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1. Molecular profiling of pre- and post-treatment pediatric high-grade astrocytomas reveals acquired increased tumor mutation burden in a subset of recurrences

Author

Matthew D. Wood, Carol Beadling, Tanaya Neff, Steve Moore, Christina A. Harrington, Lissa Baird, and Christopher Corless

Subjects
High-grade astrocytoma, Pediatric brain tumor, Hypermutation, DNA mismatch repair, Molecular profiling, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Diffuse gliomas are a heterogeneous category of primary central nervous system tumors. Due to their infiltrative growth precluding complete surgical resection, most diffuse high-grade gliomas are treated with adjuvant chemotherapy and radiation. Recurrent/progressive diffuse gliomas may show genetic differences when compared to the primary tumors, giving insight into their molecular evolution and mechanisms of treatment resistance. In adult-type diffuse gliomas with or without isocitrate dehydrogenase gene mutations, tumor recurrence/progression can be associated with mutations in genes encoding DNA mismatch repair proteins, leading to a dramatic increase in tumor mutation burden. This phenomenon is closely linked to treatment with the DNA alkylating agent temozolomide, a mainstay of adult diffuse glioma chemotherapeutic management. Post-treatment mismatch repair deficiency and acquired high tumor mutation burden is relatively unexplored in pediatric patients who have recurrent high-grade gliomas. Here, we report a molecular and histological analysis of an institutional cohort of eleven pediatric patients with paired initial and recurrent high-grade astrocytoma samples with intervening temozolomide treatment. We identified three cases with evidence for increased tumor mutation burden at recurrence, including two cases of diffuse hemispheric glioma H3 G34-mutant (one previously reported). We also show that molecular analysis by next-generation DNA sequencing and DNA methylation-based profiling enabled an integrated diagnosis per 2021 World Health Organization criteria in 10 of 11 cases (91%). Our findings indicate that increased tumor mutation burden at post-treatment recurrence is relevant in pediatric-type diffuse high-grade gliomas. Diffuse hemispheric glioma H3 G34-mutant may be particularly susceptible to this phenomenon.

Published
2023
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2. Novel recruitment approaches and operational results for a statewide population Cohort for cancer research: The Healthy Oregon Project

Author

Zhenzhen Zhang, Autumn Shafer, Katie Johnson-Camacho, Andrew Adey, Pavana Anur, Kim A. Brown, Casey Conrad, Rachel Crist, Paige E. Farris, Christina A. Harrington, Lisa K. Marriott, Asia Mitchell, Brian O’Roak, Vanessa Serrato, C. Sue Richards, Paul T. Spellman, and Jackilen Shannon

Subjects
Cohort, population, HOP, genetics, app, Medicine
Abstract

Abstract Background: Cancer health research relies on large-scale cohorts to derive generalizable results for different populations. While traditional epidemiological cohorts often use costly random sampling or self-motivated, preselected groups, a shift toward health system-based cohorts has emerged. However, such cohorts depend on participants remaining within a single system. Recent consumer engagement models using smartphone-based communication, driving projects, and social media have begun to upend these paradigms. Methods: We initiated the Healthy Oregon Project (HOP) to support basic and clinical cancer research. HOP study employs a novel, cost-effective remote recruitment approach to effectively establish a large-scale cohort for population-based studies. The recruitment leverages the unique email account, the HOP website, and social media platforms to direct smartphone users to the study app, which facilitates saliva sample collection and survey administration. Monthly newsletters further facilitate engagement and outreach to broader communities. Results: By the end of 2022, the HOP has enrolled approximately 35,000 participants aged 18–100 years (median = 44.2 years), comprising more than 1% of the Oregon adult population. Among those who have app access, ∼87% provided consent to genetic screening. The HOP monthly email newsletters have an average open rate of 38%. Efforts continue to be made to improve survey response rates. Conclusion: This study underscores the efficacy of remote recruitment approaches in establishing large-scale cohorts for population-based cancer studies. The implementation of the study facilitates the collection of extensive survey and biological data into a repository that can be broadly shared and supports collaborative clinical and translational research.

