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3. A mixed-method study evaluating an innovative care model for rural patients undergoing outpatient breast surgery

Author

Chiu, Sharon, Fowler, Samantha, Bridges, Sarah, Hanson, Natasha, King, Jordan, Street, Sarah, Tait, Heather, Irving, Karen, Mclean, Peggy, Mclaughlin, Lauren, and Gulliver, Adrienne

Subjects
Medical research -- Methods, Medicine, Experimental -- Methods, Nurses -- Methods, Stress (Psychology) -- Care and treatment, Health, Health care industry
Abstract

Background: The Delta Oasis program was launched in New Brunswick in 2006 to offer patients from rural areas who were undergoing breast cancer surgery and their families 1 night of free accommodations and a postoperative consultation with an extramural nurse. We sought to investigate patient experiences with this program. Methods: This mixed-method retrospective study took place from 2020 to 2022 and compared the preoperative anxiety and quality of recovery of program participants and control patients who were discharged home over 100 km from hospital. We conducted 2x2 analysis of variance to evaluate the effects of intervention group and surgery type. We conducted semistructured interviews with intervention participants, which we then thematically analyzed. Two patient partners were engaged during data synthesis to support the interpretation of results. Results: We included 34 patients who participated in the program and 18 control patients. No statistically significant differences were found between treatment groups in preoperative anxiety and quality of recovery, regardless of surgery type. Thematic analysis of interviews with 17 intervention participants revealed that they were highly satisfied with the program and that the experience helped reduce stress and discomfort related to their surgery. Interpretation: The Delta Oasis program is a cost-effective alternative to inpatient care after breast cancer surgery and is highly regarded by rural patients; expansion to other regions with the inclusion of additional low-risk surgeries could help address hospital capacity issues. This study contributes to our understanding of the patient experience with the Delta Oasis program and informs the development of similar programs elsewhere. Contexte : Le programme Delta Oasis a t lanc au Nouveau-Brunswick en 2006 pour offrir aux personnes des r gions rurales devant subir une intervention chirurgicale pour un cancer du sein et leur famille 1 nuit d'h bergement gratuite et une consultation postop ratoire avec une infirmi re ou un infirmier hors murs. Nous avons voulu interroger la patient le sur son exp rience du programme. M thodes : Il s'agit d'une tude r trospective m thodes mixtes men e de 2020 2022 pour comparer l'anxi t pr op ratoire et la qualit du r tablissement de personnes participant au programme avec celles des membres d'un groupe t moin retourn s leur domicile, plus de 100 km de l'h pital. Nous avons men une analyse de la variance 2 facteurs pour valuer les effets selon le groupe et le type de chirurgie. Nous avons r alis aupr s des membres du groupe sous intervention des entrevues semi-structur es que nous avons ensuite analys es th matiquement. Deux patients partenaires ont t consult s pendant la synth se des donn es pour confirmer l'interpr tation des r sultats. R sultats : Nous avons interrog 34 personnes ayant particip au programme et 18 du groupe t moin. Aucune diff rence statistiquement significative n'a t constat e entre les groupes quant l'anxi t pr op ratoire et la qualit du r tablissement, quel que soit le type de chirurgie. L'analyse th matique des entrevues men es aupr s de 17 membres du groupe sous intervention a r v l qu'ils taient extr mement satisfaits du programme et que l'exp rience avait att nu le stress et l'inconfort li s l'intervention chirurgicale. Conclusion : Le programme Delta Oasis est une fa on rentable de remplacer les soins hospitaliers apr s une chirurgie pour un cancer du sein; il est tr s appr ci des personnes qui vivent en r gion rurale. En l' tendant d'autres r gions et d'autres interventions chirurgicales faible risque, on pourrait contribuer r soudre les probl mes de capacit hospitali re. Cette tude nous aide comprendre l'exp rience de la patient le dans le programme Delta Oasis et claire l'instauration de programmes semblables ailleurs., In recent decades, developed countries have seen a major increase in outpatient surgeries, which allow stable patients to be discharged home on the same day of surgery after a period [...]

Published
2024
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6. The role of admixture in the rare variant contribution to inflammatory bowel disease

Author

Courtney Astore, Shivam Sharma, Sini Nagpal, NIDDK IBD Genetics Consortium, David J. Cutler, John D. Rioux, Judy H. Cho, Dermot P. B. McGovern, Steven R. Brant, Subra Kugathasan, I. King Jordan, and Greg Gibson

Subjects
Trans-ancestry, Crohn’s disease, NOD2, Genetic risk assessment, Whole genome sequencing, Medicine, Genetics, QH426-470
Abstract

Abstract Background Identification of rare variants involved in complex, polygenic diseases like Crohn’s disease (CD) has accelerated with the introduction of whole exome/genome sequencing association studies. Rare variants can be used in both diagnostic and therapeutic assessments; however, since they are likely to be restricted to specific ancestry groups, their contributions to risk assessment need to be evaluated outside the discovery population. Prior studies implied that the three known rare variants in NOD2 are absent in West African and Asian populations and only contribute in African Americans via admixture. Methods Whole genome sequencing (WGS) data from 3418 African American individuals, 1774 inflammatory bowel disease (IBD) cases, and 1644 controls were used to assess odds ratios and allele frequencies (AF), as well as haplotype-specific ancestral origins of European-derived CD variants discovered in a large exome-wide association study. Local and global ancestry was performed to assess the contribution of admixture to IBD contrasting European and African American cohorts. Results Twenty-five rare variants associated with CD in European discovery cohorts are typically five-fold lower frequency in African Americans. Correspondingly, where comparisons could be made, the rare variants were found to have a predicted four-fold reduced burden for IBD in African Americans, when compared to European individuals. Almost all of the rare CD European variants were found on European haplotypes in the African American cohort, implying that they contribute to disease risk in African Americans primarily due to recent admixture. In addition, proportion of European ancestry correlates the number of rare CD European variants each African American individual carry, as well as their polygenic risk of disease. Similar findings were observed for 23 mutations affecting 10 other common complex diseases for which the rare variants were discovered in European cohorts. Conclusions European-derived Crohn’s disease rare variants are even more rare in African Americans and contribute to disease risk mainly due to admixture, which needs to be accounted for when performing cross-ancestry genetic assessments.

Published
2023
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8. Ancestral origins of TYR and OCA2 gene mutations in oculocutaneous albinism from two admixed populations in Colombia.

Author

Wilmer A Cárdenas, Andrew B Conley, Shashwat Deepali Nagar, Diana L Núñez-Ríos, I King Jordan, and María Claudia Lattig

Subjects
Medicine, Science
Abstract

Autosomal recessive conditions are often associated with homozygous mutations showing common ancestral origins and are frequently linked to consanguinity. However, an increasing number of compound heterozygotes are found in diverse, admixed populations. Oculocutaneous albinism (OCA) is a recessive condition caused mainly by mutations in the TYR and OCA2 genes involved in skin pigmentation. We previously screened the TYR and OCA2 genes in Colombian OCA families, identifying both known and novel mutations. Affected family members were found to be either homozygous or compound heterozygous for these gene mutations. Compound heterozygosity, where two different recessive alleles inherited from each parent lead to the expression of an autosomal recessive trait, poses a challenge in genetic diagnosis. Estimating the ancestry of these disease-associated variants, in conjunction with understanding the colonization history of admixed populations, can enhance the precision of association mapping in genetic studies. The aim of this study was to determine the ancestral origins of TYR and OCA2 mutations for OCA patients from two populations located in the Andes region of Colombia-Altiplano Cundiboyacense and Marinilla-Santuario. Comparison of OCA patients, and their unaffected relatives, with global reference populations showed a pattern of European and Native American admixture, with little African ancestry, for these two populations. Mutation-bearing TYR and OCA2 haplotypes from Colombian OCA patients were compared against haplotypes from Spanish, Native American, and Sephardic Jewish reference populations to infer their ancestral origins. For 12 OCA1 patients from the Altiplano Cundiboyacense region, 21 out of 24 mutated TYR haplotypes show Spanish origins, two show Native American origins, and one shows a Sephardic Jewish origin. The two Native American TYR haplotypes, and the single Sephardic Jewish haplotype, are all found in compound heterozygote patients, paired with the predominant Spanish TYR haplotype G47D. OCA in these three patients is a result of genetic admixture that brought together disease-causing mutations with distinct ancestral origins. Both OCA2 patients from the Marinilla-Santuario region show homozygous OCA2 mutations with a Spanish origin. These findings underscore the complexity of the genetic architecture of Mendelian disease in admixed American populations, with both consanguinity and admixture contributing to the risk of autosomal recessive OCA in Colombia.

