and Reproductive Medicine, Obstetrics & Reproductive Medicine, Clinical sciences, Reproductive medicine
Abstract

ObjectivesThe performance of noninvasive prenatal screening (NIPS) for fetal aneuploidy in twin pregnancies is dependent on the amount of placentally derived cell-free DNA, the "fetal fraction (FF)," present in maternal plasma. We report FF values in monozygotic (MZ) and dizygotic (DZ) pregnancies.MethodsWe reviewed FF in pregnancies at 10 to 20 completed weeks gestational age based on single-nucleotide polymorphism (SNP)-based NIPS where zygosity was routinely established in twin pregnancies. The cohort included 121 446 (96.3%) singleton, 1454 (1.2%) MZ, and 3161 (2.5%) DZ pregnancies. For DZ twins, individual FFs were measured.ResultsCombined FF for DZ and MZ fetuses were 35% and 26% greater than singletons, respectively. The individual FF contributions from each fetus in DZ twins were, on average, 32% less than singletons. FF in DZ twin pairs were moderately correlated (Pearson correlation coefficient.66). When a threshold of 2.8% FF was applied to define uninterpretable results, 1.7% (2102/121 446) of singletons, 0.8% (11/1454) of MZ pairs, and 5.6% (178/3161) of DZ pairs were uninterpretable.ConclusionFor optimal aneuploidy NIPS in twin pregnancies, zygosity should be established and in DZ twins FF for both fetuses should be determined to identify those cases where results can be reliably interpreted.

Published
2020

9. The role of cell-free DNA biomarkers and patient data in the early prediction of preeclampsia: an artificial intelligence model

Author

Khalil, Asma, Bellesia, Giovanni, Norton, Mary E., Jacobsson, Bo, Haeri, Sina, Egbert, Melissa, Malone, Fergal D., Wapner, Ronald J., Roman, Ashley, Faro, Revital, Madankumar, Rajeevi, Strong, Noel, Silver, Robert M., Vohra, Nidhi, Hyett, Jon, MacPherson, Cora, Prigmore, Brittany, Ahmed, Ebad, Demko, Zachary, Ortiz, J. Bryce, Souter, Vivienne, and Dar, Pe’er

Published
2024
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10. Validation of a Single-Nucleotide Polymorphism-Based Non-Invasive Prenatal Test in Twin Gestations: Determination of Zygosity, Individual Fetal Sex, and Fetal Aneuploidy.

Author

Norwitz, Errol R, McNeill, Gabriel, Kalyan, Akshita, Rivers, Elizabeth, Ahmed, Ebad, Meng, Ling, Vu, Phikhanh, Egbert, Melissa, Shapira, Marlene, Kobara, Katie, Parmar, Sheetal, Goel, Shruti, Prins, Sarah A, Aruh, Israel, Persico, Nicola, Robins, Jared C, Kirshon, Brian, Demko, Zachary P, Ryan, Allison, Billings, Paul R, Rabinowitz, Matthew, Benn, Peter, Martin, Kimberly A, and Hedriana, Herman L

Subjects
Down syndrome, aneuploidy, chorionicity, non-invasive prenatal testing, prenatal screening, twins, zygosity, Clinical Sciences
Abstract

We analyzed maternal plasma cell-free DNA samples from twin pregnancies in a prospective blinded study to validate a single-nucleotide polymorphism (SNP)-based non-invasive prenatal test (NIPT) for zygosity, fetal sex, and aneuploidy. Zygosity was evaluated by looking for either one or two fetal genome complements, fetal sex was evaluated by evaluating Y-chromosome loci, and aneuploidy was assessed through SNP ratios. Zygosity was correctly predicted in 100% of cases (93/93; 95% confidence interval (CI) 96.1%-100%). Individual fetal sex for both twins was also called with 100% accuracy (102/102; 95% weighted CI 95.2%-100%). All cases with copy number truth were also correctly identified. The dizygotic aneuploidy sensitivity was 100% (10/10; 95% CI 69.2%-100%), and overall specificity was 100% (96/96; 95% weighted CI, 94.8%-100%). The mean fetal fraction (FF) of monozygotic twins (n = 43) was 13.0% (standard deviation (SD), 4.5%); for dizygotic twins (n = 79), the mean lower FF was 6.5% (SD, 3.1%) and the mean higher FF was 8.1% (SD, 3.5%). We conclude SNP-based NIPT for zygosity is of value when chorionicity is uncertain or anomalies are identified. Zygosity, fetal sex, and aneuploidy are complementary evaluations that can be carried out on the same specimen as early as 9 weeks' gestation.

