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1. Distinct spatial immune microlandscapes are independently associated with outcomes in triple-negative breast cancer

Author

Carter, Jodi M., Chumsri, Saranya, Hinerfeld, Douglas A., Ma, Yaohua, Wang, Xue, Zahrieh, David, Hillman, David W., Tenner, Kathleen S., Kachergus, Jennifer M., Brauer, Heather Ann, Warren, Sarah E., Henderson, David, Shi, Ji, Liu, Yi, Joensuu, Heikki, Lindman, Henrik, Leon-Ferre, Roberto A., Boughey, Judy C., Liu, Minetta C., Ingle, James N., Kalari, Krishna R., Couch, Fergus J., Knutson, Keith L., Goetz, Matthew P., Perez, Edith A., and Thompson, E. Aubrey

Published
2023
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2. Rejuvenation of the aged brain immune cell landscape in mice through p16-positive senescent cell clearance

Author

Zhang, Xu, Pearsall, Vesselina M., Carver, Chase M., Atkinson, Elizabeth J., Clarkson, Benjamin D. S., Grund, Ethan M., Baez-Faria, Michelle, Pavelko, Kevin D., Kachergus, Jennifer M., White, Thomas A., Johnson, Renee K., Malo, Courtney S., Gonzalez-Suarez, Alan M., Ayasoufi, Katayoun, Johnson, Kurt O., Tritz, Zachariah P., Fain, Cori E., Khadka, Roman H., Ogrodnik, Mikolaj, Jurk, Diana, Zhu, Yi, Tchkonia, Tamara, Revzin, Alexander, Kirkland, James L., Johnson, Aaron J., Howe, Charles L., Thompson, E. Aubrey, LeBrasseur, Nathan K., and Schafer, Marissa J.

Published
2022
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3. Evidence of cerebellar TDP-43 loss of function in FTLD-TDP

Author

Pickles, Sarah, Gendron, Tania F., Koike, Yuka, Yue, Mei, Song, Yuping, Kachergus, Jennifer M., Shi, J., DeTure, Michael, Thompson, E. Aubrey, Oskarsson, Björn, Graff-Radford, Neill R., Boeve, Bradley F., Petersen, Ronald C., Wszolek, Zbigniew K., Josephs, Keith A., Dickson, Dennis W., Petrucelli, Leonard, Cook, Casey N., and Prudencio, Mercedes

Published
2022
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4. Truncated stathmin-2 is a marker of TDP-43 pathology in frontotemporal dementia

Author

Petrucelli, Leonard, Prudencio, Mercedes, Humphrey, Jack, Pickles, Sarah, Brown, Anna-Leigh, Hill, Sarah E., Kachergus, Jennifer M., Shi, J., Heckman, Michael G., Spiegel, Matthew R., Cook, Casey, Song, Yuping, Daughrity, Lilian M., Carlomagno, Yari, Sivakumar, Prasanth, Yue, Mei, Jansen-West, Karen, Fernandez de Castro, Cristhoper, DeTure, Michael, Koga, Shunsuke, Wang, Ying-Chih, Bodo, Cristian, Candalija, Ana, Talbot, Kevin, Selvaraj, Bhuvaneish T., Burr, Karen, Chandran, Siddharthan, Newcombe, Jia, Lashley, Tammaryn, Hubbard, Isabel, Catalano, Demetra, Kim, Duyang, Propp, Nadia, Fennessey, Samantha, Fagegaltier, Delphine, Phatnani, Hemali, Secrier, Maria, Fisher, Elizabeth M.C., Oskarsson, Bjorn, van Blitterswijk, Marka, Rademakers, Rosa, Graff-Radford, Neil, Boeve, Bradley F., Knopman, David S., Petersen, Ronald C., Josephs, Keith A., Thompson, E. Aubrey, Raj, Towfique, Ward, Michael, Dickson, Dennis W., Gendron, Tania F., and Fratta, Pietro

Subjects
Frontotemporal dementia -- Diagnosis -- Genetic aspects -- Care and treatment, DNA binding proteins -- Health aspects -- Structure, Health care industry
Abstract

No treatment for frontotemporal dementia (FTD), the second most common type of early-onset dementia, is available, but therapeutics are being investigated to target the 2 main proteins associated with FTD pathological subtypes: TDP-43 (FTLD-TDP) and tau (FTLD-tau). Testing potential therapies in clinical trials is hampered by our inability to distinguish between patients with FTLD-TDP and FTLD-tau. Therefore, we evaluated truncated stathmin-2 (STMN2) as a proxy of TDP-43 pathology, given the reports that TDP-43 dysfunction causes truncated STMN2 accumulation. Truncated STMN2 accumulated in human induced pluripotent stem cell-derived neurons depleted of TDP-43, but not in those with pathogenic TARDBP mutations in the absence of TDP-43 aggregation or loss of nuclear protein. In RNA-Seq analyses of human brain samples from the NYGC ALS cohort, truncated STMN2 RNA was confined to tissues and disease subtypes marked by TDP43 inclusions. Last, we validated that truncated STMN2 RNA was elevated in the frontal cortex of a cohort of patients with FTLD-TDP but not in controls or patients with progressive supranuclear palsy, a type of FTLD-tau. Further, in patients with FTLD-TDP, we observed significant associations of truncated STMN2 RNA with phosphorylated TDP-43 levels and an earlier age of disease onset. Overall, our data uncovered truncated STMN2 as a marker for TDP-43 dysfunction in FTD., Introduction Tar DNA-binding protein 43 (TDP-43) regulates multiple aspects of RNA metabolism, including RNA stabilization, transcription, splicing, and transport (1). TDP-43 binds thousands of RNAs (2, 3) and, for particular [...]