Published
2024
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9. Transcriptome Analysis Identifies Tumor Immune Microenvironment Signaling Networks Supporting Metastatic Castration-Resistant Prostate Cancer

Author

Lawrence P. McKinney, Rajesh Singh, I. King Jordan, Sooryanarayana Varambally, Eric B. Dammer, and James W. Lillard

Subjects
transcriptomics, metastasis, tumor microenvironment, prostate cancer, signaling, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Prostate cancer (PCa) is the second most common cause of cancer death in American men. Metastatic castration-resistant prostate cancer (mCRPC) is the most lethal form of PCa and preferentially metastasizes to the bones through incompletely understood molecular mechanisms. Herein, we processed RNA sequencing data from patients with mCRPC (n = 60) and identified 14 gene clusters (modules) highly correlated with mCRPC bone metastasis. We used a novel combination of weighted gene co-expression network analysis (WGCNA) and upstream regulator and gene ontology analyses of clinically annotated transcriptomes to identify the genes. The cyan module (M14) had the strongest positive correlation (0.81, p = 4 × 10−15) with mCRPC bone metastasis. It was associated with two significant biological pathways through KEGG enrichment analysis (parathyroid hormone synthesis, secretion, and action and protein digestion and absorption). In particular, we identified 10 hub genes (ALPL, PHEX, RUNX2, ENPP1, PHOSPHO1, PTH1R, COL11A1, COL24A1, COL22A1, and COL13A1) using cytoHubba of Cytoscape. We also found high gene expression for collagen formation, degradation, absorption, cell-signaling peptides, and bone regulation processes through Gene Ontology (GO) enrichment analysis.

Published
2023
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10. Teacher Education for Sustainable Development: A Review of an Emerging Research Field

Author

Fischer, Daniel, King, Jordan, Rieckmann, Marco, Barth, Matthias, Büssing, Alexander, Hemmer, Ingrid, and Lindau-Bank, Detlev

Abstract

Teacher Education for Sustainable Development (TESD) is a niche innovation in teacher education that empowers teachers to prepare learners to address global socio-environmental challenges. To advance the diffusion of this niche innovation into general teacher education, this article offers a systematic literature review based on a qualitative analysis of 158 peer-reviewed publications on TESD research. Our results show that TESD research is a growing field characterized by five types of inquiry: designing learning environments, understanding learner attributes, measuring learning outcomes, promoting systems change, and advancing visions for the field. Major innovation potentials of TESD for more general teacher education are its emphasis on the grand socio-environmental challenges of our times, methodologies to engage with knowledge diversity (e.g., inter/transdisciplinarity), and sustainability science learning approaches (e.g., backcasting). We suggest that future work builds from this review to strengthen links between teacher education and TESD in enhancing quality education.

Published
2022
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11. Sick individuals, sick populations revisited: a test of the Rose hypothesis for type 2 diabetes disparities

Author

I King Jordan and Leonardo Mariño-Ramírez

Subjects
Public aspects of medicine, RA1-1270
Abstract

Introduction The Rose hypothesis predicts that since genetic variation is greater within than between populations, genetic risk factors will be associated with individuals’ risk of disease but not population disparities, and since socioenvironmental variation is greater between than within populations, socioenvironmental risk factors will be associated with population disparities but not individuals’ disease risk.Methods We used the UK Biobank to test the Rose hypothesis for type 2 diabetes (T2D) ethnic disparities in the UK. Our cohort consists of 26 912 participants from Asian, black and white ethnic groups. Participants were characterised as T2D cases or controls based on the presence or absence of T2D diagnosis codes in electronic health records. T2D genetic risk was measured using a polygenic risk score (PRS), and socioeconomic deprivation was measured with the Townsend Index (TI). The variation of genetic (PRS) and socioeconomic (TI) risk factors within and between ethnic groups was calculated using analysis of variance. Multivariable logistic regression was used to associate PRS and TI with T2D cases, and mediation analysis was used to analyse the effect of PRS and TI on T2D ethnic group disparities.Results T2D prevalence differs for Asian 23.34% (OR=5.14, CI=4.68 to 5.65), black 16.64% (OR=3.81, CI=3.44 to 4.22) and white 7.35% (reference) ethnic groups in the UK. Both genetic and socioenvironmental T2D risk factors show greater within (w) than between (b) ethnic group variation: PRS w=64.60%, b=35.40%; TI w=71.18%, b=28.19%. Nevertheless, both genetic risk (PRS OR=1.96, CI=1.87 to 2.07) and socioeconomic deprivation (TI OR=1.09, CI=1.08 to 1.10) are associated with T2D individual risk and mediate T2D ethnic disparities (Asian PRS=22.5%, TI=9.8%; black PRS=32.0%, TI=25.3%).Conclusion A relative excess of within-group versus between-group variation does not preclude T2D risk factors from contributing to T2D ethnic disparities. Our results support an integrative approach to health disparities research that includes both genetic and socioenvironmental risk factors.

Published
2023
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13. Investigation of hypertension and type 2 diabetes as risk factors for dementia in the All of Us cohort

Author

Shashwat Deepali Nagar, Priscilla Pemu, Jun Qian, Eric Boerwinkle, Mine Cicek, Cheryl R. Clark, Elizabeth Cohn, Kelly Gebo, Roxana Loperena, Kelsey Mayo, Stephen Mockrin, Lucila Ohno-Machado, Andrea H. Ramirez, Sheri Schully, Ashley Able, Ashley Green, Stephan Zuchner, SEEC Consortium, I. King Jordan, and Robert Meller

Subjects
Medicine, Science
Abstract

Abstract The World Health Organization recently defined hypertension and type 2 diabetes (T2D) as modifiable comorbidities leading to dementia and Alzheimer’s disease. In the United States (US), hypertension and T2D are health disparities, with higher prevalence seen for Black and Hispanic minority groups compared to the majority White population. We hypothesized that elevated prevalence of hypertension and T2D risk factors in Black and Hispanic groups may be associated with dementia disparities. We interrogated this hypothesis using a cross-sectional analysis of participant data from the All of Us (AoU) Research Program, a large observational cohort study of US residents. The specific objectives of our study were: (1) to compare the prevalence of dementia, hypertension, and T2D in the AoU cohort to previously reported prevalence values for the US population, (2) to investigate the association of hypertension, T2D, and race/ethnicity with dementia, and (3) to investigate whether race/ethnicity modify the association of hypertension and T2D with dementia. AoU participants were recruited from 2018 to 2019 as part of the initial project cohort (R2019Q4R3). Participants aged 40–80 with electronic health records and demographic data (age, sex, race, and ethnicity) were included for analysis, yielding a final cohort of 125,637 individuals. AoU participants show similar prevalence of hypertension (32.1%) and T2D (13.9%) compared to the US population (32.0% and 10.5%, respectively); however, the prevalence of dementia for AoU participants (0.44%) is an order of magnitude lower than seen for the US population (5%). AoU participants with dementia show a higher prevalence of hypertension (81.6% vs. 31.9%) and T2D (45.9% vs. 11.4%) compared to non-dementia participants. Dominance analysis of a multivariable logistic regression model with dementia as the outcome shows that hypertension, age, and T2D have the strongest associations with dementia. Hispanic was the only race/ethnicity group that showed a significant association with dementia, and the association of sex with dementia was non-significant. The association of T2D with dementia is likely explained by concurrent hypertension, since > 90% of participants with T2D also had hypertension. Black race and Hispanic ethnicity interact with hypertension, but not T2D, to increase the odds of dementia. This study underscores the utility of the AoU participant cohort to study disease prevalence and risk factors. We do notice a lower participation of aged minorities and participants with dementia, revealing an opportunity for targeted engagement. Our results indicate that targeting hypertension should be a priority for risk factor modifications to reduce dementia incidence.