Published
2019

11. Optimizing Detection of Kidney Transplant Injury by Assessment of Donor-Derived Cell-Free DNA via Massively Multiplex PCR

Author

Sigdel, Tara K, Archila, Felipe Acosta, Constantin, Tudor, Prins, Sarah A, Liberto, Juliane, Damm, Izabella, Towfighi, Parhom, Navarro, Samantha, Kirkizlar, Eser, Demko, Zachary P, Ryan, Allison, Sigurjonsson, Styrmir, Sarwal, Reuben D, Hseish, Szu-Chuan, Chan-On, Chitranon, Zimmermann, Bernhard, Billings, Paul R, Moshkevich, Solomon, and Sarwal, Minnie M

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Kidney Disease, Organ Transplantation, Transplantation, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Renal and urogenital, cfDNA, kidney transplantation, rejection, Biomedical and clinical sciences
Abstract

Standard noninvasive methods for detecting renal allograft rejection and injury have poor sensitivity and specificity. Plasma donor-derived cell-free DNA (dd-cfDNA) has been reported to accurately detect allograft rejection and injury in transplant recipients and shown to discriminate rejection from stable organ function in kidney transplant recipients. This study used a novel single nucleotide polymorphism (SNP)-based massively multiplexed PCR (mmPCR) methodology to measure dd-cfDNA in various types of renal transplant recipients for the detection of allograft rejection/injury without prior knowledge of donor genotypes. A total of 300 plasma samples (217 biopsy-matched: 38 with active rejection (AR), 72 borderline rejection (BL), 82 with stable allografts (STA), and 25 with other injury (OI)) were collected from 193 unique renal transplant patients; dd- cfDNA was processed by mmPCR targeting 13,392 SNPs. Median dd-cfDNA was significantly higher in samples with biopsy-proven AR (2.3%) versus BL (0.6%), OI (0.7%), and STA (0.4%) (p < 0.0001 all comparisons). The SNP-based dd-cfDNA assay discriminated active from non-rejection status with an area under the curve (AUC) of 0.87, 88.7% sensitivity (95% CI, 77.7⁻99.8%) and 72.6% specificity (95% CI, 65.4⁻79.8%) at a prespecified cutoff (>1% dd-cfDNA). Of 13 patients with AR findings at a routine protocol biopsy six-months post transplantation, 12 (92%) were detected positive by dd-cfDNA. This SNP-based dd-cfDNA assay detected allograft rejection with superior performance compared with the current standard of care. These data support the feasibility of using this assay to detect disease prior to renal failure and optimize patient management in the case of allograft injury.

Published
2019

12. Optimizing Detection of Kidney Transplant Injury by Assessment of Donor-Derived Cell-Free DNA via Massively Multiplex PCR.

Author

Sigdel, Tara K, Archila, Felipe Acosta, Constantin, Tudor, Prins, Sarah A, Liberto, Juliane, Damm, Izabella, Towfighi, Parhom, Navarro, Samantha, Kirkizlar, Eser, Demko, Zachary P, Ryan, Allison, Sigurjonsson, Styrmir, Sarwal, Reuben D, Hseish, Szu-Chuan, Chan-On, Chitranon, Zimmermann, Bernhard, Billings, Paul R, Moshkevich, Solomon, and Sarwal, Minnie M

Subjects
cfDNA, kidney transplantation, rejection, Organ Transplantation, Transplantation, Kidney Disease, 4.1 Discovery and preclinical testing of markers and technologies, Renal and urogenital, Clinical Sciences
Abstract

