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151. In-depth phenotyping for clinical stratification of Gaucher disease

Author

D’Amore, Simona, Page, Kathleen, Donald, Aimée, Taiyari, Khadijeh, Tom, Brian, Deegan, Patrick, Tan, Chong Y., Poole, Kenneth, Jones, Simon A., Mehta, Atul, Hughes, Derralynn, Sharma, Reena, Lachmann, Robin H., Chakrapani, Anupam, Geberhiwot, Tarekegn, Santra, Saikat, Banka, Siddarth, Cox, Timothy M., Cox, T. M., Platt, F. M., Banka, S., Chakrapani, A., Deegan, P. B., Geberhiwot, T., Hughes, D. A., Jones, S., Lachmann, R. H., Santra, S., Sharma, R., Vellodi, A., Cox, Timothy M [0000-0002-4951-9941], Apollo - University of Cambridge Repository, and Cox, Timothy M. [0000-0002-4951-9941]

Subjects
Pediatrics, medicine.medical_specialty, medicine.medical_treatment, Splenectomy, Disease, Cohort Studies, Lysosomal storage diseases, medicine, Humans, Disease-modifying therapies, GAUCHERITE, Pharmacology (medical), Substrate reduction therapy, Prospective Studies, Bone pain, Genetics (clinical), Retrospective Studies, Gaucher Disease, business.industry, Research, Cohort, Genetic disorder, General Medicine, Enzyme replacement therapy, medicine.disease, Orthopedic surgery, Medicine, Glucosylceramidase, Nervous System Diseases, medicine.symptom, business
Abstract

Background The Gaucher Investigative Therapy Evaluation is a national clinical cohort of 250 patients aged 5–87 years with Gaucher disease in the United Kingdom—an ultra-rare genetic disorder. To inform clinical decision-making and improve pathophysiological understanding, we characterized the course of Gaucher disease and explored the influence of costly innovative medication and other interventions. Retrospective and prospective clinical, laboratory and radiological information including molecular analysis of the GBA1 gene and comprising > 2500 variables were collected systematically into a relational database with banking of collated biological samples in a central bioresource. Data for deep phenotyping and life-quality evaluation, including skeletal, visceral, haematological and neurological manifestations were recorded for a median of 17.3 years; the skeletal and neurological manifestations are the main focus of this study. Results At baseline, 223 of the 250 patients were classified as type 1 Gaucher disease. Skeletal manifestations occurred in most patients in the cohort (131 of 201 specifically reported bone pain). Symptomatic osteonecrosis and fragility fractures occurred respectively in 76 and 37 of all 250 patients and the first osseous events occurred significantly earlier in those with neuronopathic disease. Intensive phenotyping in a subgroup of 40 patients originally considered to have only systemic features, revealed neurological involvement in 18: two had Parkinson disease and 16 had clinical signs compatible with neuronopathic Gaucher disease—indicating a greater than expected prevalence of neurological features. Analysis of longitudinal real-world data enabled Gaucher disease to be stratified with respect to advanced therapies and splenectomy. Splenectomy was associated with an increased hazard of fragility fractures, in addition to osteonecrosis and orthopaedic surgery; there were marked gender differences in fracture risk over time since splenectomy. Skeletal disease was a heavy burden of illness, especially where access to specific therapy was delayed and in patients requiring orthopaedic surgery. Conclusion Gaucher disease has been explored using real-world data obtained in an era of therapeutic transformation. Introduction of advanced therapies and repeated longitudinal measures enabled this heterogeneous condition to be stratified into obvious clinical endotypes. The study reveals diverse and changing phenotypic manifestations with systemic, skeletal and neurological disease as inter-related sources of disability.

Published
2021
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155. Effect of Endobronchial Coils vs Usual Care on Exercise Tolerance in Patients With Severe Emphysema: The RENEW Randomized Clinical Trial

Author

Sciurba, Frank C., Criner, Gerard J., Strange, Charlie, Shah, Pallav L., Michaud, Gaetane, Connolly, Timothy A., Deslée, Gaëtan, Tillis, William P., Delage, Antoine, Marquette, Charles-Hugo, Krishna, Ganesh, Kalhan, Ravi, Ferguson, J. Scott, Jantz, Michael, Maldonado, Fabien, McKenna, Robert, Majid, Adnan, Rai, Navdeep, Gay, Steven, Dransfield, Mark T., Angel, Luis, Maxfield, Roger, Herth, Felix J. F., Wahidi, Momen M., Mehta, Atul, and Slebos, Dirk-Jan

Published
2016
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161. Lung Ultrasonographic Signs in Pulmonary Disease – A Video Review.