Published
2024
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3. RNA-seq from archival FFPE breast cancer samples: molecular pathway fidelity and novel discovery

Author

Nathan D. Pennock, Sonali Jindal, Wesley Horton, Duanchen Sun, Jayasri Narasimhan, Lucia Carbone, Suzanne S. Fei, Robert Searles, Christina A. Harrington, Julja Burchard, Sheila Weinmann, Pepper Schedin, and Zheng Xia

Subjects
FFPE, Formalin fixed paraffin embedded, Breast Cancer, RNA sequencing, RNA-Seq, genomics, Archival tissue, Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Formalin-fixed, paraffin-embedded (FFPE) tissues for RNA-seq have advantages over fresh frozen tissue including abundance and availability, connection to rich clinical data, and association with patient outcomes. However, FFPE-derived RNA is highly degraded and chemically modified, which impacts its utility as a faithful source for biological inquiry. Methods True archival FFPE breast cancer cases (n = 58), stored at room temperature for 2–23 years, were utilized to identify key steps in tissue selection, RNA isolation, and library choice. Gene expression fidelity was evaluated by comparing FFPE data to public data obtained from fresh tissues, and by employing single-gene, gene set and transcription network-based regulon analyses. Results We report a single 10 μm section of breast tissue yields sufficient RNA for RNA-seq, and a relationship between RNA quality and block age that was not linear. We find single-gene analysis is limiting with FFPE tissues, while targeted gene set approaches effectively distinguish ER+ from ER- breast cancers. Novel utilization of regulon analysis identified the transcription factor KDM4B to associate with ER+ disease, with KDM4B regulon activity and gene expression having prognostic significance in an independent cohort of ER+ cases. Conclusion Our results, which outline a robust FFPE-RNA-seq pipeline for broad use, support utilizing FFPE tissues to address key questions in the breast cancer field, including the delineation between indolent and life-threatening disease, biological stratification and molecular mechanisms of treatment resistance.

Published
2019
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4. Analysis of extracellular RNA in cerebrospinal fluid

Author

Julie A. Saugstad, Theresa A. Lusardi, Kendall R. Van Keuren-Jensen, Jay I. Phillips, Babett Lind, Christina A. Harrington, Trevor J. McFarland, Amanda L. Courtright, Rebecca A. Reiman, Ashish S. Yeri, M. Yashar S. Kalani, P. David Adelson, Jorge Arango, John P. Nolan, Erika Duggan, Karen Messer, Johnny C. Akers, Douglas R. Galasko, Joseph F. Quinn, Bob S. Carter, and Fred H. Hochberg

Subjects
Extracellular vesicles, extracellular RNA, cerebrospinal fluid, neurological diseases, Cytology, QH573-671
Abstract

We examined the extracellular vesicle (EV) and RNA composition of pooled normal cerebrospinal fluid (CSF) samples and CSF from five major neurological disorders: Alzheimer’s disease (AD), Parkinson’s disease (PD), low-grade glioma (LGG), glioblastoma multiforme (GBM), and subarachnoid haemorrhage (SAH), representing neurodegenerative disease, cancer, and severe acute brain injury. We evaluated: (I) size and quantity of EVs by nanoparticle tracking analysis (NTA) and vesicle flow cytometry (VFC), (II) RNA yield and purity using four RNA isolation kits, (III) replication of RNA yields within and between laboratories, and (IV) composition of total and EV RNAs by reverse transcription–quantitative polymerase chain reaction (RT-qPCR) and RNA sequencing (RNASeq). The CSF contained ~106 EVs/μL by NTA and VFC. Brain tumour and SAH CSF contained more EVs and RNA relative to normal, AD, and PD. RT-qPCR and RNASeq identified disease-related populations of microRNAs and messenger RNAs (mRNAs) relative to normal CSF, in both total and EV fractions. This work presents relevant measures selected to inform the design of subsequent replicative CSF studies. The range of neurological diseases highlights variations in total and EV RNA content due to disease or collection site, revealing critical considerations guiding the selection of appropriate approaches and controls for CSF studies.