Published
2020
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5. Elevated methylation levels, reduced expression levels, and frequent contractions in a clinical cohort of C9orf72 expansion carriers

Author

Jackson, Jazmyne L., Finch, NiCole A., Baker, Matthew C., Kachergus, Jennifer M., DeJesus-Hernandez, Mariely, Pereira, Kimberly, Christopher, Elizabeth, Prudencio, Mercedes, Heckman, Michael G., Thompson, E. Aubrey, Dickson, Dennis W., Shah, Jaimin, Oskarsson, Björn, Petrucelli, Leonard, Rademakers, Rosa, and van Blitterswijk, Marka

Published
2020
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6. Discrete class I molecules on brain endothelium differentially regulate neuropathology in experimental cerebral malaria.

Author

Fain, Cori E, Zheng, Jiaying, Jin, Fang, Ayasoufi, Katayoun, Wu, Yue, Lilley, Meredith T, Dropik, Abigail R, Wolf, Delaney M, Rodriguez, Robert C, Aibaidula, Abudumijiti, Tritz, Zachariah P, Bouchal, Samantha M, Pewe, Lecia L, Urban, Stina L, Chen, Yin, Chang, Su-Youne, Hansen, Michael J, Kachergus, Jennifer M, Shi, Ji, and Thompson, E Aubrey

Subjects
CEREBRAL malaria, T cell receptors, NEUROLOGICAL disorders, ENDOTHELIUM, IRON in the body, MAJOR histocompatibility complex
Abstract

Cerebral malaria is the deadliest complication that can arise from Plasmodium infection. CD8 T-cell engagement of brain vasculature is a putative mechanism of neuropathology in cerebral malaria. To define contributions of brain endothelial cell major histocompatibility complex (MHC) class I antigen-presentation to CD8 T cells in establishing cerebral malaria pathology, we developed novel H-2Kb LoxP and H-2Db LoxP mice crossed with Cdh5-Cre mice to achieve targeted deletion of discrete class I molecules, specifically from brain endothelium. This strategy allowed us to avoid off-target effects on iron homeostasis and class I-like molecules, which are known to perturb Plasmodium infection. This is the first endothelial-specific ablation of individual class-I molecules enabling us to interrogate these molecular interactions. In these studies, we interrogated human and mouse transcriptomics data to compare antigen presentation capacity during cerebral malaria. Using the Plasmodium berghei ANKA model of experimental cerebral malaria (ECM), we observed that H-2Kb and H-2Db class I molecules regulate distinct patterns of disease onset, CD8 T-cell infiltration, targeted cell death and regional blood–brain barrier disruption. Strikingly, ablation of either molecule from brain endothelial cells resulted in reduced CD8 T-cell activation, attenuated T-cell interaction with brain vasculature, lessened targeted cell death, preserved blood–brain barrier integrity and prevention of ECM and the death of the animal. We were able to show that these events were brain-specific through the use of parabiosis and created the novel technique of dual small animal MRI to simultaneously scan conjoined parabionts during infection. These data demonstrate that interactions of CD8 T cells with discrete MHC class I molecules on brain endothelium differentially regulate development of ECM neuropathology. Therefore, targeting MHC class I interactions therapeutically may hold potential for treatment of cases of severe malaria. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Glucocerebrosidase mutations in diffuse Lewy body disease

Author

Nishioka, Kenya, Ross, Owen A., Vilariño-Güell, Carles, Cobb, Stephanie A., Kachergus, Jennifer M., Mann, David M.A., Snowden, Julie, Richardson, Anna M.T., Neary, David, Robinson, Christopher A., Rajput, Alex, Papapetropoulos, Spiridon, Mash, Deborah C., Pahwa, Rajesh, Lyons, Kelly E., Wszolek, Zbigniew K., Dickson, Dennis W., and Farrer, Matthew J.

Published
2011
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11. A Swedish family with de novo α-synuclein A53T mutation: Evidence for early cortical dysfunction

Author

Puschmann, Andreas, Ross, Owen A., Vilariño-Güell, Carles, Lincoln, Sarah J., Kachergus, Jennifer M., Cobb, Stephanie A., Lindquist, Suzanne G., Nielsen, Jørgen E., Wszolek, Zbigniew K., Farrer, Matthew, Widner, Håkan, van Westen, Danielle, Hägerström, Douglas, Markopoulou, Katerina, Chase, Bruce A., Nilsson, Karin, Reimer, Jan, and Nilsson, Christer

Published
2009
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15. Novel pathogenic LRRK2 p.Asn1437His substitution in familial Parkinsonʼs disease

Author

Aasly, Jan O., Vilariño-Güell, Carles, Dachsel, Justus C., Webber, Philip J., West, Andrew B., Haugarvoll, Kristoffer, Johansen, Krisztina K., Toft, Mathias, Nutt, John G., Payami, Haydeh, Kachergus, Jennifer M., Lincoln, Sarah J., Felic, Amela, Wider, Christian, Soto-Ortolaza, Alexandra I., Cobb, Stephanie A., White, Linda R., Ross, Owen A., and Farrer, Matthew J.