Standard noninvasive methods for detecting renal allograft rejection and injury have poor sensitivity and specificity. Plasma donor-derived cell-free DNA (dd-cfDNA) has been reported to accurately detect allograft rejection and injury in transplant recipients and shown to discriminate rejection from stable organ function in kidney transplant recipients. This study used a novel single nucleotide polymorphism (SNP)-based massively multiplexed PCR (mmPCR) methodology to measure dd-cfDNA in various types of renal transplant recipients for the detection of allograft rejection/injury without prior knowledge of donor genotypes. A total of 300 plasma samples (217 biopsy-matched: 38 with active rejection (AR), 72 borderline rejection (BL), 82 with stable allografts (STA), and 25 with other injury (OI)) were collected from 193 unique renal transplant patients; dd- cfDNA was processed by mmPCR targeting 13,392 SNPs. Median dd-cfDNA was significantly higher in samples with biopsy-proven AR (2.3%) versus BL (0.6%), OI (0.7%), and STA (0.4%) (p < 0.0001 all comparisons). The SNP-based dd-cfDNA assay discriminated active from non-rejection status with an area under the curve (AUC) of 0.87, 88.7% sensitivity (95% CI, 77.7⁻99.8%) and 72.6% specificity (95% CI, 65.4⁻79.8%) at a prespecified cutoff (>1% dd-cfDNA). Of 13 patients with AR findings at a routine protocol biopsy six-months post transplantation, 12 (92%) were detected positive by dd-cfDNA. This SNP-based dd-cfDNA assay detected allograft rejection with superior performance compared with the current standard of care. These data support the feasibility of using this assay to detect disease prior to renal failure and optimize patient management in the case of allograft injury.

Published
2018

15. Accuracy of fetal fraction measurements in a single‐nucleotide polymorphism‐based noninvasive prenatal test.

Author

Benn, Peter, Zhang, Jingwen, Lyons, Daniel, Xu, Wenbo, Leonard, Samantha, and Demko, Zachary

Abstract

Background: Noninvasive prenatal testing (NIPT) for fetal aneuploidy relies on the analysis of fetoplacental cell‐free DNA (cfDNA) found in maternal plasma. A minimum cfDNA fetal fraction (FF) is required for reliable test performance, but some methods may have suboptimal accuracy for FF measurement. This study investigated the accuracy of a single‐nucleotide polymorphism‐ (SNP‐) based NIPT method to assess FF. Methods: FF measurements using SNP‐based NIPT in consecutive samples from singleton male pregnancies were compared with FF measured using a "gold standard" Y‐chromosome method. Results: In a cohort of 106,846 samples, the SNP‐based FF method showed a standard deviation (SD) of 0.42%. Compared to the Y chromosome FF method, a correlation coefficient, r, of 0.995, and bias of 0.17% were observed. The SD was not substantially different across specific FF ranges or for samples with high‐risk NIPT results. Conclusions: The SNP‐based NIPT method estimates FF with good accuracy, with a SD three to eight times better than other NIPT methods (0.42% vs. 1.3%–3.4%). FF is an important quality control parameter and should be routinely reported as part of NIPT. Key points: What's already known about this topic?An adequate fetal fraction (FF) is an essential pre‐requisite for noninvasive prenatal testing (NIPT).Various methods have been developed to measure FF.The accuracy of these methods has been assessed by comparing results with those obtained for the Y‐chromosome when there is a male fetus. What does this study add?The accuracy of FF measurement was assessed for SNP‐based NIPT.FF measurements showed a higher level of accuracy than previously reported for other NIPTs. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Tripolar chromosome segregation drives the association between maternal genotype at variants spanning PLK4 and aneuploidy in human preimplantation embryos

Author

McCoy, Rajiv C, Newnham, Louise J, Ottolini, Christian S, Hoffmann, Eva R, Chatzimeletiou, Katerina, Cornejo, Omar E, Zhan, Qiansheng, Zaninovic, Nikica, Rosenwaks, Zev, Petrov, Dmitri A, Demko, Zachary P, Sigurjonsson, Styrmir, and Handyside, Alan H

Subjects
Biological Sciences, Genetics, 2.1 Biological and endogenous factors, Aetiology, Adolescent, Adult, Aneuploidy, Blastocyst, Blastomeres, Chromosome Segregation, Female, Genetic Testing, Genetic Variation, Genotype, Humans, Karyotype, Maternal Age, Middle Aged, Mitosis, Oogenesis, Pregnancy, Protein Serine-Threonine Kinases, Spindle Apparatus, Medical and Health Sciences, Genetics & Heredity
Abstract