Published
2022
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14. Factors affecting assessment, uptake and adherence to physical activities in people with dementia : an inclusive approach

Author

Elliott-King, Jordan

Subjects
616.8, Dementia, Physical Acitvity, Diagnosis, Adherence, Exercise, Alzheimer's diseases
Abstract

Dementia is a growing problem worldwide. There is no available long term effective treatment and many cases of dementia remain undiagnosed. Within this context, appropriate, accurate and reliable cognitive assessments are important in informing the process of diagnosing dementia, and monitoring the effects of subsequent interventions. Previous research has often researched the journey of dementia in stages. This thesis, however, was guided by inclusivity, a concept applied to encapsulate the need for the inclusion of all individuals across the whole journey of dementia. Assessments utilised during diagnostics should be cross-culturally applicable, easy and quick to administer, inexpensive, non-invasive and able to identify changes in cognitive functioning. Little research has explored cognitive assessments for people with intellectual disabilities, a growing group at high risk for experiencing dementia at a younger age. Moreover, physical activity could be a key intervention for people with dementia, with the potential to slow cognitive symptoms and promote independence. However, meta-analyses show mixed outcomes for the success of physical activity interventions. This may partly be due to low levels of engagement and adherence. Therefore, both cognitive assessments and physical activity, including factors influencing adherence, are important aspects of the journey of dementia, which require more research with an inclusive approach. This thesis was divided into 2 parts to reflect the underpinning paradigms that informed the investigations in each part. Hence, a mixed methods approach is used to investigate more inclusive practices in dementia diagnostics, intervention assessment and delivery of physical activity. Applied quantitative methods were used in part 1 to assess the accuracy of a battery of cognitive assessments (Mini Mental State Examination or MMSE, Hopkins Verbal Learning Test or HVLT, Verbal Fluency or VF, and the novel: Cognitive Computerized Test Battery for Individuals with Intellectual Disabilities or CCIID) in informing dementia diagnostics for individuals with (n=30) and without (n=25) intellectual disabilities (chapters 4 and 5). The same cognitive tests were then utilised to assess the acute effects of a physical activity intervention compared to a psychosocial control activity using a cross-over design involving people with dementia (chapter 6). The second part of the thesis informed by critical realism, but continuing the inclusive approach began by exploring the barriers and facilitators to physical activity for people with dementia (chapter 7). Novel mobile methods of interviewing were applied to explore the perspectives of people with dementia towards physical activity (chapter 8). These walking interviews were also discussed in comparison to more traditional seated interviews for their application in understanding the perspectives of people with demenita. This was only the second study to conduct walking interviews with people who have dementia, but the first to discuss physical activity within this context. Chapter 9 then sought to investigate the perspectives of professionals who work to provide physical activity for and with people who have dementia. This study investigated how professionals navigate barriers and facilitate adherence to physical activity for people with dementia within the community, and hence offers a discussion of practical solutions to barriers identified in the literature and from interviews with people with dementia. The findings from the initial investigations in this thesis showed that participants with and without a pre-existing cognitive impairment who had dementia scored significantly lower on all included cognitive assessments (MMSE, VF, HVLT, Series and Jigsaw subtests and total CCIID) than their age-matched counterparts. Receiver Operating Characteristic analysis revealed that all included assessments significantly classified those who had dementia, with a high accuracy of above 0.80 for all assessments with all populations. Assessments were well tolerated by all participants, including those with an intellectual disability. Acute cognitive benefits of physical activity were demonstrated over and above a psychosocial control using an order balanced cross-over design. An increase in cognitive scores was visible on the MMSE, VF, HVLT, Series and Jigsaw subtests and total CCIID after engaging in a short bout of resistance band physical activity versus a bingo (psychosocial) activity. This study confirms earlier research with resistance band physical activities in promoting memory in older people with and without dementia, but adds another new sensitive planning and logical reasoning test (CCIID) which could be important for early stages- or different types- of dementia. This study shows that the same well tolerated cognitive tests can be used for the initial screening and subsequent assessment of interventions. Systematic literature review (chapter 7) revealed that people with dementia have problems adhering to regular physical activity. The following thematic analysis of walking interview data with people who have dementia in chapter 8 revealed four key themes as to why this might be. The themes were: i) competition, ii) physical activity across the lifespan, iii) injury and decline; and iv) barriers to physical activity. The themes indicated that competitive aspects of physical activities can be encouraging or discouraging depending upon the individual participating, by giving the activity purpose, whether this is through competition or an activity goal, more people with dementia are interested in repeatedly engaging. Furthermore, injuries and decline in physical functioning frequently impacted participants' ability to enjoy physical activity. This often led to adapted physical activities rather than traditional sports that participants described enjoying earlier on in their lives. Each participant also discussed different logistical barriers outside of physical capabilities that limited their consistent participation in physical activity. The final study of the thesis, in chapter 9, analysed interviews with professionals, and offered methods of navigating the barriers highlighted by people with dementia; and discussed the potential for professional engagement with dementia care to increase physical activity participation and inclusively deliver interventions. This often meant providing a personalised activity that includes social interaction for the participants to further engage with, and benefit from. The professionals discussed the structure of the context in which physical activity is provided for people with dementia. Overall, this thesis argues for inclusive practices for people with dementia regardless of pre-existing cognitive ability, from diagnosis through to strategies for sustaining interventions that could offer substantial benefits. The empirical chapters are potentially limited by the small numbers of participants per study (n=9-25). However, this also allowed for in-depth analyses. The findings demonstrate the need for increased communication between healthcare professionals and people with dementia to offer more inclusive practices that can give greater insight into our understanding of dementia, as well as offer better care throughout the journey of dementia for all individuals.

Published
2019
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15. Factors associated with antihypertensive monotherapy among US adults with treated hypertension and uncontrolled blood pressure overall and by race/ethnicity, National Health and Nutrition Examination Survey 2013-2018

Author

Zheutlin, Alexander R., Derington, Catherine G., King, Jordan B., Berchie, Ransmond O., Herrick, Jennifer S., Dixon, Dave L., Cohen, Jordana B., Shimbo, Daichi, Kronish, Ian M., Saseen, Joseph J., Muntner, Paul, Moran, Andrew E., and Bress, Adam P.

Published
2022
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16. Ethnic disparities in mortality and group-specific risk factors in the UK Biobank.

Author

Kara Keun Lee, Emily T Norris, Lavanya Rishishwar, Andrew B Conley, Leonardo Mariño-Ramírez, John F McDonald, and I King Jordan

Subjects
Public aspects of medicine, RA1-1270
Abstract

Despite a substantial overall decrease in mortality, disparities among ethnic minorities in developed countries persist. This study investigated mortality disparities and their associated risk factors for the three largest ethnic groups in the United Kingdom: Asian, Black, and White. Study participants were sampled from the UK Biobank (UKB), a prospective cohort enrolled between 2006 and 2010. Genetics, biological samples, and health information and outcomes data of UKB participants were downloaded and data-fields were prioritized based on participants with death registry records. Kaplan-Meier method was used to evaluate survival differences among ethnic groups; survival random forest feature selection followed by Cox proportional-hazard modeling was used to identify and estimate the effects of shared and ethnic group-specific mortality risk factors. The White ethnic group showed significantly worse survival probability than the Asian and Black groups. In all three ethnic groups, endoscopy and colonoscopy procedures showed significant protective effects on overall mortality. Asian and Black women show lower relative risk of mortality than men, whereas no significant effect of sex was seen for the White group. The strongest ethnic group-specific mortality associations were ischemic heart disease for Asians, COVID-19 for Blacks, and cancers of respiratory/intrathoracic organs for Whites. Mental health-related diagnoses, including substance abuse, anxiety, and depression, were a major risk factor for overall mortality in the Asian group. The effect of mental health on Asian mortality, particularly for digestive cancers, was exacerbated by an observed hesitance to answer mental health questions, possibly related to cultural stigma. C-reactive protein (CRP) serum levels were associated with both overall and cause-specific mortality due to COVID-19 and digestive cancers in the Black group, where elevated CRP has previously been linked to psychosocial stress due to discrimination. Our results point to mortality risk factors that are group-specific and modifiable, supporting targeted interventions towards greater health equity.