Author

Dugar, Siddharth, Fox, Steven, Koratala, Abhilash, Moghekar, Ajit, and Mehta, Atul C.

Subjects
LUNG diseases, PLEURAL effusions, ULTRASONIC imaging, LEARNING ability, CLINICAL trials
Abstract

Lung ultrasound (US) is a well-established imaging tool in the inpatient and critical care setting. It has proven its worth in the rapid bedside diagnosis of a variety of conditions pertaining to the lungs and the thorax. Lung US was initially introduced as a bedside imaging tool to evaluate the size and characteristics of pleural effusion. Over the years, the field of lung ultrasonography has rapidly expanded introducing nuances in image interpretation. Numerous primary and secondary signs have been described in the literature to identify both normal and abnormal findings. The primary signs can help narrow the list of differential diagnoses, whereas the addition of secondary signs help create an imaging pattern facilitating the confirmation of diagnosis or recognition of the underlying disease process. These wide variety of signs and patterns can present a challenge to the learning of lung ultrasonography, particularly to a novice user. We sought to compile a comprehensive list of these findings to serve as a useful resource to aid effortless adoption of lung ultrasonography in clinical practice. In this review, we narrate the evolution of lung US, describe common protocols applied in performance of the lung US, and illustrate a comprehensive list of common lung US signs and patterns along with their differential diagnosis and clinical utility. [ABSTRACT FROM AUTHOR]

Published
2023
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189. Predicting Lymph Node Metastasis in Non-small Cell Lung Cancer: Prospective External and Temporal Validation of the HAL and HOMER Models

Author

Martinez-Zayas, Gabriela, Almeida, Francisco A., Yarmus, Lonny, Steinfort, Daniel, Lazarus, Donald R., Simoff, Michael J., Saettele, Timothy, Murgu, Septimiu, Dammad, Tarek, Duong, D. Kevin, Mudambi, Lakshmi, Filner, Joshua J., Molina, Sofia, Aravena, Carlos, Thiboutot, Jeffrey, Bonney, Asha, Rueda, Adriana M., Debiane, Labib G., Hogarth, D. Kyle, Bedi, Harmeet, Deffebach, Mark, Sagar, Ala-Eddin S., Cicenia, Joseph, Yu, Diana H., Cohen, Avi, Frye, Laura, Grosu, Horiana B., Gildea, Thomas, Feller-Kopman, David, Casal, Roberto F., Machuzak, Michael, Arain, Muhammad H., Sethi, Sonali, Eapen, George A., Lam, Louis, Jimenez, Carlos A., Ribeiro, Manuel, Noor, Laila Z., Mehta, Atul, Song, Juhee, Choi, Humberto, Ma, Junsheng, Li, Liang, and Ost, David E.

Subjects
Image-Guided Biopsy, Male, Lung Neoplasms, Patient Selection, Biopsy, Fine-Needle, Mediastinum, Middle Aged, Thoracic Oncology: Original Research, Prognosis, United States, Endosonography, Predictive Value of Tests, Carcinoma, Non-Small-Cell Lung, Lymphatic Metastasis, Bronchoscopy, Calibration, Humans, Female, Neoplasm Staging
Abstract

