12 results on '"Pike, Mindy M."'
Search Results
2. Abstract 18814: Glycoprotein VI is Critical for the Detection and Progression of Abdominal Aortic Aneurysms
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Benson, Tyler W, Pike, Mindy M, Spuzzillo, Anthony, Hicks, Sarah, Pham, Michael, Bhandari, Rohan, Brunner, Seth, Wadding-Lee, Caris, Conrad, Kelsey, Russell, Hannah, Coughlin, Taylor, Aggarwal, Anu, Lyden, Sean, Mani, Kevin, Bjorck, Martin Gustaf, Wanhainen, Anders, Mix, Doran S, Lipworth, Loren, Robinson Cohen, Cassianne, Shim, Sharon, Edwards, Todd I, Tranter, Michael, Gardiner, Elizabeth, Mackman, Nigel, Cameron, Scott J, and Owens, A. Phillip
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- 2023
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3. Supervised Exercise Intervention and Overall Activity in CKD
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Pike, Mindy M., Alsouqi, Aseel, Headley, Samuel A.E., Tuttle, Katherine, Evans, Elizabeth Elspeth, Milch, Charles M., Moody, Kelsey Anne, Germain, Michael, Stewart, Thomas G., Lipworth, Loren, Himmelfarb, Jonathan, Ikizler, T. Alp, and Robinson-Cohen, Cassianne
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- 2020
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4. Improvement in Cardiovascular Risk Prediction with Electronic Health Records
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Pike, Mindy M., Decker, Paul A., Larson, Nicholas B., St. Sauver, Jennifer L., Takahashi, Paul Y., Roger, Véronique L., Rocca, Walter A., Miller, Virginia M., Olson, Janet E., Pathak, Jyotishman, and Bielinski, Suzette J.
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- 2016
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5. Genetic Variants Associated With Systolic Blood Pressure in Children and Adolescents.
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Pike, Mindy M., Schildcrout, Jonathan, Baldwin, Scott, Edwards, Todd, Lipworth, Loren, and Robinson-Cohen, Cassianne
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- 2023
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6. Effects of caloric restriction and aerobic exercise on circulating cell-free mitochondrial DNA in patients with moderate to severe chronic kidney disease.
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Jaramillo-Morales, Javier, Korucu, Berfu, Pike, Mindy M., Lipworth, Loren, Stewart, Thomas, Headley, Samuel A. E., Germain, Michael, Begue, Gwenaelle, Roshanravan, Baback, Tuttle, Katherine R., Himmelfarb, Jonathan, Robinson-Cohen, Cassianne, Ikizler, T. Alp, and Gamboa, Jorge L.
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AEROBIC exercises ,LOW-calorie diet ,CHRONIC kidney failure ,GLOMERULAR filtration rate ,BODY mass index - Abstract
Circulating cell-free mitochondrial DNA (ccf-mtDNA) may induce systemic inflammation, a common condition in chronic kidney disease (CKD), by acting as a damage-associated molecular pattern. We hypothesized that in patients with moderate to severe CKD, aerobic exercise would reduce ccf-mtDNA levels. We performed a post hoc analysis of a multicenter randomized trial (NCT01150851) measuring plasma concentrations of ccf-mtDNA at baseline and 2 and 4 mo after aerobic exercise and caloric restriction. A total of 99 participants had baseline ccf-mtDNA, and 92 participants completed the study. The median age of the participants was 57 yr, 44% were female and 55% were male, 23% had diabetes, and 92% had hypertension. After adjusting for demographics, blood pressure, body mass index, diabetes, and estimated glomerular filtration rate, median ccf-mtDNA concentrations at baseline, 2 mo, and 4 mo were 3.62, 3.08, and 2.78 pM for the usual activity group and 2.01, 2.20, and 2.67 pM for the aerobic exercise group, respectively. A 16.1% greater increase per month in ccf-mtDNA was seen in aerobic exercise versus usual activity (P = 0.024), which was more pronounced with the combination of aerobic exercise and caloric restriction (29.5% greater increase per month). After 4 mo of intervention, ccf-mtDNA increased in the aerobic exercise group by 81.6% (95% confidence interval: 8.2-204.8, P = 0.024) compared with the usual activity group and was more marked in the aerobic exercise and caloric restriction group (181.7% increase, 95% confidence interval: 41.1-462.2, P = 0.003). There was no statistically significant correlation between markers of oxidative stress and inflammation with ccf-mtDNA. Our data indicate that aerobic exercise increased ccf-mtDNA levels in patients with moderate to severe CKD. [ABSTRACT FROM AUTHOR]
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- 2022
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7. Effects of diet and exercise on adipocytokine levels in patients with moderate to severe chronic kidney disease.