Published
2017
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41. RNA isolation from micro-quantity of articular cartilage for quantitative gene expression by microarray analysis

Author

Xiaowei Zhang, Trevor J. McFarland, Kristina Vartanian, Yong Zhu, Christina A. Harrington, and Cong-Qiu Chu

Subjects
Cartilage, Articular, Gene Expression, General Medicine, Microarray Analysis, RNA isolation, Chondrocytes, Animals, RNA, articular cartilage, cartilage repair, Female, Rabbits, microarray, Research Paper
Abstract

Isolation of quality RNA from articular cartilage has been challenging due to low cellularity and the high abundance of extracellular matrix and proteoglycan proteins. Recently developed methods for isolation of high quality RNA from cartilage are more applicable to larger cartilage specimens typically weighing at least 25 mg. While these methods generate RNA suitable for analysis, they are less successful with smaller tissue inputs. For the study of small focal defect cartilage specimens an improved RNA extraction method is needed. Here we report a protocol for direct RNA isolation from less than 3 mg of wet weight rabbit articular cartilage for quantitative microarray gene profiling. This protocol is useful for identifying differentially expressed genes in chondrocytes following focal cartilage repair and can potentially be adopted for gene expression analysis of cartilage biopsy specimens from human joints.

Published
2022

43. Identifying RNA Biomarkers and Molecular Pathways Involved in Multiple Subtypes of Uveitis

Author

Amr Zaki, Stephen R. Planck, Christopher D. Conrady, Suzanne S. Fei, Christina A. Harrington, Dongseok Choi, Albert T. Vitale, Robert P. Searles, Lynn M. Hassman, Lindsey Watson, Tammy M. Martin, Puthyda Keath, Sruthi Arepalli, James T. Rosenbaum, Claire Mitchell, and Michael A. Paley

Subjects
Genetic Markers, Disease, Inflammatory bowel disease, Article, Uveitis, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Gene Regulatory Networks, RNA, Messenger, KEGG, Eye Proteins, Gene, 030304 developmental biology, 0303 health sciences, business.industry, Gene Expression Profiling, medicine.disease, Gene expression profiling, Ophthalmology, Gene Expression Regulation, Immunology, 030221 ophthalmology & optometry, RNA, Sarcoidosis, business
Abstract

Uveitis is a heterogeneous collection of diseases. We tested the hypothesis that despite the diversity of uveitides, there could be common mechanisms shared by multiple subtypes, and that evidence of these common mechanisms may be detected as gene expression profiles in whole blood.Cohort study.Ninety subjects with uveitis including axial spondyloarthritis (n = 17), sarcoidosis (n = 13), inflammatory bowel disease (n = 12), tubulointerstitial nephritis with uveitis (n = 10), or idiopathic uveitis (n = 38) as well as 18 healthy controls were enrolled, predominantly at Oregon HealthScience University. RNA-Seq data generated from peripheral, whole blood identified 19,859 unique transcripts. We analyzed gene expression pathways via Kyoto Encyclopedia of Genes and Genomes and Gene Ontology (GO). We validated our list of upregulated genes by comparison to a previously published study on peripheral blood gene expression among 50 subjects with diverse forms of uveitis.Both the Kyoto Encyclopedia of Genes and Genomes and GO analysis identified multiple shared pathways or GO terms with a P value of.0001. Almost all pathways related to the immune response and/or response to an infection. A total of 119 individual transcripts were upregulated by at least 1.5-fold and false discovery rate.05, and 61 were downregulated by similar criteria. Comparing mRNA from our study with a false discovery rate.05 and the prior report, we identified 10 common gene transcripts: ICAM1, IL15RA, IL15, IRF1, IL10RB, GSK3A, TYK2, MEF2A, MEF2B, and MEF2D.Many forms of uveitis share overlapping mechanisms. These data support the concept that a single therapeutic approach could benefit diverse forms of this disease.