Published
2010
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16. Association of α-, β-, and γ-Synuclein With Diffuse Lewy Body Disease

Author

Nishioka, Kenya, Wider, Christian, Vilariño-Güell, Carles, Soto-Ortolaza, Alexandra I., Lincoln, Sarah J., Kachergus, Jennifer M., Jasinska-Myga, Barbara, Ross, Owen A., Rajput, Alex, Robinson, Christopher A., Ferman, Tanis J., Wszolek, Zbigniew K., Dickson, Dennis W., and Farrer, Matthew J.

Published
2010

18. LRRK2 mutations and Parkinsonism

Author

Toft, Mathias, Mata, Ignacio F., Kachergus, Jennifer M., Ross, Owen A., Farrer, Matthew J., and Albrecht, Mario

Subjects
Parkinson's disease -- Diagnosis, Parkinson's disease -- Care and treatment, Gene mutations -- Research
Published
2005

19. Intrinsic Subtype and Therapeutic Response Among HER2-Positive Breast Tumors from the NCCTG (Alliance) N9831 Trial.

Author

Perez, Edith A., Ballman, Karla V., Mashadi-Hossein, Afshin, Tenner, Kathleen S., Kachergus, Jennifer M., Norton, Nadine, Necela, Brian M., Carr, Jennifer M., Ferree, Sean, Perou, Charles M., Baehner, Frederick, Cheang, Maggie Chon U., and Thompson, E. Aubrey

Subjects
BREAST tumors, EPIDERMAL growth factor receptors, KAPLAN-Meier estimator, TRASTUZUMAB, CANCER chemotherapy
Abstract

Background: Genomic data from human epidermal growth factor receptor 2-positive (HER2+) tumors were analyzed to assess the association between intrinsic subtype and clinical outcome in a large, well-annotated patient cohort.Methods: Samples from the NCCTG (Alliance) N9831 trial were analyzed using the Prosigna algorithm on the NanoString platform to define intrinsic subtype, risk of recurrence scores, and risk categories for 1392 HER2+ tumors. Subtypes were evaluated for recurrence-free survival (RFS) using Kaplan-Meier and Cox model analysis following adjuvant chemotherapy (n = 484) or chemotherapy plus trastuzumab (n = 908). All statistical tests were two-sided.Results: Patients with HER2+ tumors from N9831 were primarily scored as HER2-enriched (72.1%). These individuals received statistically significant benefit from trastuzumab (hazard ratio [HR] = 0.68, 95% confidence interval [CI] = 0.52 to 0.89, P = .005), as did the patients (291 of 1392) with luminal-type tumors (HR = 0.52, 95% CI = 0.32 to 0.85, P = .01). Patients with basal-like tumors (97 of 1392) did not have statistically significantly better RFS when treated with trastuzumab and chemotherapy compared with chemotherapy alone (HR = 1.06, 95% CI = 0.53 to 2.13, P = .87).Conclusions: The majority of clinically defined HER2-positive tumors were classified as HER2-enriched or luminal using the Prosigna algorithm. Intrinsic subtype alone cannot replace conventional histopathological evaluation of HER2 status because many tumors that are classified as luminal A or luminal B will benefit from adjuvant trastuzumab if that subtype is accompanied by HER2 overexpression. However, among tumors that overexpress HER2, we speculate that assessment of intrinsic subtype may influence treatment, particularly with respect to evaluating alternative therapeutic approaches for that subset of HER2-positive tumors of the basal-like subtype. [ABSTRACT FROM AUTHOR]

Published
2017
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20. Assessment of Tumor Heterogeneity, as Evidenced by Gene Expression Profiles, Pathway Activation, and Gene Copy Number, in Patients with Multifocal Invasive Lobular Breast Tumors.

Author

Norton, Nadine, Advani, Pooja P., Serie, Daniel J., Geiger, Xochiquetzal J., Necela, Brian M., Axenfeld, Bianca C., Kachergus, Jennifer M., Feathers, Ryan W., Carr, Jennifer M., Crook, Julia E., Moreno-Aspitia, Alvaro, Anastasiadis, Panos Z., Perez, Edith A., and Thompson, E. Aubrey

Subjects
BREAST tumors, LOBULAR carcinoma, GENE expression, DNA copy number variations, LYMPH node cancer, PATIENTS
Abstract

Background: Invasive lobular carcinoma (ILC) comprises approximately ~10–20% of breast cancers. In general, multifocal/multicentric (MF/MC) breast cancer has been associated with an increased rate of regional lymph node metastases. Tumor heterogeneity between foci represents a largely unstudied source of genomic variation in those rare patients with MF/MC ILC. Methods: We characterized gene expression and copy number in 2 or more foci from 11 patients with MF/MC ILC (all ER+, HER2-) and adjacent normal tissue. RNA and DNA were extracted from 3x1.5mm cores from all foci. Gene expression (730 genes) and copy number (80 genes) were measured using Nanostring PanCancer and Cancer CNV panels. Linear mixed models were employed to compare expression in tumor versus normal samples from the same patient, and to assess heterogeneity (variability) in expression among multiple ILC within an individual. Results: 35 and 34 genes were upregulated (FC>2) and down-regulated (FC<0.5) respectively in ILC tumor relative to adjacent normal tissue, q<0.05. 9/34 down-regulated genes (FIGF, RELN, PROM1, SFRP1, MMP7, NTRK2, LAMB3, SPRY2, KIT) had changes larger than CDH1, a hallmark of ILC. Copy number changes in these patients were relatively few but consistent across foci within each patient. Amplification of three genes (CCND1, FADD, ORAOV1) at 11q13.3 was present in 2/11 patients in both foci. We observed significant evidence of within-patient between-foci variability (heterogeneity) in gene expression for 466 genes (p<0.05 with FDR 8%), including CDH1, FIGF, RELN, SFRP1, MMP7, NTRK2, LAMB3, SPRY2 and KIT. Conclusions: There was substantial variation in gene expression between ILC foci within patients, including known markers of ILC, suggesting an additional level of complexity that should be addressed. [ABSTRACT FROM AUTHOR]

Published
2016
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21. Folate Receptor-α (FOLR1) Expression and Function in Triple Negative Tumors.