Published
2023
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18. Race, Ethnicity, and Pharmacogenomic Variation in the United States and the United Kingdom

Author

Shivam Sharma, Leonardo Mariño-Ramírez, and I. King Jordan

Subjects
pharmacogenetics, human genome, health disparities, genetic ancestry, race, ethnicity, Pharmacy and materia medica, RS1-441
Abstract

The relevance of race and ethnicity to genetics and medicine has long been a matter of debate. An emerging consensus holds that race and ethnicity are social constructs and thus poor proxies for genetic diversity. The goal of this study was to evaluate the relationship between race, ethnicity, and clinically relevant pharmacogenomic variation in cosmopolitan populations. We studied racially and ethnically diverse cohorts of 65,120 participants from the United States All of Us Research Program (All of Us) and 31,396 participants from the United Kingdom Biobank (UKB). Genome-wide patterns of pharmacogenomic variation—6311 drug response-associated variants for All of Us and 5966 variants for UKB—were analyzed with machine learning classifiers to predict participants’ self-identified race and ethnicity. Pharmacogenomic variation predicts race/ethnicity with averages of 92.1% accuracy for All of Us and 94.3% accuracy for UKB. Group-specific prediction accuracies range from 99.0% for the White group in UKB to 92.9% for the Hispanic group in All of Us. Prediction accuracies are substantially lower for individuals who identified with more than one group in All of Us (16.7%) or as Mixed in UKB (70.7%). There are numerous individual pharmacogenomic variants with large allele frequency differences between race/ethnicity groups in both cohorts. Frequency differences for toxicity-associated variants predict hundreds of adverse drug reactions per 1000 treated participants for minority groups in All of Us. Our results indicate that race and ethnicity can be used to stratify pharmacogenomic risk in the US and UK populations and should not be discounted when making treatment decisions. We resolve the contradiction between the results reported here and the orthodoxy of race and ethnicity as non-genetic, social constructs by emphasizing the distinction between global and local patterns of human genetic diversity, and we stress the current and future limitations of race and ethnicity as proxies for pharmacogenomic variation.

Published
2023
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20. Genomic characterization and computational phenotyping of nitrogen-fixing bacteria isolated from Colombian sugarcane fields

Author

Luz K. Medina-Cordoba, Aroon T. Chande, Lavanya Rishishwar, Leonard W. Mayer, Lina C. Valderrama-Aguirre, Augusto Valderrama-Aguirre, John Christian Gaby, Joel E. Kostka, and I. King Jordan

Subjects
Medicine, Science
Abstract

Abstract Previous studies have shown the sugarcane microbiome harbors diverse plant growth promoting microorganisms, including nitrogen-fixing bacteria (diazotrophs), which can serve as biofertilizers. The genomes of 22 diazotrophs from Colombian sugarcane fields were sequenced to investigate potential biofertilizers. A genome-enabled computational phenotyping approach was developed to prioritize sugarcane associated diazotrophs according to their potential as biofertilizers. This method selects isolates that have potential for nitrogen fixation and other plant growth promoting (PGP) phenotypes while showing low risk for virulence and antibiotic resistance. Intact nitrogenase (nif) genes and operons were found in 18 of the isolates. Isolates also encode phosphate solubilization and siderophore production operons, and other PGP genes. The majority of sugarcane isolates showed uniformly low predicted virulence and antibiotic resistance compared to clinical isolates. Six strains with the highest overall genotype scores were experimentally evaluated for nitrogen fixation, phosphate solubilization, and the production of siderophores, gibberellic acid, and indole acetic acid. Results from the biochemical assays were consistent and validated computational phenotype predictions. A genotypic and phenotypic threshold was observed that separated strains by their potential for PGP versus predicted pathogenicity. Our results indicate that computational phenotyping is a promising tool for the assessment of bacteria detected in agricultural ecosystems.

Published
2021
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21. Psychological formulation in residential teams working with people with dementia : an exploration of multidisciplinary views using Q-methodology

Author

King, Jordan Matthew

Subjects
616.8
Abstract

Psychologists are encouraged to integrate their practice more closely within multidisciplinary mental health teams, whilst maintaining their professional identity (Onyett, 2007). The Team Formulation approach is one solution; this aims to provide a protected thinking space for a group staff to construct a shared understanding of a service user’s difficulties which guides intervention planning (Johnstone, 2014). However, it requires some initial investment from services. Chapter one investigated the evidence relating to the use and effects of team formulation in secondary mental healthcare. Eleven papers were systematically critiqued. A synthesis of findings revealed that whilst team formulations had no direct impact on clinical outcomes, they helped promote psychological thinking and facilitated better working alliances with service users. Several quantitative studies minimised bias through control groups and randomised designs, although practicebased evidence may have overstated effects due to a lack of methodological rigour. To address the identified gaps and limitations of the literature, chapter two describes a Q methodology study exploring multidisciplinary views on formulating with teams in dementia care settings. Participants ranked the relative importance of various aspects of sessions, and elaborated on their views through a semistructured interview. Results indicated three shared viewpoints regarding what was most valued about a team formulation approach, namely: Working together to identify residents’ unmet needs; Prioritising the needs of the resident versus those of the team; and Being heard – Valuing the relationship between the facilitating clinician and team. Viewpoints were explored in terms of their implications for clinical practice, including supporting residential teams to process the emotional impact of their work in addition to maintaining a focus on residents’ individual needs. Finally, chapter three provides a first person reflective account of the process of completing this thesis, and it’s impact on the personal and professional development of the author.

Published
2016

22. Explaining Housing Policy Change through Discursive Institutionalism.

Author

King, Jordan Carnaby

Subjects
*HOUSING, *HOUSING policy, *HISTORICAL institutionalism (Sociology), *POLITICAL science, *POLITICAL sociology
Abstract

Explaining how and why housing policies change is an ongoing theoretical challenge for housing scholars. A key approach is the 'housing regimes' framework (Kemeny 2006), drawing from Esping-Andersen's work on the role of labour/capital struggles in shaping welfare states. However, this framework has been criticised (Stephens 2020; Clapham 2020) for inadequately explaining housing system changes, including neoliberal shifts and financialization. In response, scholars have turned to political science and sociology theories on policy change, such as historical institutionalism (Ruonavaara 2020) and discursive theories focusing on interactions between policy actors (Clapham 2018). This article builds on Clapham's discursive turn in housing studies by incorporating concepts from 'discursive institutionalism' (DI) (Schmidt 2008). DI explains policy change by examining the interplay of ideas, interactions, and power dynamics in a given policy field. DI provides a methodological framework for understanding how policy actors develop and use ideas to shape policies, while considering the influence of the institutional context and power relations. The aim of the article is to highlight the utility of DI as a framework for examining housing policy change. As a vehicle for doing so, an analysis of social housing policy change in New Zealand employing DI is provided for empirical reference. The article builds on Clapham's (2018) focus on discourse in housing studies, adding DI to the repertoire of conceptual frameworks available to researchers interested in the causal role of ideas and discourse in policy change processes. [ABSTRACT FROM AUTHOR]

Published
2024
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23. Student agency in a sustainability-oriented assessment process: exploring expansive learning in student-led rubric co-design.