Aneuploidy is prevalent in human embryos and is the leading cause of pregnancy loss. Many aneuploidies arise during oogenesis, increasing with maternal age. Superimposed on these meiotic aneuploidies are frequent errors occurring during early mitotic divisions, contributing to widespread chromosomal mosaicism. Here we reanalyzed a published dataset comprising preimplantation genetic testing for aneuploidy in 24 653 blastomere biopsies from day-3 cleavage-stage embryos, as well as 17 051 trophectoderm biopsies from day-5 blastocysts. We focused on complex abnormalities that affected multiple chromosomes simultaneously, seeking insights into their formation. In addition to well-described patterns such as triploidy and haploidy, we identified 4.7% of blastomeres possessing characteristic hypodiploid karyotypes. We inferred this signature to have arisen from tripolar chromosome segregation in normally fertilized diploid zygotes or their descendant diploid cells. This could occur via segregation on a tripolar mitotic spindle or by rapid sequential bipolar mitoses without an intervening S-phase. Both models are consistent with time-lapse data from an intersecting set of 77 cleavage-stage embryos, which were enriched for the tripolar signature among embryos exhibiting abnormal cleavage. The tripolar signature was strongly associated with common maternal genetic variants spanning the centrosomal regulator PLK4, driving the association we previously reported with overall mitotic errors. Our findings are consistent with the known capacity of PLK4 to induce tripolar mitosis or precocious M-phase upon dysregulation. Together, our data support tripolar chromosome segregation as a key mechanism generating complex aneuploidy in cleavage-stage embryos and implicate maternal genotype at a quantitative trait locus spanning PLK4 as a factor influencing its occurrence.

Published
2018

18. Obstetrical, Perinatal, and Genetic Outcomes Associated With Nonreportable Prenatal Cell-Free DNA Screening Results

Author

Norton, Mary E., primary, MacPherson, Cora, additional, Demko, Zachary, additional, Egbert, Melissa, additional, Malone, Fergal, additional, Wapner, Ronald J., additional, Roman, Ashley S., additional, Khalil, Asma, additional, Faro, Revital, additional, Madankumar, Rajeevi, additional, Strong, Noel, additional, Haeri, Sina, additional, Silver, Robert, additional, Vohra, Nidhi, additional, Hyett, Jon, additional, Martin, Kimberly, additional, Rabinowitz, Matthew, additional, Jacobsson, Bo, additional, and Dar, Pe'er, additional

Published
2024
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24. Impact of high‐risk prenatal screening results for 22q11.2 deletion syndrome on obstetric and neonatal management: Secondary analysis from the SMART study

Author

Martin, Kimberly, primary, Norton, Mary E., additional, MacPherson, Cora, additional, Demko, Zachary, additional, Egbert, Melissa, additional, Haeri, Sina, additional, Malone, Fergal, additional, Wapner, Ronald J., additional, Roman, Ashley S., additional, Khalil, Asma, additional, Faro, Revital, additional, Madankumar, Rajeevi, additional, Strong, Noel, additional, Silver, Robert, additional, Vohra, Nidhi, additional, Hyett, Jon, additional, Kao, Charlly, additional, Hakonarson, Hakon, additional, Jacobson, Bo, additional, and Dar, Pe'er, additional

Published
2023
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25. Impact of Circulating Tumor DNA–Based Detection of Molecular Residual Disease on the Conduct and Design of Clinical Trials for Solid Tumors

Author

Kasi, Pashtoon M., Fehringer, Gordon, Taniguchi, Hiroya, Starling, Naureen, Nakamura, Yoshiaki, Kotani, Daisuke, Powles, Thomas, Li, Bob T., Pusztai, Lajos, Aushev, Vasily N., Kalashnikova, Ekaterina, Sharma, Shruti, Malhotra, Meenakshi, Demko, Zachary P., Aleshin, Alexey, Rodriguez, Angel, Billings, Paul R., Grothey, Axel, Taieb, Julien, Cunningham, David, Yoshino, Takayuki, and Kopetz, Scott

Published
2022
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29. Cell-free DNA screening for trisomies 21, 18, and 13 in pregnancies at low and high risk for aneuploidy with genetic confirmation

