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51. Prolonged and tunable residence time using reversible covalent kinase inhibitors

Author

Bradshaw, J Michael, McFarland, Jesse M, Paavilainen, Ville O, Bisconte, Angelina, Tam, Danny, Phan, Vernon T, Romanov, Sergei, Finkle, David, Shu, Jin, Patel, Vaishali, Ton, Tony, Li, Xiaoyan, Loughhead, David G, Nunn, Philip A, Karr, Dane E, Gerritsen, Mary E, Funk, Jens Oliver, Owens, Timothy D, Verner, Erik, Brameld, Ken A, Hill, Ronald J, Goldstein, David M, and Taunton, Jack

Subjects
Acrylamides, Agammaglobulinaemia Tyrosine Kinase, Animals, B-Lymphocytes, Cell Line, Tumor, Crystallography, X-Ray, Cyanoacrylates, Dasatinib, Female, Gene Expression, Humans, Ligands, Molecular Docking Simulation, Protein Kinase Inhibitors, Protein Structure, Tertiary, Protein-Tyrosine Kinases, Pyrimidines, Rats, Rats, Sprague-Dawley, Recombinant Proteins, Sf9 Cells, Spodoptera, Structure-Activity Relationship, Substrate Specificity, Thiazoles, Time Factors, Medicinal and Biomolecular Chemistry, Biochemistry and Cell Biology, Biochemistry & Molecular Biology
Abstract

Drugs with prolonged on-target residence times often show superior efficacy, yet general strategies for optimizing drug-target residence time are lacking. Here we made progress toward this elusive goal by targeting a noncatalytic cysteine in Bruton's tyrosine kinase (BTK) with reversible covalent inhibitors. Using an inverted orientation of the cysteine-reactive cyanoacrylamide electrophile, we identified potent and selective BTK inhibitors that demonstrated biochemical residence times spanning from minutes to 7 d. An inverted cyanoacrylamide with prolonged residence time in vivo remained bound to BTK for more than 18 h after clearance from the circulation. The inverted cyanoacrylamide strategy was further used to discover fibroblast growth factor receptor (FGFR) kinase inhibitors with residence times of several days, demonstrating the generalizability of the approach. Targeting of noncatalytic cysteines with inverted cyanoacrylamides may serve as a broadly applicable platform that facilitates 'residence time by design', the ability to modulate and improve the duration of target engagement in vivo.

Published
2015

52. Submandibular Parasympathetic Gangliogenesis Requires Sprouty-Dependent Wnt Signals from Epithelial Progenitors

Author

Knosp, Wendy M, Knox, Sarah M, Lombaert, Isabelle MA, Haddox, Candace L, Patel, Vaishali N, and Hoffman, Matthew P

Subjects
Biochemistry and Cell Biology, Biological Sciences, Neurosciences, Stem Cell Research, Digestive Diseases, Stem Cell Research - Nonembryonic - Non-Human, Regenerative Medicine, Adaptor Proteins, Signal Transducing, Animals, Cell Differentiation, Cell Proliferation, Fibroblast Growth Factors, Ganglia, Parasympathetic, Gene Dosage, Intracellular Signaling Peptides and Proteins, Keratin-15, Membrane Proteins, Mice, Mice, Inbred ICR, Mice, Knockout, Neuregulins, Neurons, Organ Culture Techniques, Organogenesis, Pancreas, Phosphatidylinositol 3-Kinases, Phosphoproteins, Protein Serine-Threonine Kinases, Schwann Cells, Stem Cells, Submandibular Gland, Wnt Proteins, Wnt Signaling Pathway, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology
Abstract

Parasympathetic innervation is critical for submandibular gland (SMG) development and regeneration. Parasympathetic ganglia (PSG) are derived from Schwann cell precursors that migrate along nerves, differentiate into neurons, and coalesce within their target tissue to form ganglia. However, signals that initiate gangliogenesis after the precursors differentiate into neurons are unknown. We found that deleting negative regulators of FGF signaling, Sprouty1 and Sprouty2 (Spry1/2DKO), resulted in a striking loss of gangliogenesis, innervation, and keratin 5-positive (K5+) epithelial progenitors in the SMG. Here we identify Wnts produced by K5+ progenitors in the SMG as key mediators of gangliogenesis. Wnt signaling increases survival and proliferation of PSG neurons, and inhibiting Wnt signaling disrupts gangliogenesis and organ innervation. Activating Wnt signaling and reducing FGF gene dosage rescues gangliogenesis and innervation in both the Spry1/2DKO SMG and pancreas. Thus, K5+ progenitors produce Wnt signals to establish the PSG-epithelial communication required for organ innervation and progenitor cell maintenance.