Author

King, Jordan, Brundiers, Katja, and Fischer, Daniel

Subjects
*SUSTAINABILITY, *INTERACTIVE learning, *EDUCATIONAL evaluation, *EDUCATIONAL intervention, UNDERGRADUATE education
Abstract

Evolving conceptions of the purposes of higher education suggest the need for assessment practices that contribute to preparing students to navigate complex social-ecological challenges. Though shifts in assessment discourse have begun to respond to this need, further examination of the role of students in assessment processes is required. One strategy that has been highlighted is rubric co-design, in which students and instructors interactively deliberate assessment criteria. However, the literature shows that student voices are typically limited in these processes. To address this gap, this study advances a student-led rubric co-design process to promote student agency and learning. Principles from sustainability are applied to orient the activities of students in this approach by emphasizing the participative, normative and integrative features of the process. A formative intervention was conducted in an undergraduate course focused on professional skill development. Data were collected through individual and group reflections, with reflexive thematic analysis applied to develop themes that represented the ways that students navigated their experiences in the assessment process. Findings demonstrate the promise of the approach in enhancing student agency and promoting self-formation as emerging professionals, while articulating the phases and strategies that shape students' leading role in rubric co-design processes. [ABSTRACT FROM AUTHOR]

Published
2024
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25. Population structure and pharmacogenomic risk stratification in the United States

Author

Shashwat Deepali Nagar, Andrew B. Conley, and I. King Jordan

Subjects
Population genomics, Pharmacogenomics, Precision public health, Genetic ancestry, Race, Ethnicity, Biology (General), QH301-705.5
Abstract

Abstract Background Pharmacogenomic (PGx) variants mediate how individuals respond to medication, and response differences among racial/ethnic groups have been attributed to patterns of PGx diversity. We hypothesized that genetic ancestry (GA) would provide higher resolution for stratifying PGx risk, since it serves as a more reliable surrogate for genetic diversity than self-identified race/ethnicity (SIRE), which includes a substantial social component. We analyzed a cohort of 8628 individuals from the United States (US), for whom we had both SIRE information and whole genome genotypes, with a focus on the three largest SIRE groups in the US: White, Black (African-American), and Hispanic (Latino). Our approach to the question of PGx risk stratification entailed the integration of two distinct methodologies: population genetics and evidence-based medicine. This integrated approach allowed us to consider the clinical implications for the observed patterns of PGx variation found within and between population groups. Results Whole genome genotypes were used to characterize individuals’ continental ancestry fractions—European, African, and Native American—and individuals were grouped according to their GA profiles. SIRE and GA groups were found to be highly concordant. Continental ancestry predicts individuals’ SIRE with > 96% accuracy, and accordingly, GA provides only a marginal increase in resolution for PGx risk stratification. In light of the concordance between SIRE and GA, taken together with the fact that information on SIRE is readily available to clinicians, we evaluated PGx variation between SIRE groups to explore the potential clinical utility of race and ethnicity. PGx variants are highly diverged compared to the genomic background; 82 variants show significant frequency differences among SIRE groups, and genome-wide patterns of PGx variation are almost entirely concordant with SIRE. The vast majority of PGx variation is found within rather than between groups, a well-established fact for almost all genetic variants, which is often taken to argue against the clinical utility of population stratification. Nevertheless, analysis of highly differentiated PGx variants illustrates how SIRE partitions PGx variation based on groups’ characteristic ancestry patterns. These cases underscore the extent to which SIRE carries clinically valuable information for stratifying PGx risk among populations, albeit with less utility for predicting individual-level PGx alleles (genotypes), supporting the concept of population pharmacogenomics. Conclusions Perhaps most interestingly, we show that individuals who identify as Black or Hispanic stand to gain far more from the consideration of race/ethnicity in treatment decisions than individuals from the majority White population.

Published
2020
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26. Ancestry effects on type 2 diabetes genetic risk inference in Hispanic/Latino populations

Author

Aroon T. Chande, Lavanya Rishishwar, Andrew B. Conley, Augusto Valderrama-Aguirre, Miguel A. Medina-Rivas, and I. King Jordan

Subjects
Polygenic risk score (PRS), Genetic risk, Type 2 diabetes (T2D), Genetic ancestry, Population genetics, Hispanic/Latino (HL), Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background Hispanic/Latino (HL) populations bear a disproportionately high burden of type 2 diabetes (T2D). The ability to predict T2D genetic risk using polygenic risk scores (PRS) offers great promise for improved screening and prevention. However, there are a number of complications related to the accurate inference of genetic risk across HL populations with distinct ancestry profiles. We investigated how ancestry affects the inference of T2D genetic risk using PRS in diverse HL populations from Colombia and the United States (US). In Colombia, we compared T2D genetic risk for the Mestizo population of Antioquia to the Afro-Colombian population of Chocó, and in the US, we compared European-American versus Mexican-American populations. Methods Whole genome sequences and genotypes from the 1000 Genomes Project and the ChocoGen Research Project were used for genetic ancestry inference and for T2D polygenic risk score (PRS) calculation. Continental ancestry fractions for HL genomes were inferred via comparison with African, European, and Native American reference genomes, and PRS were calculated using T2D risk variants taken from multiple genome-wide association studies (GWAS) conducted on cohorts with diverse ancestries. A correction for ancestry bias in T2D risk inference based on the frequencies of ancestral versus derived alleles was developed and applied to PRS calculations in the HL populations studied here. Results T2D genetic risk in Colombian and US HL populations is positively correlated with African and Native American ancestry and negatively correlated with European ancestry. The Afro-Colombian population of Chocó has higher predicted T2D risk than Antioquia, and the Mexican-American population has higher predicted risk than the European-American population. The inferred relative risk of T2D is robust to differences in the ancestry of the GWAS cohorts used for variant discovery. For trans-ethnic GWAS, population-specific variants and variants with same direction effects across populations yield consistent results. Nevertheless, the control for bias in T2D risk prediction confirms that explicit consideration of genetic ancestry can yield more reliable cross-population genetic risk inferences. Conclusions T2D associations that replicate across populations provide for more reliable risk inference, and modeling population-specific frequencies of ancestral and derived risk alleles can help control for biases in PRS estimation.

Published
2020
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27. Admixture-enabled selection for rapid adaptive evolution in the Americas

Author

Emily T. Norris, Lavanya Rishishwar, Aroon T. Chande, Andrew B. Conley, Kaixiong Ye, Augusto Valderrama-Aguirre, and I. King Jordan

Subjects
Rapid adaptive evolution, Positive selection, Genetic ancestry, Admixture, Population genomics, Polygenic traits, Biology (General), QH301-705.5, Genetics, QH426-470
Abstract

Abstract Background Admixture occurs when previously isolated populations come together and exchange genetic material. We hypothesize that admixture can enable rapid adaptive evolution in human populations by introducing novel genetic variants (haplotypes) at intermediate frequencies, and we test this hypothesis through the analysis of whole genome sequences sampled from admixed Latin American populations in Colombia, Mexico, Peru, and Puerto Rico. Results Our screen for admixture-enabled selection relies on the identification of loci that contain more or less ancestry from a given source population than would be expected given the genome-wide ancestry frequencies. We employ a combined evidence approach to evaluate levels of ancestry enrichment at single loci across multiple populations and multiple loci that function together to encode polygenic traits. We find cross-population signals of African ancestry enrichment at the major histocompatibility locus on chromosome 6, consistent with admixture-enabled selection for enhanced adaptive immune response. Several of the human leukocyte antigen genes at this locus, such as HLA-A, HLA-DRB51, and HLA-DRB5, show independent evidence of positive selection prior to admixture, based on extended haplotype homozygosity in African populations. A number of traits related to inflammation, blood metabolites, and both the innate and adaptive immune system show evidence of admixture-enabled polygenic selection in Latin American populations. Conclusions The results reported here, considered together with the ubiquity of admixture in human evolution, suggest that admixture serves as a fundamental mechanism that drives rapid adaptive evolution in human populations.

Published
2020
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28. Mutations in SORL1 and MTHFDL1 possibly contribute to the development of Alzheimer's disease in a multigenerational Colombian Family.