Author

Dar, Pe’er, Jacobsson, Bo, MacPherson, Cora, Egbert, Melissa, Malone, Fergal, Wapner, Ronald J., Roman, Ashley S., Khalil, Asma, Faro, Revital, Madankumar, Rajeevi, Edwards, Lance, Haeri, Sina, Silver, Robert, Vohra, Nidhi, Hyett, Jon, Clunie, Garfield, Demko, Zachary, Martin, Kimberly, Rabinowitz, Matthew, Flood, Karen, Carlsson, Ylva, Doulaveris, Georgios, Malone, Ciara, Hallingstrom, Maria, Klugman, Susan, Clifton, Rebecca, Kao, Charlly, Hakonarson, Hakon, and Norton, Mary E.

Published
2022
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30. Cell-free DNA screening for prenatal detection of 22q11.2 deletion syndrome

Author

Dar, Pe’er, Jacobsson, Bo, Clifton, Rebecca, Egbert, Melissa, Malone, Fergal, Wapner, Ronald J., Roman, Ashley S., Khalil, Asma, Faro, Revital, Madankumar, Rajeevi, Edwards, Lance, Strong, Noel, Haeri, Sina, Silver, Robert, Vohra, Nidhi, Hyett, Jon, Demko, Zachary, Martin, Kimberly, Rabinowitz, Matthew, Flood, Karen, Carlsson, Ylva, Doulaveris, Georgios, Daly, Sean, Hallingström, Maria, MacPherson, Cora, Kao, Charlly, Hakonarson, Hakon, and Norton, Mary E.

Published
2022
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36. Obstetrical, perinatal and genetic outcomes associated with non-reportable prenatal cell free DNA screening results

Author

Norton, Mary E., primary, Macpherson, Cora, additional, Demko, Zachary, additional, Egbert, Melissa, additional, Malone, Fergal, additional, Wapner, Ronald J, additional, Roman, Ashley S., additional, Khalil, Asma, additional, Faro, Revital, additional, Madankumar, Rajeevi, additional, Strong, Noel, additional, Haeri, Sina, additional, Silver, Robert, additional, Vohra, Nidhi, additional, Hyett, Jon, additional, Martin, Kimberly, additional, Rabinowitz, Matthew, additional, Jacobsson, Bo, additional, and Dar, Pe’er, additional

Published
2023
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39. The Trifecta Study: Comparing Plasma Levels of Donor-derived Cell-Free DNA with the Molecular Phenotype of Kidney Transplant Biopsies

Author

Halloran, Philip F., Reeve, Jeff, Madill-Thomsen, Katelynn S., Demko, Zachary, Prewett, Adam, and Billings, Paul

Subjects
Graft Rejection, Clinical Research, Nephrology, Biopsy, Gene Expression, Humans, General Medicine, Kidney, Cell-Free Nucleic Acids, Tissue Donors
Abstract

BACKGROUND: The relationship between the donor-derived cell-free DNA fraction (dd-cfDNA[%]) in plasma in kidney transplant recipients at time of indication biopsy and gene expression in the biopsied allograft has not been defined. METHODS: In the prospective, multicenter Trifecta study, we collected tissue from 300 biopsies from 289 kidney transplant recipients to compare genome-wide gene expression in biopsies with dd-cfDNA(%) in corresponding plasma samples drawn just before biopsy. Rejection was assessed with the microarray-based Molecular Microscope Diagnostic System using automatically assigned rejection archetypes and molecular report sign-outs, and histology assessments that followed Banff guidelines. RESULTS: The median time of biopsy post-transplantation was 455 days (5 days to 32 years), with a case mix similar to that of previous studies: 180 (60%) no rejection, 89 (30%) antibody-mediated rejection (ABMR), and 31 (10%) T cell–mediated rejection (TCMR) and mixed. In genome-wide mRNA measurements, all 20 top probe sets correlating with dd-cfDNA(%) were previously annotated for association with ABMR and all types of rejection, either natural killer (NK) cell–expressed (e.g., GNLY, CCL4, TRDC, and S1PR5) or IFN-γ–inducible (e.g., PLA1A, IDO1, CXCL11, and WARS). Among gene set and classifier scores, dd-cfDNA(%) correlated very strongly with ABMR and all types of rejection, reasonably strongly with active TCMR, and weakly with inactive TCMR, kidney injury, and atrophy fibrosis. Active ABMR, mixed, and active TCMR had the highest dd-cfDNA(%), whereas dd-cfDNA(%) was lower in late-stage ABMR and less-active TCMR. By multivariate random forests and logistic regression, molecular rejection variables predicted dd-cfDNA(%) better than histologic variables. CONCLUSIONS: The dd-cfDNA(%) at time of indication biopsy strongly correlates with active molecular rejection and has the potential to reduce unnecessary biopsies. CLINICAL TRIAL REGISTRATION NUMBER: NCT04239703