BACKGROUND: Two models, the Help with the Assessment of Adenopathy in Lung cancer (HAL) and Help with Oncologic Mediastinal Evaluation for Radiation (HOMER), were recently developed to estimate the probability of nodal disease in patients with non-small cell lung cancer (NSCLC) as determined by endobronchial ultrasound-transbronchial needle aspiration (EBUS-TBNA). The objective of this study was to prospectively externally validate both models at multiple centers. RESEARCH QUESTION: Are the HAL and HOMER models valid across multiple centers? STUDY DESIGN AND METHODS: This multicenter prospective observational cohort study enrolled consecutive patients with PET-CT clinical-radiographic stages T1-3, N0-3, M0 NSCLC undergoing EBUS-TBNA staging. HOMER was used to predict the probability of N0 vs N1 vs N2 or N3 (N2|3) disease, and HAL was used to predict the probability of N2|3 (vs N0 or N1) disease. Model discrimination was assessed using the area under the receiver operating characteristics curve (ROC-AUC), and calibration was assessed using the Brier score, calibration plots, and the Hosmer-Lemeshow test. RESULTS: Thirteen centers enrolled 1,799 patients. HAL and HOMER demonstrated good discrimination: HAL ROC-AUC = 0.873 (95%CI, 0.856-0.891) and HOMER ROC-AUC = 0.837 (95%CI, 0.814-0.859) for predicting N1 disease or higher (N1|2|3) and 0.876 (95%CI, 0.855-0.897) for predicting N2|3 disease. Brier scores were 0.117 and 0.349, respectively. Calibration plots demonstrated good calibration for both models. For HAL, the difference between forecast and observed probability of N2|3 disease was +0.012; for HOMER, the difference for N1|2|3 was −0.018 and for N2|3 was +0.002. The Hosmer-Lemeshow test was significant for both models (P = .034 and .002), indicating a small but statistically significant calibration error. INTERPRETATION: HAL and HOMER demonstrated good discrimination and calibration in multiple centers. Although calibration error was present, the magnitude of the error is small, such that the models are informative.

Published
2021

192. Predicting Lymph Node Metastasis in Non-small Cell Lung Cancer

Author

Martinez-Zayas, Gabriela, primary, Almeida, Francisco A., additional, Yarmus, Lonny, additional, Steinfort, Daniel, additional, Lazarus, Donald R., additional, Simoff, Michael J., additional, Saettele, Timothy, additional, Murgu, Septimiu, additional, Dammad, Tarek, additional, Duong, D. Kevin, additional, Mudambi, Lakshmi, additional, Filner, Joshua J., additional, Molina, Sofia, additional, Aravena, Carlos, additional, Thiboutot, Jeffrey, additional, Bonney, Asha, additional, Rueda, Adriana M., additional, Debiane, Labib G., additional, Hogarth, D. Kyle, additional, Bedi, Harmeet, additional, Deffebach, Mark, additional, Sagar, Ala-Eddin S., additional, Cicenia, Joseph, additional, Yu, Diana H., additional, Cohen, Avi, additional, Frye, Laura, additional, Grosu, Horiana B., additional, Gildea, Thomas, additional, Feller-Kopman, David, additional, Casal, Roberto F., additional, Machuzak, Michael, additional, Arain, Muhammad H., additional, Sethi, Sonali, additional, Eapen, George A., additional, Lam, Louis, additional, Jimenez, Carlos A., additional, Ribeiro, Manuel, additional, Noor, Laila Z., additional, Mehta, Atul, additional, Song, Juhee, additional, Choi, Humberto, additional, Ma, Junsheng, additional, Li, Liang, additional, and Ost, David E., additional

Published
2021
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195. Correction: Assessment of plasma lyso-Gb3 for clinical monitoring of treatment response in migalastat-treated patients with Fabry disease (Genetics in Medicine, (2021), 23, 1, (192-201), 10.1038/s41436-020-00968-z)

Author

Bichet, Daniel G., Aerts, Johannes M., Auray-Blais, Christiane, Maruyama, Hiroki, Mehta, Atul B., Skuban, Nina, Krusinska, Eva, Schiffmann, Raphael, Amsterdam Gastroenterology Endocrinology Metabolism, and Amsterdam Cardiovascular Sciences

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published
2021

196. Additional file 1 of In-depth phenotyping for clinical stratification of Gaucher disease

Author

D’Amore, Simona, Page, Kathleen, Donald, Aimée, Taiyari, Khadijeh, Tom, Brian, Deegan, Patrick, Tan, Chong Y., Poole, Kenneth, Jones, Simon A., Mehta, Atul, Hughes, Derralynn, Sharma, Reena, Lachmann, Robin H., Chakrapani, Anupam, Geberhiwot, Tarekegn, Santra, Saikat, Banka, Siddarth, and Cox, Timothy M.

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, nutritional and metabolic diseases, nervous system diseases
Abstract

Additional file 1. Deep Phenotyping of Gaucher disease with supplementary materials, methods, results and references.

Published
2021
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