Author

Johanna Alexandra Tejada Moreno, Andrés Villegas Lanau, Lucia Madrigal Zapata, Ana Yulied Baena Pineda, Juan Velez Hernandez, Omer Campo Nieto, Alejandro Soto Ospina, Pedronel Araque Marín, Lavanya Rishishwar, Emily T Norris, Aroon T Chande, I King Jordan, and Gabriel Bedoya Berrio

Subjects
Medicine, Science
Abstract

Alzheimer's disease (AD) is the most common cause of dementia in the elderly, affecting over 50 million people worldwide in 2020 and this number will triple to 152 million by 2050. Much of the increase will be in developing countries like Colombia. In familial forms, highly penetrant mutations have been identified in three genes, APP, PSEN1, and PSEN2, supporting a role for amyloid-β peptide. In sporadic forms, more than 30 risk genes involved in the lipid metabolism, the immune system, and synaptic functioning mechanisms. We used whole-exome sequencing (WES) to evaluate a family of 97 members, spanning three generations, with a familiar AD, and without mutations in APP, PSEN1, or PSEN2. We sequenced two affected and one unaffected member with the aim of identifying genetic variants that could explain the presence of the disease in the family and the candidate variants were validated in eleven members. We also built a structural model to try to determine the effect on protein function. WES analysis identified two rare variants in SORL1 and MTHFD1L genes segregating in the family with other potential risk variants in APOE, ABCA7, and CHAT, suggesting an oligogenic inheritance. Additionally, the structural 3D models of SORL1 and MTHFD1L variants shows that these variants produce polarity changes that favor hydrophobic interactions, resulting in local structural changes that could affect the protein function and may contribute to the development of the disease in this family.

Published
2022
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30. Genome-Enabled Molecular Subtyping and Serotyping for Shiga Toxin-Producing Escherichia coli

Author

Sung B. Im, Sonali Gupta, Mani Jain, Aroon T. Chande, Heather A. Carleton, I. King Jordan, and Lavanya Rishishwar

Subjects
foodborne surveillance, PulseNet, machine learning, random forest, pulsed-field gel electrophoresis (PFGE), Nutrition. Foods and food supply, TX341-641, Food processing and manufacture, TP368-456
Abstract

Foodborne pathogens are a major public health burden in the United States, leading to 9.4 million illnesses annually. Since 1996, a national laboratory-based surveillance program, PulseNet, has used molecular subtyping and serotyping methods with the aim to reduce the burden of foodborne illness through early detection of emerging outbreaks. PulseNet affiliated laboratories have used pulsed-field gel electrophoresis (PFGE) and immunoassays to subtype and serotype bacterial isolates. Widespread use of serotyping and PFGE for foodborne illness surveillance over the years has resulted in the accumulation of a wealth of routine surveillance and outbreak epidemiological data. This valuable source of data has been used to understand seasonal frequency, geographic distribution, demographic information, exposure information, disease severity, and source of foodborne isolates. In 2019, PulseNet adopted whole genome sequencing (WGS) at a national scale to replace PFGE with higher-resolution methods such as the core genome multilocus sequence typing. Consequently, PulseNet's recent shift to genome-based subtyping methods has rendered the vast collection of historic surveillance data associated with serogroups and PFGE patterns potentially unusable. The goal of this study was to develop a bioinformatics method to associate the WGS data that are currently used by PulseNet for bacterial pathogen subtyping to previously characterized serogroup and PFGE patterns. Previous efforts to associate WGS to PFGE patterns relied on predicting DNA molecular weight based on restriction site analysis. However, these approaches failed owing to the non-uniform usage of genomic restriction sites by PFGE restriction enzymes. We developed a machine learning approach to classify isolates to their most probable serogroup and PFGE pattern, based on comparisons of genomic k-mer signatures. We applied our WGS classification method to 5,970 Shiga toxin-producing Escherichia coli (STEC) isolates collected as part of PulseNet's routine foodborne surveillance activities between 2003 and 2018. Our machine learning classifier is able to associate STEC WGS to higher-level serogroups with very high accuracy and lower-level PFGE patterns with somewhat lower accuracy. Taken together, these classifications support the ability of public health investigators to associate currently generated WGS data with historical epidemiological knowledge linked to serogroups and PFGE patterns in support of outbreak surveillance for food safety and public health.

Published
2021
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31. Genetic ancestry and ethnic identity in Ecuador

Author

Shashwat Deepali Nagar, Andrew B. Conley, Aroon T. Chande, Lavanya Rishishwar, Shivam Sharma, Leonardo Mariño-Ramírez, Gabriela Aguinaga-Romero, Fabricio González-Andrade, and I. King Jordan

Subjects
genetic ancestry, ethnicity, Ecuador, Latin America, population genetics, genomics, Genetics, QH426-470
Abstract

Summary: We investigated the ancestral origins of four Ecuadorian ethnic groups—Afro-Ecuadorian, Mestizo, Montubio, and the Indigenous Tsáchila—in an effort to gain insight on the relationship between ancestry, culture, and the formation of ethnic identities in Latin America. The observed patterns of genetic ancestry are largely concordant with ethnic identities and historical records of conquest and colonization in Ecuador. Nevertheless, a number of exceptional findings highlight the complex relationship between genetic ancestry and ethnicity in Ecuador. Afro-Ecuadorians show far less African ancestry, and the highest levels of Native American ancestry, seen for any Afro-descendant population in the Americas. Mestizos in Ecuador show high levels of Native American ancestry, with substantially less European ancestry, despite the relatively low Indigenous population in the country. The recently recognized Montubio ethnic group is highly admixed, with substantial contributions from all three continental ancestries. The Tsáchila show two distinct ancestry subgroups, with most individuals showing almost exclusively Native American ancestry and a smaller group showing a Mestizo characteristic pattern. Considered together with historical data and sociological studies, our results indicate the extent to which ancestry and culture interact, often in unexpected ways, to shape ethnic identity in Ecuador.

Published
2021
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32. Comparing Genetic and Socioenvironmental Contributions to Ethnic Differences in C-Reactive Protein

Author

Shashwat Deepali Nagar, Andrew B. Conley, Shivam Sharma, Lavanya Rishishwar, I. King Jordan, and Leonardo Mariño-Ramírez

Subjects
C-reacitve protein, inflammation, race and ethnicity (minority issues), health disparities, genetic ancestry, socioeconomic stages, Genetics, QH426-470
Abstract

C-reactive protein (CRP) is a routinely measured blood biomarker for inflammation. Elevated levels of circulating CRP are associated with response to infection, risk for a number of complex common diseases, and psychosocial stress. The objective of this study was to compare the contributions of genetic ancestry, socioenvironmental factors, and inflammation-related health conditions to ethnic differences in C-reactive protein levels. We used multivariable regression to compare CRP blood serum levels between Black and White ethnic groups from the United Kingdom Biobank (UKBB) prospective cohort study. CRP serum levels are significantly associated with ethnicity in an age and sex adjusted model. Study participants who identify as Black have higher average CRP than those who identify as White, CRP increases with age, and females have higher average CRP than males. Ethnicity and sex show a significant interaction effect on CRP. Black females have higher average CRP levels than White females, whereas White males have higher average CRP than Black males. Significant associations between CRP, ethnicity, and genetic ancestry are almost completely attenuated in a fully adjusted model that includes socioenvironmental factors and inflammation-related health conditions. BMI, smoking, and socioeconomic deprivation all have high relative effects on CRP. These results indicate that socioenvironmental factors contribute more to CRP ethnic differences than genetics. Differences in CRP are associated with ethnic disparities for a number of chronic diseases, including type 2 diabetes, essential hypertension, sarcoidosis, and lupus erythematosus. Our results indicate that ethnic differences in CRP are linked to both socioenvironmental factors and numerous ethnic health disparities.