Author

Necela, Brian M., Crozier, Jennifer A., Andorfer, Cathy A., Lewis-Tuffin, Laura, Kachergus, Jennifer M., Geiger, Xochiquetzal J., Kalari, Krishna R., Serie, Daniel J., Sun, Zhifu, Aspita, Alvaro Moreno, O’Shannessy, Daniel J., Maltzman, Julia D., McCullough, Ann E., Pockaj, Barbara A., Cunliffe, Heather E., Ballman, Karla V., Thompson, E. Aubrey, and Perez, Edith A.

Subjects
JUNO protein, PROTEIN expression, CANCER treatment, BREAST cancer prognosis, CLINICAL trials, EPIDERMAL growth factor receptors
Abstract

Folate receptor alpha (FOLR1) has been identified as a potential prognostic and therapeutic target in a number of cancers. A correlation has been shown between intense overexpression of FOLR1 in breast tumors and poor prognosis, yet there is limited examination of the distribution of FOLR1 across clinically relevant breast cancer subtypes. To explore this further, we used RNA-seq data from multiple patient cohorts to analyze the distribution of FOLR1 mRNA across breast cancer subtypes comprised of estrogen receptor positive (ER+), human epidermal growth factor receptor positive (HER2+), and triple negative (TNBC) tumors. FOLR1 expression varied within breast tumor subtypes; triple negative/basal tumors were significantly associated with increased expression of FOLR1 mRNA, compared to ER+ and HER2+ tumors. However, subsets of high level FOLR1 expressing tumors were observed in all clinical subtypes. These observations were supported by immunohistochemical analysis of tissue microarrays, with the largest number of 3+ positive tumors and highest H-scores of any subtype represented by triple negatives, and lowest by ER+ tumors. FOLR1 expression did not correlate to common clinicopathological parameters such as tumor stage and nodal status. To delineate the importance of FOLR1 overexpression in triple negative cancers, RNA-interference was used to deplete FOLR1 in overexpressing triple negative cell breast lines. Loss of FOLR1 resulted in growth inhibition, whereas FOLR1 overexpression promoted folate uptake and growth advantage in low folate conditions. Taken together, our data suggests patients with triple negative cancers expressing high FOLR1 expression represent an important population of patients that may benefit from targeted anti-FOLR1 therapy. This may prove particularly helpful for a large number of patients who would typically be classified as triple negative and who to this point have been left without any targeted treatment options. [ABSTRACT FROM AUTHOR]

Published
2015
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23. Fine-mapping and candidate gene investigation within the PARK10 locus.

Author

Haugarvoll, Kristoffer, Toft, Mathias, Skipper, Lisa, Heckman, Michael G., Crook, Julia E., Soto, Alexandra, Ross, Owen A., Hulihan, Mary M., Kachergus, Jennifer M., Sando, Sigrid B., White, Linda R., Lynch, Timothy, Gibson, J. Mark, Uitti, Ryan J., Wszolek, Zbigniew K., Aasly, Jan O., and Farrer, Matthew J.

Subjects
CLINICAL trials, GENE mapping, PARKINSON'S disease, NUCLEOTIDES, GENETIC polymorphisms, GENOTYPE-environment interaction
Abstract

Herein, we investigate whether single-nucleotide polymorphisms (SNPs) across the PARK10 locus are associated with susceptibility to Parkinson's disease (PD) or age at onset (AAO) of disease. One hundred and eighty-eight SNPs were genotyped across the PARK10 locus in 180 PD patients and 180 controls from central Norway (stage 1). We then used the linkage disequilibrium (LD) structure from stage 1 to select 75 SNPs for genotyping in 186 patients and 186 controls from Ireland (stage 2). Nineteen SNPs were selected from this and previous studies for follow-up in an extended Norwegian series (530 patients and 1142 controls), the Irish series and a US series (221 patients and 221 controls) (stage 3). After correction for multiple testing, markers within ubiquitin specific peptidase 24 (USP24) are significantly associated with PD within Norwegian, Irish, and US series combined (rs13312: odds ratio (OR) 0.78, P<0.001; rs487230: OR 0.80, P=0.001). Independently, the association for rs13312 is strongest in the extended Norwegian series (OR 0.76, P=0.005), although not significant after correction for multiple testing (P≤0.003 is considered significant). ORs in the Irish series are almost identical, and a similar but a weaker effect was observed for the US series. No marker showed consistent association with AAO. Our data indicate that genetic variability in USP24 is associated with PD. Although our work extends and confirms a previous report, the observed effect size does not explain the PARK10 linkage peak.European Journal of Human Genetics (2009) 17, 336–343; doi:10.1038/ejhg.2008.187; published online 15 October 2008 [ABSTRACT FROM AUTHOR]

Published
2009
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24. DCTN1 mutations in Perry syndrome.