Published
2015

60. Physicians in ACOs Report Greater Documentation Burden.

Author

Apathy, Nate C., Patel, Vaishali, Rolle, Tricia Lee, and Holmgren, A. Jay

Subjects
*DOCUMENTATION, *CROSS-sectional method, *SELF-evaluation, *RESEARCH funding, *INDUSTRIAL psychology, *VALUE-based healthcare, *ACCOUNTABLE care organizations, *RETROSPECTIVE studies, *DESCRIPTIVE statistics, *PHYSICIANS' attitudes, *SURVEYS, *ELECTRONIC health records, *RESEARCH methodology, *PHYSICIANS, *DATA analysis software, *LABOR incentives, *REGRESSION analysis, *PAY for performance
Abstract

OBJECTIVES: First, to analyze the relationship between value-based payment (VBP) program participation and documentation burden among office-based physicians. Second, to analyze the relationship between specific VBP programs (eg, accountable care organizations [ACOs]) and documentation burden. STUDY DESIGN: Retrospective analyses of US office-based physicians in 2019 and 2021. METHODS: We used cross-sectional data from the National Electronic Health Records Survey to measure VBP program participation and our outcomes of reported electronic health record (EHR) documentation burden. We used ordinary least squares regression models adjusting for physician and practice characteristics to estimate the relationship between participation in any VBP program and EHR burden outcomes. We also estimated the relationship between participation in 6 distinct VBP programs and our outcomes to decompose the aggregate relationship into program-specific estimates. RESULTS: In adjusted analyses, participation in any VBP program was associated with 10.5% greater probability of reporting more than 1 hour per day of after-hours documentation time (P = .01), which corresponded to an estimated additional 11 minutes per day (P = .03). Program-specific estimates illustrated that ACO participation drove the aggregate relationship, with ACO participants reporting greater after-hours documentation time (18 additional minutes per day; P < .001), more difficulty documenting (30.6% more likely; P < .001), and more inappropriateness of time spent documenting (21.7% more likely; P < .001). CONCLUSIONS: Office-based physicians participating in ACOs report greater documentation burden across several measures; the same is not true for other VBP programs. Although many ACOs relax documentation requirements for reimbursement, documentation for quality reporting and risk adjustment may lead to a net increase in burden, especially for physicians exposed to numerous programs and payers. [ABSTRACT FROM AUTHOR]

Published
2024
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62. S133 Long-Term Outcomes of ERCP in the Management of Chronic Pancreatitis Over a 10-year Period at a Tertiary Care Center

Author

Emelogu, Ikenna K., primary, Brooks, Carolyn G., additional, Deliwala, Smit, additional, Calderon, Lucie F., additional, Abraham, Fiyinfoluwa O., additional, Kumar, Vishnu Ravi, additional, Willingham, Field, additional, Keilin, Steven, additional, Patel, Vaishali, additional, Orr, Jordan, additional, Park, Walter, additional, and Chawla, Saurabh, additional

Published
2023
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66. S1819 Predictors of Recurrent AVM-Related Bleeding in Patients With Advanced CKD Receiving Balloon Enteroscopy

Author

Do, Kevin O., primary, Issac, Aaron, additional, Tran, Cynthia N., additional, Biermann, Maya, additional, Youngblood, Alix, additional, Spandorfer, Adam, additional, Desai, Nikita, additional, Abdalla, Abubaker, additional, Khare, Anshika P., additional, Vachaparambil, Cicily, additional, Willingham, Field, additional, Keilin, Steven, additional, Patel, Vaishali, additional, and Chawla, Saurabh, additional

Published
2023
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75. Interplay Between Dyslipidemia, Atherogenic Lipoproteins, and Residual Atherogenic Risk in Liver Transplant Recipients

Author

Tseng, Michael, primary, Connelly, Margery A., additional, Vanier, Dylan, additional, Arshad, Tamoore, additional, Kirkman, Danielle, additional, Siddiqui, Mohammad Shadab, additional, Flynn, Sean, additional, Syed, Taseen, additional, Hassouneh, Ramzi, additional, Patel, Vaishali, additional, Asgharpour, Amon, additional, and Muthiah, Mark, additional

Published
2023
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76. Increased 3- O -sulfated heparan sulfate in Alzheimer’s disease brain is associated with genetic risk gene HS3ST1

Author

Wang, Zhangjie, primary, Patel, Vaishali N., additional, Song, Xuehong, additional, Xu, Yongmei, additional, Kaminski, Andrea M., additional, Doan, Vivien Uyen, additional, Su, Guowei, additional, Liao, Yien, additional, Mah, Dylan, additional, Zhang, Fuming, additional, Pagadala, Vijayakanth, additional, Wang, Chunyu, additional, Pedersen, Lars C., additional, Wang, Lianchun, additional, Hoffman, Matthew P., additional, Gearing, Marla, additional, and Liu, Jian, additional