Published
2021
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34. The Impact of Ethnicity and Genetic Ancestry on Disease Prevalence and Risk in Colombia

Author

Aroon T. Chande, Shashwat Deepali Nagar, Lavanya Rishishwar, Leonardo Mariño-Ramírez, Miguel A. Medina-Rivas, Augusto E. Valderrama-Aguirre, I. King Jordan, and Juan Esteban Gallo

Subjects
Colombia, Latin America, health disparities, precision medicine, ethnicity, genetic ancestry, Genetics, QH426-470
Abstract

Currently, the vast majority of genomic research cohorts are made up of participants with European ancestry. Genomic medicine will only reach its full potential when genomic studies become more broadly representative of global populations. We are working to support the establishment of genomic medicine in developing countries in Latin America via studies of ethnically and ancestrally diverse Colombian populations. The goal of this study was to analyze the effect of ethnicity and genetic ancestry on observed disease prevalence and predicted disease risk in Colombia. Population distributions of Colombia’s three major ethnic groups – Mestizo, Afro-Colombian, and Indigenous – were compared to disease prevalence and socioeconomic indicators. Indigenous and Mestizo ethnicity show the highest correlations with disease prevalence, whereas the effect of Afro-Colombian ethnicity is substantially lower. Mestizo ethnicity is mostly negatively correlated with six high-impact health conditions and positively correlated with seven of eight common cancers; Indigenous ethnicity shows the opposite effect. Malaria prevalence in particular is strongly correlated with ethnicity. Disease prevalence co-varies across geographic regions, consistent with the regional distribution of ethnic groups. Ethnicity is also correlated with regional variation in human development, partially explaining the observed differences in disease prevalence. Patterns of genetic ancestry and admixture for a cohort of 624 individuals from Medellín were compared to disease risk inferred via polygenic risk scores (PRS). African genetic ancestry is most strongly correlated with predicted disease risk, whereas European and Native American ancestry show weaker effects. African ancestry is mostly positively correlated with disease risk, and European ancestry is mostly negatively correlated. The relationships between ethnicity and disease prevalence do not show an overall correspondence with the relationships between ancestry and disease risk. We discuss possible reasons for the divergent health effects of ethnicity and ancestry as well as the implication of our results for the development of precision medicine in Colombia.

Published
2021
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35. Genomic Diversity of Azole-Resistant Aspergillus fumigatus in the United States

Author

Kizee A. Etienne, Elizabeth L. Berkow, Lalitha Gade, Natalie Nunnally, Shawn R. Lockhart, Karlyn Beer, I. King Jordan, Lavanya Rishishwar, and Anastasia P. Litvintseva

Subjects
azole resistance, Aspergillus fumigatus, whole-genome sequencing, population genomics, population structure, TR34/L98H, Microbiology, QR1-502
Abstract

ABSTRACT Azole resistance in pathogenic Aspergillus fumigatus has become a global public health issue threatening the use of medical azoles. The environmentally occurring resistance mutations, TR34/L98H (TR34) and TR46/Y121F/T289A (TR46), are widespread across multiple continents and emerging in the United States. We used whole-genome single nucleotide polymorphism (SNP) analysis on 179 nationally represented clinical and environmental A. fumigatus genomes from the United States along with 18 non-U.S. genomes to evaluate the genetic diversity and foundation of the emergence of azole resistance in the United States. We demonstrated the presence of clades of A. fumigatus isolates: clade A (17%) comprised a global collection of clinical and environmental azole-resistant strains, including all strains with the TR34/L98H allele from India, The Netherlands, the United Kingdom, and the United States, and clade B (83%) consisted of isolates without this marker mainly from the United States. The TR34/L98H polymorphism was shared among azole-resistant A. fumigatus strains from India, The Netherlands, the United Kingdom, and the United States, suggesting the common origin of this resistance mechanism. Six percent of azole-resistant A. fumigatus isolates from the United States with the TR34 resistance marker had a mixture of clade A and clade B alleles, suggestive of recombination. Additionally, the presence of equal proportions of both mating types further suggests the ongoing presence of recombination. This study demonstrates the genetic background for the emergence of azole resistance in the United States, supporting a single introduction and subsequent propagation, possibly through recombination of environmentally driven resistance mutations. IMPORTANCE Aspergillus fumigatus is one of the most common causes of invasive mold infections in patients with immune deficiencies and has also been reported in patients with severe influenza and severe acute respiratory syndrome coronavirus 2 (SARs-CoV-2). Triazole drugs are the first line of therapy for this infection; however, their efficacy has been compromised by the emergence of azole resistance in A. fumigatus, which was proposed to be selected for by exposure to azole fungicides in the environment [P. E. Verweij, E. Snelders, G. H. J. Kema, E. Mellado, et al., Lancet Infect Dis 9:789–795, 2009, https://doi.org/10.1016/S1473-3099(09)70265-8]. Isolates with environmentally driven resistance mutations, TR34/L98H (TR34) and TR46/Y121F/T289A (TR46), have been reported worldwide. Here, we used genomic analysis of a large sample of resistant and susceptible A. fumigatus isolates to demonstrate a single introduction of TR34 in the United States and suggest its ability to spread into the susceptible population is through recombination between resistant and susceptible isolates.

Published
2021
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36. Socioeconomic deprivation and genetic ancestry interact to modify type 2 diabetes ethnic disparities in the United Kingdom

Author

Shashwat Deepali Nagar, Anna María Nápoles, I. King Jordan, and Leonardo Mariño-Ramírez

Subjects
Medicine (General), R5-920
Abstract

Background: Type 2 diabetes (T2D) is a complex common disease that disproportionately impacts minority ethnic groups in the United Kingdom (UK). Socioeconomic deprivation (SED) is widely considered as a potential explanation for T2D ethnic disparities in the UK, whereas the effect of genetic ancestry (GA) on such disparities has yet to be studied. Methods: We leveraged data from the UK Biobank prospective cohort study, with participants enrolled between 2006 and 2010, to model the relationship between SED (Townsend index), GA (clustering principal components of whole genome genotype data), and T2D status (ICD-10 codes) across the three largest ethnic groups in the UK – Asian, Black, and White – using multivariable logistic regression. Findings: The Asian group shows the highest T2D prevalence (17·9%), followed by the Black (11·7%) and White (5·5%) ethnic groups. We find that both SED (OR: 1·11, 95% CI: 1·10–1·11) and non-European GA (OR South Asian versus European: 4·37, 95% CI: 4·10–4·66; OR African versus European: 2·52, 95% CI: 2·23–2·85) are significantly associated with the observed T2D disparities. GA and SED show significant interaction effects on T2D, with SED being a relatively greater risk factor for T2D for individuals with South Asian and African ancestry, compared to those with European ancestry. Interpretation: The significant interactions between SED and GA underscore how the effects of environmental risk factors can differ among ancestry groups, suggesting the need for group-specific interventions. Funding: This work was supported by the National Institutes of Health (NIH) Distinguished Scholars Program (DSP) to LMR and the Division of Intramural Research (DIR) of the National Institute on Minority Health and Health Disparities (NIMHD) at NIH.

Published
2021
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37. Analysis of Vibrio cholerae genomes identifies new type VI secretion system gene clusters

Author

Cristian V. Crisan, Aroon T. Chande, Kenneth Williams, Vishnu Raghuram, Lavanya Rishishwar, Gabi Steinbach, Samit S. Watve, Peter Yunker, I. King Jordan, and Brian K. Hammer

Subjects
Vibrio cholerae, Type VI secretion clusters, Bacterial toxins, Biology (General), QH301-705.5, Genetics, QH426-470
Abstract

Abstract Background Like many bacteria, Vibrio cholerae deploys a harpoon-like type VI secretion system (T6SS) to compete against other microbes in environmental and host settings. The T6SS punctures adjacent cells and delivers toxic effector proteins that are harmless to bacteria carrying cognate immunity factors. Only four effector/immunity pairs encoded on one large and three auxiliary gene clusters have been characterized from largely clonal, patient-derived strains of V. cholerae. Results We sequence two dozen V. cholerae strain genomes from diverse sources and develop a novel and adaptable bioinformatics tool based on hidden Markov models. We identify two new T6SS auxiliary gene clusters and describe Aux 5 here. Four Aux 5 loci are present in the host strain, each with an atypical effector/immunity gene organization. Structural prediction of the putative effector indicates it is a lipase, which we name TleV1 (type VI lipase effector Vibrio). Ectopic TleV1 expression induces toxicity in Escherichia coli, which is rescued by co-expression of the TliV1a immunity factor. A clinical V. cholerae reference strain expressing the Aux 5 cluster uses TleV1 to lyse its parental strain upon contact via its T6SS but is unable to kill parental cells expressing the TliV1a immunity factor. Conclusion We develop a novel bioinformatics method and identify new T6SS gene clusters in V. cholerae. We also show the TleV1 toxin is delivered in a T6SS manner by V. cholerae and can lyse other bacterial cells. Our web-based tool can be modified to identify additional novel T6SS genomic loci in diverse bacterial species.