Published
2022

40. Behavioral Differences Associated with Internet Gaming Disorder

Author

Demko, Zachary, Klecka, Hanna, Green, C. Shawn, Curtis, Brenda, Anthony, Lauren Elise, and Liu, Tingting

Subjects
Longitudinal, video games, Internet Gaming Disorder, Self-report, behavioral addiction, Logged
Abstract

Umbrella project registry containing a pre-registration for the analysis of the first wave of an Internet Gaming Disorder study, a pre-registration of the analysis of the first and second waves combined, and a data registration for both waves combined.

Published
2023
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43. Assessment of an automated approach for variant interpretation in screening for monogenic disorders: A single‐center study

Author

Gall, Bryan J., primary, Smart, Trevor B., additional, Munch, Robin, additional, Kolluri, Supraja, additional, Tadepally, Hamsa, additional, Lim, Karen Phaik Har, additional, Demko, Zachary P., additional, Benn, Peter, additional, Souter, Vivienne, additional, Sanapareddy, Nina, additional, and Keen‐Kim, Dianne, additional

Published
2022
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44. Clinician‐reported chorionicity and zygosity assignment using single‐nucleotide polymorphism‐based cell‐free DNA: Lessons learned from 55,344 twin pregnancies

Author

Wojas, Anna, primary, Martin, Kimberly A., additional, Koyen Malashevich, Allyson, additional, Hashimoto, Katelyn, additional, Parmar, Sheetal, additional, White, Roseann, additional, Demko, Zachary, additional, Billings, Paul, additional, Jelsema, Russ, additional, and Rebarber, Andrei, additional

Published
2022
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49. Clinical Validation of a Plasma Donor-derived Cell-free DNA Assay to Detect Allograft Rejection and Injury in Lung Transplant

Author

Rosenheck, Justin P., primary, Ross, David J., additional, Botros, Mena, additional, Wong, Alexander, additional, Sternberg, Jonathan, additional, Chen, Yen-An, additional, Liang, Nathan, additional, Baer, Amy, additional, Ahmed, Ebad, additional, Swenerton, Ryan, additional, Zimmermann, Bernhard G., additional, Fehringer, Gordon, additional, Demko, Zachary P., additional, Olymbios, Michael, additional, Billings, Paul R., additional, and Keller, Brian C., additional

Published
2022
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50. Donor-derived Cell-free DNA Shows High Sensitivity for the Diagnosis of Pancreas Graft Rejection in Simultaneous Pancreas-kidney Transplantation

Author

Ventura-Aguiar, Pedro, primary, Ramirez-Bajo, Maria Jose, additional, Rovira, Jordi, additional, Bañón-Maneus, Elisenda, additional, Hierro, Natalia, additional, Lazo, Marta, additional, Cuatrecasas, Miriam, additional, Garcia-Criado, M.A., additional, Liang, Nathan, additional, Swenerton, Ryan K., additional, Cofan, Federic, additional, Cucchiari, David, additional, Esforzado, Nuria, additional, Montagud-Marrahi, Enrique, additional, Oppenheimer, Federic, additional, Piñeiro, Gaston, additional, Revuelta, Ignacio, additional, Torregrosa, Vicens, additional, Ahmed, Ebad, additional, Soboleva, Karina, additional, Kaur, Navchetan, additional, Zimmermann, Bernhard G., additional, Al Haj Baddar, Nour, additional, Demko, Zachary P., additional, Escrig, Cesar, additional, Tabriziani, Hossein, additional, Gauthier, Philippe, additional, Billings, Paul R., additional, Amor, Antonio J., additional, Ferrer, Joana, additional, Campistol, Josep M., additional, and Diekmann, Fritz, additional

Published
2022
Full Text
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