Author

Farrer, Matthew J., Hulihan, Mary M., Kachergus, Jennifer M., Dächsel, Justus C., Stoessl, A. Jon, Grantier, Linda L., Calne, Susan, Calne, Donald B., Lechevalier, Bernard, Chapon, Francoise, Tsuboi, Yoshio, Yamada, Tatsuo, Gutmann, Ludwig, Elibol, Bülent, Bhatia, Kailash P., Wider, Christian, Vilariño-Güell, Carles, Ross, Owen A., Brown, Laura A., and Castanedes-Casey, Monica

Subjects
PARKINSON'S disease, MENTAL depression, WEIGHT loss, HYPOVENTILATION, PATHOLOGY, BRAIN diseases, GENETIC mutation, NEURONS, DISEASES
Abstract

Perry syndrome consists of early-onset parkinsonism, depression, severe weight loss and hypoventilation, with brain pathology characterized by TDP-43 immunostaining. We carried out genome-wide linkage analysis and identified five disease-segregating mutations affecting the CAP-Gly domain of dynactin (encoded by DCTN1) in eight families with Perry syndrome; these mutations diminish microtubule binding and lead to intracytoplasmic inclusions. Our findings show that DCTN1 mutations, previously associated with motor neuron disease, can underlie the selective vulnerability of other neuronal populations in distinct neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published
2009
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25. Chromoanasynthesis is a common mechanism that leads to ERBB2 amplifications in a cohort of early stage HER2+ breast cancer samples.

Author

Vasmatzis, George, Wang, Xue, Smadbeck, James B, Murphy, Stephen J, Geiersbach, Katherine B, Johnson, Sarah H, Gaitatzes, Athanasios G, Asmann, Yan W, Kosari, Farhad, Borad, Mitesh J, Serie, Daniel J, McLaughlin, Sarah A, Kachergus, Jennifer M, Necela, Brian M, Aubrey Thompson, E, and Thompson, E Aubrey

Abstract

Background: HER2 positive (HER2+) breast cancers involve chromosomal structural alterations that act as oncogenic driver events.Methods: We interrogated the genomic structure of 18 clinically-defined HER2+ breast tumors through integrated analysis of whole genome and transcriptome sequencing, coupled with clinical information.Results: ERBB2 overexpression in 15 of these tumors was associated with ERBB2 amplification due to chromoanasynthesis with six of them containing single events and the other nine exhibiting multiple events. Two of the more complex cases had adverse clinical outcomes. Chromosomes 8 was commonly involved in the same chromoanasynthesis with 17. In ten cases where chromosome 8 was involved we observed NRG1 fusions (two cases), NRG1 amplification (one case), FGFR1 amplification and ADAM32 or ADAM5 fusions. ERBB3 over-expression was associated with NRG1 fusions and EGFR and ERBB3 expressions were anti-correlated. Of the remaining three cases, one had a small duplication fully encompassing ERBB2 and was accompanied with a pathogenic mutation.Conclusion: Chromoanasynthesis involving chromosome 17 can lead to ERBB2 amplifications in HER2+ breast cancer. However, additional large genomic alterations contribute to a high level of genomic complexity, generating the hypothesis that worse outcome could be associated with multiple chromoanasynthetic events. [ABSTRACT FROM AUTHOR]

Published
2018
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26. Correction: Folate Receptor-α (FOLR1) Expression and Function in Triple Negative Tumors.

Author

Necela, Brian M., Crozier, Jennifer A., Andorfer, Cathy A., Lewis-Tuffin, Laura, Kachergus, Jennifer M., Geiger, Xochiquetzal J., Kalari, Krishna R., Serie, Daniel J., Sun, Zhifu, Moreno-Aspitia, Alvaro, O’Shannessy, Daniel J., Maltzman, Julia D., McCullough, Ann E., Pockaj, Barbara A., Cunliffe, Heather E., Ballman, Karla V., Thompson, E. Aubrey, and Perez, Edith A.

Subjects
PUBLISHED errata, PERIODICAL articles, PUBLISHING, JUNO protein, GENE expression
Published
2015
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27. Gene Expression, Single Nucleotide Variant and Fusion Transcript Discovery in Archival Material from Breast Tumors.

Author

Norton, Nadine, Sun, Zhifu, Asmann, Yan W., Serie, Daniel J., Necela, Brian M., Bhagwate, Aditya, Jen, Jin, Eckloff, Bruce W., Kalari, Krishna R., Thompson, Kevin J., Carr, Jennifer M., Kachergus, Jennifer M., Geiger, Xochiquetzal J., Perez, Edith A., and Thompson, E. Aubrey

Subjects
GENE expression, SINGLE nucleotide polymorphisms, GENETIC transcription, GENE fusion, BREAST tumors, NUCLEOTIDE sequence
Abstract