Published
2019
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38. Development of anthracycline-induced dilated cardiomyopathy due to mutation on LMNA gene in a breast cancer patient: a case report

Author

Jock Chichaco Kuruc, Armando A. Durant-Archibold, Jorge Motta, K. S. Rao, Barry Trachtenberg, Carlos Ramos, Hongyu Wang, David Gorenstein, Fredrik Vannberg, and King Jordan

Subjects
Cardiotoxicity, Dilated cardiomyopathy, Antrhacyclines, LMNA gene, Breast cancer, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Background Anthracyclines are highly effective anticancer medication prescribed for the treatment of breast cancer. Nevertheless, the use of anthracyclines as chemotherapeutic agents involves a risk for development of cardiac toxicity which may cause restrictive and dilated cardiomyopathy. Currently, genetic predisposition is not considered as a risk factor for cardiotoxicity associated to the use of anthracyclines. Case presentation We report the case of a 37-years old Panamanian female patient diagnosed with breast cancer who developed clinical signs of severe heart failure after treatment with doxorubicin. A diagnosis of anthracycline induced cardiomyopathy was made and treatment was initiated accordingly. A whole exome sequencing study performed to the patient showed the presence of a missense mutation in LMNA gene, which codifies for lamin A/C. Our results points to a correlation between the LMNA variant and the anthracycline cardiotoxicity developed by the woman. Improvement of the clinical symptoms and the left ventricle ejection fraction was observed after proper treatment. Conclusions This case report suggests for the first time a potential genetic predisposition for anthracyclines induced cardiomyopathy in patients with mutations in LMNA gene. Perhaps chemotherapies accelerate or deliver the “second-hit” in the development of DCM in patients with genetic mutations. More data is needed to understand the contribution of LMNA variants that predispose to DCM in patients receiving cardiotoxic therapies.

Published
2019
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39. Just dance: Bulldog Pantry hosts dance marathon for hunger - The Collegian

Author

King, Jordan

Subjects
College students, News, opinion and commentary, Sports and fitness
Abstract

Byline: Jordan King Home is defined as 'where one lives.' While the word can be interpreted in multiple ways, Fresno is 'home' to every Fresno State student. As of 2011, [...]

Published
2023

40. Student opportunities - The Collegian

Author

King, Jordan

Subjects
College students, News, opinion and commentary, Sports and fitness
Abstract

Byline: Jordan King Saturday Sports Every Saturday morning from 10 a.m. to noon, participate in or lead sports, games and crafts at the Wesley United Methodist Church. For involvement information, [...]

Published
2023

41. What's new in ASI? - The Collegian

Author

King, Jordan

Subjects
Voter registration, College students, News, opinion and commentary, Sports and fitness
Abstract

Byline: Jordan King Get ready to stand up and speak out. November 6, 2012 is voting day. In celebration of National Voter Registration Day on Tuesday, Sept. 25, ASI will [...]

Published
2023

45. Colistin Heteroresistance Is Largely Undetected among Carbapenem-Resistant Enterobacterales in the United States

Author

Victor I. Band, Sarah W. Satola, Richard D. Smith, David A. Hufnagel, Chris Bower, Andrew B. Conley, Lavanya Rishishwar, Suzanne E. Dale, Dwight J. Hardy, Roberto L. Vargas, Ghinwa Dumyati, Marion A. Kainer, Erin C. Phipps, Rebecca Pierce, Lucy E. Wilson, Matthew Sorensen, Erik Nilsson, I. King Jordan, Eileen M. Burd, Monica M. Farley, Jesse T. Jacob, Robert K. Ernst, and David S. Weiss

Subjects
Microbiology, QR1-502
Abstract

Heteroresistance is an underappreciated phenomenon that may be the cause of some unexplained antibiotic treatment failures. Misclassification of heteroresistant isolates as susceptible may lead to inappropriate therapy.

Published
2021
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49. Genetic ancestry, admixture and health determinants in Latin America

Author

Emily T. Norris, Lu Wang, Andrew B. Conley, Lavanya Rishishwar, Leonardo Mariño-Ramírez, Augusto Valderrama-Aguirre, and I. King Jordan

Subjects
Genetic ancestry, Admixture, Ancestry-enrichment, Adaptive introgression, Health, Disease, Biotechnology, TP248.13-248.65, Genetics, QH426-470
Abstract

Abstract Background Modern Latin American populations were formed via genetic admixture among ancestral source populations from Africa, the Americas and Europe. We are interested in studying how combinations of genetic ancestry in admixed Latin American populations may impact genomic determinants of health and disease. For this study, we characterized the impact of ancestry and admixture on genetic variants that underlie health- and disease-related phenotypes in population genomic samples from Colombia, Mexico, Peru, and Puerto Rico. Results We analyzed a total of 347 admixed Latin American genomes along with 1102 putative ancestral source genomes from Africans, Europeans, and Native Americans. We characterized the genetic ancestry, relatedness, and admixture patterns for each of the admixed Latin American genomes, finding a spectrum of ancestry proportions within and between populations. We then identified single nucleotide polymorphisms (SNPs) with anomalous ancestry-enrichment patterns, i.e. SNPs that exist in any given Latin American population at a higher frequency than expected based on the population’s genetic ancestry profile. For this set of ancestry-enriched SNPs, we inspected their phenotypic impact on disease, metabolism, and the immune system. All four of the Latin American populations show ancestry-enrichment for a number of shared pathways, yielding evidence of similar selection pressures on these populations during their evolution. For example, all four populations show ancestry-enriched SNPs in multiple genes from immune system pathways, such as the cytokine receptor interaction, T cell receptor signaling, and antigen presentation pathways. We also found SNPs with excess African or European ancestry that are associated with ancestry-specific gene expression patterns and play crucial roles in the immune system and infectious disease responses. Genes from both the innate and adaptive immune system were found to be regulated by ancestry-enriched SNPs with population-specific regulatory effects. Conclusions Ancestry-enriched SNPs in Latin American populations have a substantial effect on health- and disease-related phenotypes. The concordant impact observed for same phenotypes across populations points to a process of adaptive introgression, whereby ancestry-enriched SNPs with specific functional utility appear to have been retained in modern populations by virtue of their effects on health and fitness.

Published
2018
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50. Thyroid Stimulating Hormone Stability in Patients Prescribed Synthetic or Desiccated Thyroid Products: A Retrospective Study

Author

Kuye, Rolake, Riggs, Catherine, King, Jordan, Heilmann, Rachel, Kurz, Deanna, and Milchak, Jessica

Subjects
Hypothyroidism -- Drug therapy -- Patient outcomes, Thyrotropin -- Statistics -- Health aspects, Biopharmaceuticals -- Comparative analysis -- Patient outcomes, Antithyroid agents -- Comparative analysis -- Patient outcomes, Health, Science and technology
Abstract

The purpose of this retrospective matched-cohort study was to evaluate the stability of thyroid stimulating hormone (TSH) in patients using synthetic compared with desiccated thyroid products. Patients using a thyroid product for the treatment of hypothyroidism were matched 1:1 on age, sex, race/ethnicity, and had a follow-up period of 3 years after the index date. The primary outcome was percent of in-range TSH values. Over 3 years, TSH values in both groups were inrange 79% of the time (P = 0.905). Our results showed no difference in longitudinal TSH stability between desiccated thyroid products and synthetic levothyroxine. Key words: thyroid stimulating hormone (TSH); levothyroxine; desiccated thyroid; stability; hypothyroidism; thyrotropin, thyroxine, thyroid (USP), INTRODUCTION Hypothyroidism is a common endocrine disorder that affects approximately 5% of the population. (1) Both synthetic and desiccated thyroid are used in the treatment of hypothyroidism. Synthetic levothyroxine ([T.sub.4]) [...]

Published
2020
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