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Aydemir, Nihal, Pike, Mindy M., Alsouqi, Aseel, Headley, Samuel A.E., Tuttle, Katherine, Evans, Elizabeth E., Milch, Charles M., Moody, Kelsey A., Germain, Michael, Lipworth, Loren, Himmelfarb, Jonathan, Ikizler, T.A., and Robinson-Cohen, Cassianne
- Abstract
Background and Aims: Obesity is a pro-inflammatory risk factor for progression of CKD and cardiovascular disease. We hypothesized that implementation of caloric restriction and endurance exercise would improve adipocytokine profiles in patients with moderate to severe CKD.Methods and Results: We enrolled patients with moderate to severe CKD through a multi-center pilot randomized trial of diet and exercise in a 4-arm design (dietary restriction of 10%-15% reduction in caloric intake, exercise three times/week, combined diet and exercise, and control) (NCT01150851). Adipocytokines (adiponectin and leptin) were measured at the beginning and end of the study period as secondary outcomes. Treatment effect was analyzed in a multivariable model adjusted for baseline outcome values, age, gender, site and diabetes. A total of 122 participants were consented, 111 were randomized (42% female, 25% diabetic, and 91% hypertensive), 104 started intervention and 92 completed the study (Figure 1). Plasma adiponectin levels increased significantly in response to diet by 23% (95% CI: 0.2%, 49.8%, p = 0.048) among participants randomized to the caloric restriction and usual activity arm but not to exercise, whereas circulating leptin did not change by either treatment.Conclusion: Our data suggest that dietary caloric restriction increases plasma adiponectin levels in stage 3-4 CKD patients, with limited effect on leptin levels. These findings suggest the potential for improving the metabolic milieu of CKD with moderate calorie restriction. [ABSTRACT FROM AUTHOR]- Published
- 2020
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8. The Authors Reply
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Pike, Mindy M., Alsouqi, Aseel, Headley, Samuel A.E., Tuttle, Katherine, Evans, Elizabeth Elspeth, Milch, Charles M., Moody, Kelsey Anne, Germain, Michael, Stewart, Thomas G., Lipworth, Loren, Himmelfarb, Jonathan, Ikizler, T. Alp, and Robinson-Cohen, Cassianne
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- 2020
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9. ABO blood group is associated with peripheral arterial disease in African Americans: The Multi-Ethnic Study of Atherosclerosis (MESA).
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Pike, Mindy M., Larson, Nicholas B., Wassel, Christina L., Cohoon, Kevin P., Tsai, Michael Y., Pankow, James S., Hanson, Naomi Q., Decker, Paul A., Berardi, Cecilia, Alexander, Kristine S., Cushman, Mary, Zakai, Neil A., and Bielinski, Suzette J.
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ABO blood group system , *ARTERIAL diseases , *ATHEROSCLEROSIS , *DISEASE prevalence , *ALLELES - Abstract
Introduction Peripheral artery disease (PAD) affects 8.5 million Americans and thus improving our understanding of PAD is critical to developing strategies to reduce disease burden. The objective of the study was to determine the association of ABO blood type with ankle brachial index (ABI) as well as prevalent and incident PAD in a multi-ethnic cohort. Methods The Multi-Ethnic Study of Atherosclerosis includes non-Hispanic White, African, Hispanic, and Chinese Americans aged 45–84. ABO blood type was estimated using ABO genotypes in 6027 participants who had ABI assessed at the baseline exam. Associations with ABO blood type were evaluated categorically and under an additive genetic model by number of major ABO alleles. After excluding those with ABI > 1.4, prevalent PAD was defined as ABI ≤ 0.9 at baseline and incident PAD as ABI ≤ 0.9 for 5137 participants eligible for analysis. Results There were 222 prevalent cases and 239 incident cases of PAD. In African Americans, each additional copy of the A allele was associated with a 0.02 lower baseline ABI ( p = 0.006). Each copy of the A allele also corresponded to 1.57-fold greater odds of prevalent PAD (95% CI, 1.17–2.35; p = 0.004), but was not associated with incident PAD. No associations were found in other racial/ethnic groups for ABI, prevalent PAD, or incident PAD across all races/ethnicities. Conclusions Blood type A and the A allele count were significantly associated with baseline ABI and prevalent PAD in African Americans. Further research is needed to confirm and study the mechanisms of this association in African Americans. [ABSTRACT FROM AUTHOR]
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- 2017
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10. Glycoprotein VI is Critical for the Detection and Progression of Abdominal Aortic Aneurysms.