Advantages of RNA-Seq over array based platforms are quantitative gene expression and discovery of expressed single nucleotide variants (eSNVs) and fusion transcripts from a single platform, but the sensitivity for each of these characteristics is unknown. We measured gene expression in a set of manually degraded RNAs, nine pairs of matched fresh-frozen, and FFPE RNA isolated from breast tumor with the hybridization based, NanoString nCounter (226 gene panel) and with whole transcriptome RNA-Seq using RiboZeroGold ScriptSeq V2 library preparation kits. We performed correlation analyses of gene expression between samples and across platforms. We then specifically assessed whole transcriptome expression of lincRNA and discovery of eSNVs and fusion transcripts in the FFPE RNA-Seq data. For gene expression in the manually degraded samples, we observed Pearson correlations of >0.94 and >0.80 with NanoString and ScriptSeq protocols, respectively. Gene expression data for matched fresh-frozen and FFPE samples yielded mean Pearson correlations of 0.874 and 0.783 for NanoString (226 genes) and ScriptSeq whole transcriptome protocols respectively, p<2x10-16. Specifically for lincRNAs, we observed superb Pearson correlation (0.988) between matched fresh-frozen and FFPE pairs. FFPE samples across NanoString and RNA-Seq platforms gave a mean Pearson correlation of 0.838. In FFPE libraries, we detected 53.4% of high confidence SNVs and 24% of high confidence fusion transcripts. Sensitivity of fusion transcript detection was not overcome by an increase in depth of sequencing up to 3-fold (increase from ~56 to ~159 million reads). Both NanoString and ScriptSeq RNA-Seq technologies yield reliable gene expression data for degraded and FFPE material. The high degree of correlation between NanoString and RNA-Seq platforms suggests discovery based whole transcriptome studies from FFPE material will produce reliable expression data. The RiboZeroGold ScriptSeq protocol performed particularly well for lincRNA expression from FFPE libraries, but detection of eSNV and fusion transcripts was less sensitive. [ABSTRACT FROM AUTHOR]

Published
2013
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28. An Integrated Model of the Transcriptome of HER2-Positive Breast Cancer.

Author

Kalari, Krishna R., Necela, Brian M., Tang, Xiaojia, Thompson, Kevin J., Lau, Melissa, Eckel-Passow, Jeanette E., Kachergus, Jennifer M., Anderson, S. Keith, Sun, Zhifu, Baheti, Saurabh, Carr, Jennifer M., Baker, Tiffany R., Barman, Poulami, Radisky, Derek C., Joseph, Richard W., McLaughlin, Sarah A., Chai, High-seng, Camille, Stephan, Rossell, David, and Asmann, Yan W.

Subjects
HER2 gene, GENETICS of breast cancer, RNA, NUCLEOTIDE sequence, PRECANCEROUS conditions, BREAST surgery, ONCOLOGY
Abstract

Our goal in these analyses was to use genomic features from a test set of primary breast tumors to build an integrated transcriptome landscape model that makes relevant hypothetical predictions about the biological and/or clinical behavior of HER2-positive breast cancer. We interrogated RNA-Seq data from benign breast lesions, ER+, triple negative, and HER2-positive tumors to identify 685 differentially expressed genes, 102 alternatively spliced genes, and 303 genes that expressed single nucleotide sequence variants (eSNVs) that were associated with the HER2-positive tumors in our survey panel. These features were integrated into a transcriptome landscape model that identified 12 highly interconnected genomic modules, each of which represents a cellular processes pathway that appears to define the genomic architecture of the HER2-positive tumors in our test set. The generality of the model was confirmed by the observation that several key pathways were enriched in HER2-positive TCGA breast tumors. The ability of this model to make relevant predictions about the biology of breast cancer cells was established by the observation that integrin signaling was linked to lapatinib sensitivity in vitro and strongly associated with risk of relapse in the NCCTG N9831 adjuvant trastuzumab clinical trial dataset. Additional modules from the HER2 transcriptome model, including ubiquitin-mediated proteolysis, TGF-beta signaling, RHO-family GTPase signaling, and M-phase progression, were linked to response to lapatinib and paclitaxel in vitro and/or risk of relapse in the N9831 dataset. These data indicate that an integrated transcriptome landscape model derived from a test set of HER2-positive breast tumors has potential for predicting outcome and for identifying novel potential therapeutic strategies for this breast cancer subtype. [ABSTRACT FROM AUTHOR]

Published
2013
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29. Truncated stathmin-2 is a marker of TDP-43 pathology in frontotemporal dementia.

Author

Prudencio, Mercedes, Humphrey, Jack, Pickles, Sarah, Brown, Anna-Leigh, Hill, Sarah E., Kachergus, Jennifer M., Shi, J., Heckman, Michael G., Spiegel, Matthew R., Cook, Casey, Yuping Song, Mei Yue, Daughrity, Lillian M., Carlomagno, Yari, Jansen-West, Karen, de Castro, Cristhoper Fernandez, DeTure, Michael, Koga, Shunsuke, Ying-Chih Wang, and Sivakumar, Prasanth

Subjects
*FRONTOTEMPORAL lobar degeneration, *FRONTOTEMPORAL dementia, *PROGRESSIVE supranuclear palsy, *NUCLEAR proteins, *PATHOLOGY, *AGE of onset, *RNA sequencing, *FRONTAL lobe, *RESEARCH, *NERVE tissue proteins, *GENETIC mutation, *RESEARCH methodology, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *DNA-binding proteins, *STEM cells, *RESEARCH funding
Abstract