Published
2021
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44. Enrichment of IGF-1R and PPARγ signalling pathways in orbital inflammatory diseases: steps toward understanding pathogenesis

Author

Bobby S. Korn, Haila Al-Hussain, Gerald J. Harris, Rohan Verma, James T. Rosenbaum, Don O. Kikkawa, Chris Alabiad, Armando L. Garcia, Michael Kazim, Dongseok Choi, Deepak P. Edward, John D. Ng, Roger A. Dailey, Craig N. Czyz, Allison J Chen, Christina A. Harrington, David J. Wilson, Azza Maktabi, Jill A. Foster, Hans E. Grossniklaus, Stephen R. Planck, and Eric A. Steele

Subjects
0301 basic medicine, MAPK/ERK pathway, Sarcoidosis, Microarray, Adipose tissue, AMP-Activated Protein Kinases, Receptor, IGF Type 1, Pathogenesis, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Adipokines, Orbital Diseases, Humans, Medicine, Protein kinase B, PI3K/AKT/mTOR pathway, Inflammation, business.industry, AMPK, Middle Aged, Sensory Systems, Graves Ophthalmopathy, PPAR gamma, Gene expression profiling, Ophthalmology, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Female, business, Orbit, Proto-Oncogene Proteins c-akt
Abstract

BackgroundOrbital inflammatory disease (OID) encompasses a wide range of pathology including thyroid-associated orbitopathy (TAO), granulomatosis with polyangiitis (GPA), sarcoidosis and non-specific orbital inflammation (NSOI), accounting for up to 6% of orbital diseases. Understanding the underlying pathophysiology of OID can improve diagnosis and help target therapy.AimsTo test the hypothesis that shared signalling pathways are activated in different forms of OID.MethodsIn this secondary analysis, pathway analysis was performed on the previously reported differentially expressed genes from orbital adipose tissue using patients with OID and healthy controls who were characterised by microarray. For the original publications, tissue specimens were collected from oculoplastic surgeons at 10 international centres representing four countries (USA, Canada, Australia and Saudi Arabia). Diagnoses were independently confirmed by two masked ocular pathologists (DJW, HEG). Gene expression profiling analysis was performed at the Oregon Health & Science University. Eighty-three participants were included: 25 with TAO, 6 with orbital GPA, 7 with orbital sarcoidosis, 25 with NSOI and 20 healthy controls.ResultsAmong the 83 subjects (mean (SD) age, 52.8 (18.3) years; 70% (n=58) female), those with OID demonstrated perturbation of the downstream gene expressions of the IGF-1R (MAPK/RAS/RAF/MEK/ERK and PI3K/Akt/mTOR pathways), peroxisome proliferator-activated receptor-γ (PPARγ), adipocytokine and AMPK signalling pathways compared with healthy controls. Specifically, GPA samples differed from controls in gene expression within the insulin-like growth factor-1 receptor (IGF-1R, PI3K-Akt (p=0.001), RAS (p=0.005)), PPARγ (p=0.002), adipocytokine (p=0.004) or AMPK (p=ConclusionsAlthough OID includes a heterogenous group of pathologies, TAO, GPA, sarcoidosis and NSOI share enrichment of common gene signalling pathways, namely IGF-1R, PPARγ, adipocytokine and AMPK. Pathway analyses of gene expression suggest that other forms of orbital inflammation in addition to TAO may benefit from blockade of IGF-1R signalling pathways.

Published
2021
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45. Revising the Diagnosis of Idiopathic Uveitis by Peripheral Blood Transcriptomics

Author

Christopher D. Conrady, Lynn M. Hassman, Tammy M. Martin, Albert T. Vitale, Robert P. Searles, Suzanne S. Fei, Dongseok Choi, Puthyda Keath, Amr Zaki, Sruthi Arepalli, Stephen R. Planck, Lindsey Watson, Christina A. Harrington, Michael A. Paley, James T. Rosenbaum, and Claire Mitchell

Subjects
Adult, Male, medicine.medical_specialty, Systemic disease, Gene Expression, Disease, Inflammatory bowel disease, Gastroenterology, Article, Diagnosis, Differential, Uveitis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, 030304 developmental biology, 0303 health sciences, business.industry, Case-control study, Middle Aged, medicine.disease, Gene expression profiling, Ophthalmology, Case-Control Studies, 030221 ophthalmology & optometry, Female, Sarcoidosis, Differential diagnosis, Transcriptome, business, Algorithms, Biomarkers
Abstract