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Benson TW, Pike MM, Spuzzillo A, Hicks SM, Pham M, Mix DS, Brunner SI, Wadding-Lee C, Conrad KA, Russell HM, Jennings C, Coughlin TM, Aggarwal A, Lyden S, Mani K, Björck M, Wanhainen A, Bhandari R, Lipworth-Elliot L, Robinson-Cohen C, Caputo FJ, Shim S, Edwards TL, Tranter M, Gardiner EE, Mackman N, Cameron SJ, and Owens AP
- Abstract
A common feature in patients with abdominal aortic aneurysms (AAA) is the formation of a nonocclusive intraluminal thrombus (ILT) in regions of aortic dilation. Platelets are known to maintain hemostasis and propagate thrombosis through several redundant activation mechanisms, yet the role of platelet activation in the pathogenesis of AAA associated ILT is still poorly understood. Thus, we sought to investigate how platelet activation impacts the pathogenesis of AAA. Using RNA-sequencing, we identify that the platelet-associated transcripts are significantly enriched in the ILT compared to the adjacent aneurysm wall and healthy control aortas. We found that the platelet specific receptor glycoprotein VI (GPVI) is among the top enriched genes in AAA ILT and is increased on the platelet surface of AAA patients. Examination of a specific indicator of platelet activity, soluble GPVI (sGPVI), in two independent AAA patient cohorts is highly predictive of a AAA diagnosis and associates more strongly with aneurysm growth rate when compared to D-dimer in humans. Finally, intervention with the anti-GPVI antibody (J) in mice with established aneurysms blunted the progression of AAA in two independent mouse models. In conclusion, we show that levels of sGPVI in humans can predict a diagnosis of AAA and AAA growth rate, which may be critical in the identification of high-risk patients. We also identify GPVI as a novel platelet-specific AAA therapeutic target, with minimal risk of adverse bleeding complications, where none currently exist., Key Points: Soluble glycoprotein VI, which is a platelet-derived blood biomarker, predicts a diagnosis of AAA, with high sensitivity and specificity in distinguishing patients with fast from slow-growing AAA.Blockade of glycoprotein VI in mice with established aneurysms reduces AAA progression and mortality, indicating therapeutic potential.
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- 2023
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11. Genetic Determinants of IL-6 Levels and Risk of ESKD.
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Wheless L, Pike MM, Chen HC, Yu Z, Tao R, Bick A, Chung CP, Robinson-Cohen C, and Hung A
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- Humans, Risk Factors, Interleukin-6, Kidney Failure, Chronic
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- 2023
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12. Association of Genetically Predicted Fibroblast Growth Factor-23 with Heart Failure: A Mendelian Randomization Study.
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Akwo E, Pike MM, Ertuglu LA, Vartanian N, Farber-Eger E, Lipworth L, Perwad F, Siew E, Hung A, Bansal N, de Boer I, Kestenbaum B, Cox NJ, Ikizler TA, Wells Q, and Robinson-Cohen C
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- Fibroblast Growth Factors genetics, Genome-Wide Association Study, Humans, Mendelian Randomization Analysis, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic genetics, Fibroblast Growth Factor-23 genetics, Heart Failure complications, Heart Failure epidemiology, Heart Failure genetics
- Abstract
Background and Objectives: Elevated fibroblast growth factor-23 (FGF23) has been consistently associated with heart failure, particularly heart failure with preserved ejection fraction, among patients with CKD and in the general population. FGF23 may directly induce cardiac remodeling and heart failure. However, biases affecting observational studies impede robust causal inferences. Mendelian randomization leverages genetic determinants of a risk factor to examine causality. We performed a two-sample Mendelian randomization to assess causal associations between FGF23 and heart failure., Design, Setting, Participants, & Measurements: Genetic instruments were genome-wide significant genetic variants associated with FGF23, including variants near PIP5K1B , RGS14 , LINC01229 , and CYP24A1. We analyzed data from the Heart Failure Molecular Epidemiology for Therapeutic Targets and BioVU biobanks to examine associations of the four variants with overall heart failure, heart failure with preserved ejection fraction, and heart failure with reduced and mid-range ejection fraction. We developed an eGFR polygenic risk score using summary statistics from the Chronic Kidney Disease Genetics Consortium (CKDGen) genome-wide association study of eGFR in >1 million individuals and performed stratified analyses across eGFR polygenic risk score strata., Results: Genetically determined FGF23 was not associated with overall heart failure in the Heart Failure Molecular Epidemiology for Therapeutic Targets consortium (odds ratio, 1.13; 95% confidence interval, 0.89 to 1.42 per unit higher genetically predicted log FGF23) and the full BioVU sample (odds ratio, 1.32; 95% confidence interval, 0.95 to 1.84). In stratified analyses in BioVU, higher FGF23 was associated with overall heart failure (odds ratio, 3.09; 95% confidence interval, 1.38 to 6.91) among individuals with low eGFR-polygenic risk score (<1 SD below the mean), but not those with high eGFR-polygenic risk score ( P interaction = 0.02). Higher FGF23 was also associated with heart failure with preserved ejection fraction among all BioVU participants (odds ratio, 1.47; 95% confidence interval, 1.01 to 2.14) and individuals with low eGFR-polygenic risk score (odds ratio, 7.20; 95% confidence interval, 2.80 to 18.49), but not those high eGFR-polygenic risk score ( P interaction = 2.25 × 10
-4 ). No significant associations were observed with heart failure with reduced and midrange ejection fraction., Conclusion: We found no association between genetically predicted FGF23 and heart failure in the Heart Failure Molecular Epidemiology for Therapeutic Targets consortium. In BioVU, genetically elevated FGF23 was associated with higher heart failure risk, specifically heart failure with preserved ejection fraction, particularly among individuals with low genetically predicted eGFR., Podcast: This article contains a podcast at https://www.asn-online.org/media/podcast/CJASN/2022_07_28_CJN00960122.mp3., (Copyright © 2022 by the American Society of Nephrology.)- Published
- 2022
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