No treatment for frontotemporal dementia (FTD), the second most common type of early-onset dementia, is available, but therapeutics are being investigated to target the 2 main proteins associated with FTD pathological subtypes: TDP-43 (FTLD-TDP) and tau (FTLD-tau). Testing potential therapies in clinical trials is hampered by our inability to distinguish between patients with FTLD-TDP and FTLD-tau. Therefore, we evaluated truncated stathmin-2 (STMN2) as a proxy of TDP-43 pathology, given the reports that TDP-43 dysfunction causes truncated STMN2 accumulation. Truncated STMN2 accumulated in human induced pluripotent stem cell-derived neurons depleted of TDP-43, but not in those with pathogenic TARDBP mutations in the absence of TDP-43 aggregation or loss of nuclear protein. In RNA-Seq analyses of human brain samples from the NYGC ALS cohort, truncated STMN2 RNA was confined to tissues and disease subtypes marked by TDP-43 inclusions. Last, we validated that truncated STMN2 RNA was elevated in the frontal cortex of a cohort of patients with FTLD-TDP but not in controls or patients with progressive supranuclear palsy, a type of FTLD-tau. Further, in patients with FTLD-TDP, we observed significant associations of truncated STMN2 RNA with phosphorylated TDP-43 levels and an earlier age of disease onset. Overall, our data uncovered truncated STMN2 as a marker for TDP-43 dysfunction in FTD. [ABSTRACT FROM AUTHOR]

Published
2020
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30. VPS35 Mutations in Parkinson Disease

Author

Vilariño-Güell, Carles, Wider, Christian, Ross, Owen A., Dachsel, Justus C., Kachergus, Jennifer M., Lincoln, Sarah J., Soto-Ortolaza, Alexandra I., Cobb, Stephanie A., Wilhoite, Greggory J., Bacon, Justin A., Behrouz, Bahareh, Melrose, Heather L., Hentati, Emna, Puschmann, Andreas, Evans, Daniel M., Conibear, Elizabeth, Wasserman, Wyeth W., Aasly, Jan O., Burkhard, Pierre R., and Djaldetti, Ruth

Subjects
*PARKINSON'S disease, *GENETIC mutation, *GENETIC disorders, *NUCLEOTIDE sequence, *ASPARTIC acid, *MEMBRANE proteins, *LYSOSOMES
Abstract

The identification of genetic causes for Mendelian disorders has been based on the collection of multi-incident families, linkage analysis, and sequencing of genes in candidate intervals. This study describes the application of next-generation sequencing technologies to a Swiss kindred presenting with autosomal-dominant, late-onset Parkinson disease (PD). The family has tremor-predominant dopa-responsive parkinsonism with a mean onset of 50.6 ± 7.3 years. Exome analysis suggests that an aspartic-acid-to-asparagine mutation within vacuolar protein sorting 35 (VPS35 c.1858G>A; p.Asp620Asn) is the genetic determinant of disease. VPS35 is a central component of the retromer cargo-recognition complex, is critical for endosome-trans-golgi trafficking and membrane-protein recycling, and is evolutionarily highly conserved. VPS35 c.1858G>A was found in all affected members of the Swiss kindred and in three more families and one patient with sporadic PD, but it was not observed in 3,309 controls. Further sequencing of familial affected probands revealed only one other missense variant, VPS35 c.946C>T; (p.Pro316Ser), in a pedigree with one unaffected and two affected carriers, and thus the pathogenicity of this mutation remains uncertain. Retromer-mediated sorting and transport is best characterized for acid hydrolase receptors. However, the complex has many types of cargo and is involved in a diverse array of biologic pathways from developmental Wnt signaling to lysosome biogenesis. Our study implicates disruption of VPS35 and retromer-mediated trans-membrane protein sorting, rescue, and recycling in the neurodegenerative process leading to PD. [Copyright &y& Elsevier]

Published
2011
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31. Glucocerebrosidase mutations are not a common risk factor for Parkinson disease in North Africa

Author

Nishioka, Kenya, Vilariño-Güell, Carles, Cobb, Stephanie A., Kachergus, Jennifer M., Ross, Owen A., Wider, Christian, Gibson, Rachel A., Hentati, Faycal, and Farrer, Matthew J.

Subjects
*GENETIC mutation, *ENZYMES, *DISEASE risk factors, *PARKINSON'S disease, *NUCLEOTIDE sequence, *ASHKENAZIM, *NORTH Africans
Abstract

Abstract: Mutations in the glucocerebrosidase gene (GBA) have recently been associated with an increased risk of Parkinson disease (PD). GBA mutations have been observed to be particularly prevalent in the Ashkenazi Jewish population. Interestingly, this population also has a high incidence of the Lrrk2 p.G2019S mutation which is similar in North African Arab-Berber populations. Herein, our sequencing of the GBA gene, in 33 North African Arab-Berber familial parkinsonism probands, identified two novel mutations in three individuals (p.K-26R and p.K186R). Segregation analysis of these two variants did not support a pathogenic role. Genotyping of p.K-26R, p.K186R and the common p.N370S in an ethnically matched series consisting of 395 patients with PD and 372 control subjects did not show a statistically significant association (P >0.05). The p.N370S mutation was only identified in 1 sporadic patient with PD and 3 control subjects indicating that the frequency of this mutation in the North African Arab-Berber population is much lower than that observed in Ashkenazi Jews, and therefore arose in the latter after expansion of the Lrrk2 p.G2019S variant in North Africa. [Copyright &y& Elsevier]

Published
2010
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32. Lrrk2 mutations in South America: A study of Chilean Parkinson's disease

Author

Perez-Pastene, Carolina, Cobb, Stephanie A., Díaz-Grez, Fernando, Hulihan, Mary M., Miranda, Marcelo, Venegas, Pablo, Godoy, Osvaldo Trujillo, Kachergus, Jennifer M., Ross, Owen A., Layson, Luis, Farrer, Matthew J., and Segura-Aguilar, Juan