Published
2023
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77. Reduced metabolic flexibility is a predictor of weight gain among liver transplant recipients

Author

Bui, Anh T., primary, Chaudhari, Rahul, additional, Bhati, Chandra, additional, Wolver, Susan, additional, Patel, Samarth, additional, Boyett, Sherry, additional, Evans, Marie Claire, additional, Kamal, Hiba, additional, Patel, Vaishali, additional, Forsgren, Mikael, additional, Sanyal, Arun J., additional, Kirkman, Danielle, additional, and Siddiqui, Mohammad Shadab, additional

Published
2023
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79. Reduced metabolic flexibility is a predictor of weight gain among liver transplant recipients

Author

Bui, Anh T., Chaudhari, Rahul, Bhati, Chandra, Wolver, Susan, Patel, Samarth, Boyett, Sherry, Evans, Marie Claire, Kamal, Hiba, Patel, Vaishali, Forsgren, Mikael, Sanyal, Arun J., Kirkman, Danielle, Siddiqui, Mohammad Shadab, Bui, Anh T., Chaudhari, Rahul, Bhati, Chandra, Wolver, Susan, Patel, Samarth, Boyett, Sherry, Evans, Marie Claire, Kamal, Hiba, Patel, Vaishali, Forsgren, Mikael, Sanyal, Arun J., Kirkman, Danielle, and Siddiqui, Mohammad Shadab

Abstract

Metabolic flexibility is the ability to match biofuel availability to utilization and is inversely associated with increased metabolic burden among liver transplant (LT) recipients. The present study evaluated the impact of metabolic flexibility on weight gain following LT. LT recipients were enrolled prospectively (n = 47) and followed for 6 months. Metabolic flexibility was measured using whole-room calorimetry and is expressed as a respiratory quotient (RQ). Peak RQ represents maximal carbohydrate metabolism and occurs in the post-prandial state, while trough RQ represents maximal fatty acid metabolism occurring in the fasted state. The clinical, metabolic, and laboratory characteristics of the study cohort of lost weight (n = 14) and gained weight (n = 33) were similar at baseline. Patients who lost weight were more likely to reach maximal RQ (maximal carbohydrate oxidation) early and rapidly transitioned to trough RQ (maximal fatty acid oxidation). In contrast, patients who gained weight had delayed time to peak RQ and trough RQ. In multivariate modeling, time to peak RQ (& beta;-coefficient 0.509, p = 0.01), time from peak RQ to trough RQ (& beta;-coefficient 0.634, p = 0.006), and interaction between time to peak RQ to trough RQ and fasting RQ (& beta;-coefficient 0.447, p = 0.02) directly correlated with the severity of weight gain. No statistically significant relationship between peak RQ, trough RQ, and weight change was demonstrated. Inefficient transition between biofuels (carbohydrates and fatty acids) is associated with weight gain in LT recipients that is independent of clinical metabolic risk. These data offer novel insight into the physiology of obesity after LT with the potential to develop new diagnostics and therapeutics., Funding Agencies|Mohammad Shadab Siddiqui, Chandra Bhati, Danielle Kirkman, and Susan Wolver: Study design. Mohammad Shadab Siddiqui, Sherry Boyett, and Marie Claire Evans: Whole-room calorimetry. Mikael Forsgren: Radiology. Mohammad Shadab Siddiqui, Samarth Patel, and Vai

Published
2023
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80. Saroglitazar improves nonalcoholic fatty liver disease and metabolic health in liver transplant recipients

Author

Siddiqui, Mohammad Shadab, Parmar, Deven, Shaikh, Farheen, Forsgren, Mikael, Patel, Samarth, Bui, Anh Tuan, Boyett, Sherry, Patel, Vaishali, Sanyal, Arun J., Siddiqui, Mohammad Shadab, Parmar, Deven, Shaikh, Farheen, Forsgren, Mikael, Patel, Samarth, Bui, Anh Tuan, Boyett, Sherry, Patel, Vaishali, and Sanyal, Arun J.