PURPOSE: To test the hypothesis that idiopathic uveitis can be categorized into subtypes based on gene expression from blood. DESIGN: Case control study METHODS: We applied RNA-Seq to peripheral blood from patients with uveitis associated with one of four systemic diseases, including axial spondyloarthritis (n=17), sarcoidosis (n=13), inflammatory bowel disease (n=12), tubulo-interstitial nephritis with uveitis (n=10), or idiopathic uveitis (n=38) as well as 18 healthy controls evaluated predominantly at Oregon Health & Science University. A high dimensional negative binomial regression model implemented in the edgeR R package compared each disease group against the controls. The 20 most distinctive genes for each diagnosis were extracted. Out of 80 genes, there were 75 unique genes. A classification algorithm was developed by fitting a gradient boosting tree with 5-fold cross-validation. mRNA from subjects with idiopathic uveitis was analyzed to see if any fit clinically and by gene expression pattern with one of the diagnosable entities. RESULTS: For uveitis associated with a diagnosable systemic disease, gene expression profiling achieved an overall accuracy of 85% (balanced average of sensitivity plus specificity, p-value < 0.001). Although the majority of patients with idiopathic uveitis presumably have none of these four associated systemic diseases, gene expression profiles helped to reclassify 11 of 38 subjects. CONCLUSIONS: Peripheral blood gene expression profiling is a potential adjunct in accurate differential diagnosis of the cause of uveitis. Validation of these results and characterization of the gene expression profile from additional discrete diagnoses could enhance the value of these observations.

Published
2021
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46. RNA-Seq of human whole blood: Evaluation of globin RNA depletion on Ribo-Zero library method

Author

James T. Rosenbaum, Suzanne S. Fei, Stephen R. Planck, Robert P. Searles, Brett Davis, Kimberly Ogle, Christina A. Harrington, Lucia Carbone, Dongseok Choi, and Jessica Minnier

Subjects
0301 basic medicine, lcsh:Medicine, RNA-Seq, Computational biology, Biology, Article, Specimen Handling, Transcriptome, 03 medical and health sciences, Gene expression analysis, 0302 clinical medicine, Poster Abstracts, Humans, Globin, Transcriptomics, lcsh:Science, Whole blood, Multidisciplinary, lcsh:R, RNA, Ribosomal RNA, Peripheral blood, Globins, Blood, 030104 developmental biology, 030221 ophthalmology & optometry, lcsh:Q, Hemoglobin, Biomarkers
Abstract

Peripheral blood is a highly accessible biofluid providing a rich source of information about human physiology and health status. However, for studies of the blood transcriptome with RNA sequencing (RNA-Seq) techniques, high levels of hemoglobin mRNAs (hgbRNA) present in blood can occupy valuable sequencing space, impacting detection and quantification of non-hgbRNAs. In this study, we evaluated two methods for preparing ribosomal RNA (rRNA)-depleted sequencing libraries for RNA-Seq of whole blood, one of which is also designed to deplete hgbRNAs. Two experiments were performed: one evaluating library performance across 6 human blood samples and the other examining library reproducibility and performance in a two-subject subset. We find that addition of hgbRNA depletion to the rRNA-depletion protocol for library preparation from blood RNA effectively reduces highly abundant hgbRNA reads; however, it does not result in a statistically significant increase in differentially expressed genes in our patient-control study. Bioinformatic removal of globin gene counts in non-hgbRNA depleted libraries provides improvement in overall performance of these libraries. We conclude that use of a standard ribosomal RNA depletion method for library preparation coupled with bioinformatic removal of globin gene counts is sufficient for reproducible and sensitive measurement of both coding and noncoding RNAs in the blood transcriptome.

Published
2020
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47. The Role of the Immune Response in the Pathogenesis of Thyroid Eye Disease: A Reassessment.