Subjects
*PROTEIN-tyrosine kinases, *GENETIC mutation, *PARKINSON'S disease
Abstract

Abstract: Pathogenic substitutions in the leucine-rich repeat kinase 2 protein (Lrrk2), R1441G and G2019S, are a prevalent cause of autosomal dominant and sporadic Parkinson''s disease in the Northern Spanish population. In this study we examined the frequency of these two substitutions in 166 Parkinson''s disease patients and 153 controls from Chile, a population with Spanish/European-Amerindian admixture. Lrrk2 R1441G was not observed, however Lrrk2 G2019S was detected in one familial and four sporadic Parkinson''s disease patients. These findings suggest Lrrk2 G2019S may play an important role in Parkinson''s disease on the South American Continent and further studies are now warranted. [Copyright &y& Elsevier]

Published
2007
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33. EIF4G1 gene mutations are not a common cause of Parkinson's disease in the Japanese population.

Author

Nishioka, Kenya, Funayama, Manabu, Vilariño-Güell, Carles, Ogaki, Kotaro, Li, Yuanzhe, Sasaki, Ryogen, Kokubo, Yasumasa, Kuzuhara, Shigeki, Kachergus, Jennifer M., Cobb, Stephanie A., Takahashi, Hirohide, Mizuno, Yoshikuni, Farrer, Matthew J., Ross, Owen A., and Hattori, Nobutaka

Subjects
*PARKINSON'S disease, *ETIOLOGY of diseases, *GENETIC mutation, *EXONS (Genetics), *JAPANESE people, *GENETIC code, *DISEASES
Abstract

Abstract: Pathogenic mutations in the EIF4G1 gene were recently reported as a cause of autosomal dominant parkinsonism. To assess the frequency of EIF4G1 mutations in the Japanese population we sequenced the entire gene coding region (31 exons) in 95 patients with an apparent autosomal dominant inherited form of Parkinson's disease. We detected three novel point mutations located in a poly-glutamic acid repeat within exon 10. These variants were screened through 224 Parkinson's disease cases and 374 normal controls from the Japanese population. We detected the poly-glutamic acid deletion in exon 10 in two additional patients with sporadic Parkinson's disease. Although the EIF4G1 variants identified in the present study were not observed in control subjects, co-segregation analyses and population-based screening data suggest they are not pathogenic. In conclusion, we did not identify novel or previously reported pathogenic mutations (including the p.A502V and p.R1205H mutants) within EIF4G1 in the Japanese population, thus future studies are warranted to elucidate the role of this gene in Parkinson's disease. [Copyright &y& Elsevier]

Published
2014
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34. Homozygous partial genomic triplication of the parkin gene in early-onset parkinsonism

Author

Mata, Ignacio F., Alvarez, Victoria, Coto, Eliecer, Blazquez, Marta, Guisasola, Luis M., Salvador, Carlos, Kachergus, Jennifer M., Lincoln, Sarah J., and Farrer, Matthew

Subjects
*PARKINSON'S disease, *GENETIC mutation, *GENETICS, *BRAIN diseases
Abstract

Abstract: Autosomal recessive mutations in the parkin gene are the predominant cause of familial, early-onset parkinsonism; missense mutations involving one or a few nucleotides, exonic deletions and duplications have been described. Here we report a family with two affected brothers. Direct sequencing of parkin did not detect mutations, but semi-quantitative analysis identified a novel exonic rearrangement of exons 2–4. Both patients were homozygous for unique genomic triplications of the parkin gene. [Copyright &y& Elsevier]

Published
2005
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35. Genetic variation of the mitochondrial complex I subunit NDUFV2 and Parkinson's disease.

Author

Nishioka K, Vilariño-Güell C, Cobb SA, Kachergus JM, Ross OA, Hentati E, Hentati F, Farrer MJ, Nishioka, Kenya, Vilariño-Güell, Carles, Cobb, Stephanie A, Kachergus, Jennifer M, Ross, Owen A, Hentati, Emna, Hentati, Faycal, and Farrer, Matthew J

Subjects
*PROTEINS, *REVERSE transcriptase polymerase chain reaction, *BERBERS, *DNA, *GENETICS, *GENETIC mutation, *GENETIC carriers, *DOCUMENTATION, *PARKINSON'S disease, *AGE factors in disease, *GENES, *RESEARCH funding, *AMINO acids, *GENETIC techniques, *GENEALOGY
Abstract

NADH dehydrogenase ubiquinone flavoprotein 2 (NDUFV2), encoding a subunit of mitochondrial complex I, is a candidate gene for several neuronal diseases; schizophrenia, bipolar disorder and Parkinson disease (PD). We screened the entire coding region of NDUFV2 in 33 familial PD patients of North African Arab-Berber ethnicity in which all known genetic forms of PD had been excluded. We detected one novel substitution p.K209R (c.626A>G) in one PD proband. Segregation analysis within the family is inconclusive due to small sample size, but consistent with an autosomal dominant mode of inheritance. Subsequent screening of this mutation in ethnically matched sporadic PD patients (n = 238) and controls (n = 371) identified p.K209R in one additional patient. The clinical features of the mutation carriers revealed a mild form of parkinsonism with a prognosis similar to idiopathic PD. Our findings suggest further studies addressing the role of NDUFV2 variation in PD may be warranted. [ABSTRACT FROM AUTHOR]

Published
2010
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