Abstract

NAFLD is common after liver transplantation (LT) and is associated with an increased metabolic burden. Currently, there is a paucity of investigations into the treatment of post-LT NAFLD. In the present study, we evaluated the safety and efficacy of saroglitazar, a novel dual peroxisome proliferator-associated receptor & alpha;/& gamma; agonist, on the treatment of post-LT NAFLD and metabolic burden. This is a phase 2A, single-center, open-label, single-arm study in which patients with post-LT NAFLD received saroglitazar magnesium 4 mg daily for 24 weeks. NAFLD was defined by a controlled attenuation parameter & GE;264 dB/m. The primary endpoint was the reduction in liver fat as measured by MRI proton density fat fraction (MRI-PDFF). Secondary MRI-based metabolic endpoints included visceral adipose tissue, abdominal subcutaneous adipose tissue volumes, muscle fat infiltration, and fat-free muscle volume. Saroglitazar treatment led to a reduction in MRI-PDFF from 10.3 & PLUSMN;10.5% at baseline to 8.1 & PLUSMN;7.6%. A relative 30% reduction from baseline MRI-PDFF value was noted in 47% of all patients and 63% of patients with baseline MRI-PDFF >5%. Reduction in serum alkaline phosphatase was an independent predictor of MRI-PDFF response. Saroglitazar did not decrease fat-free muscle volume nor increase muscle fat infiltration, but did lead to a mild increase in visceral adipose tissue and abdominal subcutaneous adipose tissue. The study drug was well tolerated and a mild nonsignificant increase in serum creatinine was noted. Saroglitazar did not affect the weight. The study provides preliminary data demonstrating the safety and metabolic benefits of saroglitazar in LT recipients and underscores the importance of future studies to establish its efficacy after LT., Funding Agencies|Zydus Therapeutics Inc.

Published
2023
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85. Analysis of photosystem I mutants in Chlamydomonas reinhardtii

Author

Patel, Vaishali

Subjects
572, Biochemistry
Abstract

FX is a [4Fe-4S] iron-sulphur centre that is believed to be bound by both PsaA and PsaB. This is a rather unusual arrangement, as [4Fe-4S] iron-sulphur centres are usually bound by one protein, rather than two. This may impose constraints on the interactions of the other subunits of PSI. The region believed to be involved in binding FX is highly conserved, and a possible role has not yet been identified for most of the amino acids within this region. In this study, the function of several amino acids of this region has been examined, by creating amino acid substitutions, and then examining the effect on PSI assembly, and electron transport. Mutant D576L is a nonphotosynthetic mutant of C. reinhardtii. D576 is an amino acid present within the FX binding region, and is believed to be important in the coordination of PsaC, which in turn coordinates the terminal electron acceptors of PSI. The role of this conserved amino acid residue was examined by substituting it with a leucine residue. This substitution caused the PSI complex to be disrupted, and also altered electron transport to FA/FB. Second site suppressor mutants of the D576L mutation were also isolated. These suppressor mutants were effected in the same way as the original D576L mutants, in terms of electron transport to FA/FB, but were able to grow photoautotrophically. This unknown spontaneous mutation is identified as a nuclear mutation. The results show that D576 is important for the binding of PsaC, and that in the suppressor mutants electron transfer rates from A1 to FX are altered, but restored to wild type values in the suppressor mutants. A library of mutations was created by randomly mutating three amino acids, Arg572, Phe573 and Pro574, of the FX binding motif in PsaA. Three mutants of C. reinhardtii were produced. These mutants were selected for their ability to grow photoautotrophically, as the aim was to create minor disruptions in the photosystem, which would still allow PSI to assemble and function. It was hoped that this would provide information on the possible functions of these amino acids. However, all three mutants appear to assemble as much PSI as wild type C. reinhardtii, and the electron transport properties were also similar. Rates of electron transport to FA/FB were not altered, compared to wild type C. reinhardtii. The role of a small chloroplast encoded subunit, PsaJ, of PSI was also examined. The function of PsaJ, which is a membrane protein, is unknown, although it has been suggested that it may coordinate PsaF. The amino acid structure of PsaJ was examined, and revealed regions of hydrophobicity, which are consistent with a membrane protein. However, unlike most membrane proteins which are composed of α-helices, the secondary structure of PsaJ is predicted to be composed of β-sheets. This may prove to have some bearing on its function. The psaJ gene was deleted, and aadA was inserted in its place. This construct was used to transform C. reinhardtii, but transformants failed to emerge.

Published
1997

92. Clinical and Healthcare Resource Use Outcomes between Dual-plane and Prepectoral Techniques in Implant-based Breast Reconstruction: A Multicenter Retrospective Study

Author

Bruno, James R., primary, Brown, C. Coleman, additional, Gabriel, Allen, additional, Parikh, Mousam, additional, Anastassopoulos, Kathryn P., additional, Lee, Kenneth R., additional, Daniel, Shoshana, additional, Naik, Rupali, additional, Patel, Reema, additional, and Patel, Vaishali D., additional

Published
2023
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95. Evaluation of liver stiffness measurement–based scores in liver transplantation recipients

Author

Arshad, Tamoore, primary, Bhati, Chandra S., additional, Bui, Anh T., additional, Tseng, Michael, additional, Vainer, Dylan, additional, Miller, Austin, additional, Evans, Marie‐Claire, additional, Syed, Taseen, additional, Patel, Vaishali, additional, Idowu, Michael O., additional, Muthiah, Mark, additional, and Siddiqui, Mohammad Shadab, additional

Published
2023
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