Author

James T Rosenbaum, Dongseok Choi, Amanda Wong, David J Wilson, Hans E Grossniklaus, Christina A Harrington, Roger A Dailey, John D Ng, Eric A Steele, Craig N Czyz, Jill A Foster, David Tse, Chris Alabiad, Sander Dubovy, Prashant K Parekh, Gerald J Harris, Michael Kazim, Payal J Patel, Valerie A White, Peter J Dolman, Deepak P Edward, Hind M Alkatan, Hailah Al Hussain, Dinesh Selva, R Patrick Yeatts, Bobby S Korn, Don O Kikkawa, Patrick Stauffer, and Stephen R Planck

Subjects
Medicine, Science
Abstract

Although thyroid eye disease is a common complication of Graves' disease, the pathogenesis of the orbital disease is poorly understood. Most authorities implicate the immune response as an important causal factor. We sought to clarify pathogenesis by using gene expression microarray.An international consortium of ocular pathologists and orbital surgeons contributed formalin fixed orbital biopsies. RNA was extracted from orbital tissue from 20 healthy controls, 25 patients with thyroid eye disease (TED), 25 patients with nonspecific orbital inflammation (NSOI), 7 patients with sarcoidosis and 6 patients with granulomatosis with polyangiitis (GPA). Tissue was divided into a discovery set and a validation set. Gene expression was quantified using Affymetrix U133 Plus 2.0 microarrays which include 54,000 probe sets.Principal component analysis showed that gene expression from tissue from patients with TED more closely resembled gene expression from healthy control tissue in comparison to gene expression characteristic of sarcoidosis, NSOI, or granulomatosis with polyangiitis. Unsupervised cluster dendrograms further indicated the similarity between TED and healthy controls. Heat maps based on gene expression for cytokines, chemokines, or their receptors showed that these inflammatory markers were associated with NSOI, sarcoidosis, or GPA much more frequently than with TED.This is the first study to compare gene expression in TED to gene expression associated with other causes of exophthalmos. The juxtaposition shows that inflammatory markers are far less characteristic of TED relative to other orbital inflammatory diseases.

Published
2015
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48. RNA-seq from archival FFPE breast cancer samples: molecular pathway fidelity and novel discovery

Author

Julja Burchard, Jayasri Narasimhan, Sonali Jindal, Lucia Carbone, Christina A. Harrington, Wesley Horton, Suzanne S. Fei, Nathan D. Pennock, Duanchen Sun, Robert P. Searles, Sheila Weinmann, Pepper Schedin, and Zheng Xia

Subjects
lcsh:Internal medicine, Tissue Fixation, Archival tissue, lcsh:QH426-470, RNA-Seq, Breast Neoplasms, Computational biology, Biology, FFPE, Regulon, RNA-Seq, genomics, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Transcription (biology), Formaldehyde, Gene expression, KDM4B, Breast Cancer, Genetics, medicine, Estrogen receptor, Humans, lcsh:RC31-1245, Gene, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Paraffin Embedding, RNA, RNA sequencing, medicine.disease, 3. Good health, Formalin fixed paraffin embedded, lcsh:Genetics, Receptors, Estrogen, 030220 oncology & carcinogenesis, RNA extraction, DNA microarray, Research Article, Signal Transduction
Abstract

Background Formalin-fixed, paraffin-embedded (FFPE) tissues for RNA-seq have advantages over fresh frozen tissue including abundance and availability, connection to rich clinical data, and association with patient outcomes. However, FFPE-derived RNA is highly degraded and chemically modified, which impacts its utility as a faithful source for biological inquiry. Methods True archival FFPE breast cancer cases (n = 58), stored at room temperature for 2–23 years, were utilized to identify key steps in tissue selection, RNA isolation, and library choice. Gene expression fidelity was evaluated by comparing FFPE data to public data obtained from fresh tissues, and by employing single-gene, gene set and transcription network-based regulon analyses. Results We report a single 10 μm section of breast tissue yields sufficient RNA for RNA-seq, and a relationship between RNA quality and block age that was not linear. We find single-gene analysis is limiting with FFPE tissues, while targeted gene set approaches effectively distinguish ER+ from ER- breast cancers. Novel utilization of regulon analysis identified the transcription factor KDM4B to associate with ER+ disease, with KDM4B regulon activity and gene expression having prognostic significance in an independent cohort of ER+ cases. Conclusion Our results, which outline a robust FFPE-RNA-seq pipeline for broad use, support utilizing FFPE tissues to address key questions in the breast cancer field, including the delineation between indolent and life-threatening disease, biological stratification and molecular mechanisms of treatment resistance.

Published
2019

49. Deconstructing Community-Based Collaborative Design

Author

Sheena Erete, Christina N. Harrington, and Anne Marie Piper

Subjects
Human-Computer Interaction, Scholarship, Underserved Population, Harm, Computer Networks and Communications, Participatory design, Situated, Engineering ethics, Narrative, Context (language use), Sociology, Social Sciences (miscellaneous), Privilege (social inequality)
Abstract

Participatory Design (PD) is envisioned as an approach to democratizing innovation in the design process by shifting the power dynamics between researcher and participant. Recent scholarship in HCI and design has analyzed the ways collaborative design engagements, such as PD situated in the design workshop can amplify voices and empower underserved populations. Yet, we argue that PD as instantiated in the design workshop is very much an affluent and privileged activity that often neglects the challenges associated with envisioning equitable design solutions among underserved populations. Based on two series of community-based PD workshops with underserved populations in the U.S., we highlight key areas of tension and considerations for a more equitable PD approach: historical context of the research environment, community access, perceptions of materials and activities, and unintentional harm in collecting full accounts of personal narratives. By reflecting on these tensions as a call-to-action, we hope to deconstruct the privilege of the PD workshop within HCI and re-center the focus of design on individuals who are historically underserved.

Published
2019
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50. Validation of MicroRNA Biomarkers for Alzheimer’s Disease in Human Cerebrospinal Fluid

Author

Douglas Galasko, Julie A. Saugstad, Trevor J. McFarland, Theresa A. Lusardi, Christina A. Harrington, Jay Ian Phillips, Jodi Lapidus, Jack Wiedrick, Ursula S. Sandau, Joseph F. Quinn, and Babett Lind

Subjects
Male, 0301 basic medicine, Oncology, Apolipoprotein E, medicine.medical_specialty, Validation study, Genotype, Apolipoprotein E4, tau Proteins, Total tau, Disease, Real-Time Polymerase Chain Reaction, Article, 03 medical and health sciences, 0302 clinical medicine, Cerebrospinal fluid, Alzheimer Disease, Internal medicine, microRNA, Humans, Medicine, Aged, Amyloid beta-Peptides, Mini–Mental State Examination, medicine.diagnostic_test, business.industry, General Neuroscience, Reproducibility of Results, General Medicine, Peptide Fragments, MicroRNAs, Psychiatry and Mental health, Clinical Psychology, 030104 developmental biology, Case-Control Studies, Female, Geriatrics and Gerontology, business, Biomarkers, 030217 neurology & neurosurgery
Abstract

We previously discovered microRNAs (miRNAs) in cerebrospinal fluid (CSF) that differentiate Alzheimer’s disease (AD) patients from Controls. Here we examined the performance of 37 candidate AD miRNA biomarkers in a new and independent cohort of CSF from 47 AD patients and 71 Controls on custom TaqMan® arrays. We employed a consensus ranking approach to provide an overall priority score for each miRNA, then used multimarker models to assess the relative contributions of the top-ranking miRNAs to differentiate AD from Controls. We assessed classification performance of the top-ranking miRNAs when combined with apolipoprotein E4 (APOE4) genotype status or CSF amyloid-β(42) (Aβ(42)):total tau (T-tau) measures. We also assessed whether miRNAs that ranked higher as AD markers correlate with Mini-Mental State Examination (MMSE) scores. We show that of 37 miRNAs brought forth from the discovery study, 26 miRNAs remained viable as candidate biomarkers for AD in the validation study. We found that combinations of 6–7 miRNAs work better to identify AD than subsets of fewer miRNAs. Of 26 miRNAs that contribute most to the multimarker models, 14 have higher potential than the others to predict AD. Addition of these 14 miRNAs to APOE4 status or CSF Aβ(42):T-tau measures significantly improved classification performance for AD. We further show that individual miRNAs that ranked higher as AD markers correlate more strongly with changes in MMSE scores. Our studies validate that a set of CSF miRNAs serve as biomarkers for AD, and support their advancement toward development as biomarkers in the clinical setting.

Published
2019
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