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Ravindar N Girotra

Bristol-Myers Squibb

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Featured researches published by Ravindar N Girotra.

Journal of Medicinal Chemistry | 2008

Discovery of Dapagliflozin: A Potent, Selective Renal Sodium-Dependent Glucose Cotransporter 2 (SGLT2) Inhibitor for the Treatment of Type 2 Diabetes

Wei Meng; Bruce A. Ellsworth; Alexandra A. Nirschl; Peggy J. McCann; Manorama Patel; Ravindar N Girotra; Gang Wu; Philip M. Sher; Eamonn P. Morrison; Scott A. Biller; Robert Zahler; Prashant P. Deshpande; Annie Pullockaran; Deborah Hagan; Nathan Morgan; Joseph R. Taylor; Mary T. Obermeier; William G. Humphreys; Ashish Khanna; Lorell Discenza; James G. Robertson; Aiying Wang; Songping Han; John R. Wetterau; Evan B. Janovitz; Oliver P. Flint; Jean M. Whaley; William N. Washburn

The C-aryl glucoside 6 (dapagliflozin) was identified as a potent and selective hSGLT2 inhibitor which reduced blood glucose levels in a dose-dependent manner by as much as 55% in hyperglycemic streptozotocin (STZ) rats. These findings, combined with a favorable ADME profile, have prompted clinical evaluation of dapagliflozin for the treatment of type 2 diabetes.

Bioorganic & Medicinal Chemistry Letters | 1994

MERCAPTOACYL DIPEPTIDES AS DUAL INHIBITORS OF ANGIOTENSIN-CONVERTING ENZYME AND NEUTRAL ENDOPEPTIDASE PRELIMINARY STRUCTURE-ACTIVITY STUDIES

Norma G. Delaney; Joel C. Barrish; Richard Neubeck; Sesha Natarajan; Marcia Cohen; George C. Rovnyak; George Huber; Natesan Murugesan; Ravindar N Girotra; Ellen Sieber-McMaster; Jeffrey A. Robl; Magdi M. Asaad; Hong Son Cheung; J.Eileen Bird; Thomas L. Waldron; Edward W. Petrillo

Abstract Mercaptoacyl dipeptides were prepared as dual-acting ACE/NEP inhibitors. Inhibition of each enzyme may be explained by different binding models. Structure-activity studies determined that, in this series of compounds, the mercaptopropanoyl dipeptide framework leads to increased affinity for NEP but diminished ACE activity in vivo .

Bioorganic & Medicinal Chemistry Letters | 2001

Beta 3 agonists. Part 1: evolution from inception to BMS-194449.

William N. Washburn; Philip M. Sher; K.M. Poss; Ravindar N Girotra; P.J. McCann; Ashvinikumar V. Gavai; Amarendra B. Mikkilineni; Arvind Mathur; Peter T. W. Cheng; Tamara Dejneka; Chongqing Sun; Tammy C. Wang; Timothy W. Harper; Anita D. Russell; Dorothy Slusarchyk; S. Skwish; G.T. Allen; D.E. Hillyer; B.H. Frohlich; B.E. Abboa-Offei; Michael Cap; Thomas L. Waldron; R.J. George; B. Tesfamariam; Carl P. Ciosek; Denis E. Ryono; D.A. Young; Kenneth E.J. Dickinson; A.A. Seymour; C.M. Arbeeny

Screening of the BMS collection identified 4-hydroxy-3-methylsulfonanilidoethanolamines as full beta 3 agonists. Substitution of the ethanolamine nitrogen with a benzyl group bearing a para hydrogen bond acceptor promoted beta(3) selectivity. SAR elucidation established that highly selective beta(3) agonists were generated upon substitution of C(alpha) with either benzyl to form (R)-1,2-diarylethylamines or with aryl to generate 1,1-diarylmethylamines. This latter subset yielded a clinical candidate, BMS-194449 (35).(1)

Bioorganic & Medicinal Chemistry Letters | 2001

BMS-196085: A potent and selective full agonist of the human β3 adrenergic receptor

Ashvinikumar V. Gavai; Philip M. Sher; Amarendra B. Mikkilineni; K.M. Poss; P.J. McCann; Ravindar N Girotra; Liesl G. Fisher; Ginger Wu; Mark S. Bednarz; Arvind Mathur; Tammy C. Wang; Chongqing Sun; Dorothy Slusarchyk; S. Skwish; G.T. Allen; D.E. Hillyer; B.H. Frohlich; B.E. Abboa-Offei; Michael Cap; Thomas L. Waldron; R.J. George; B. Tesfamariam; Timothy W. Harper; Carl P. Ciosek; D.A. Young; Kenneth E.J. Dickinson; A.A. Seymour; C.M. Arbeeny; William N. Washburn

A series of 4-hydroxy-3-methylsulfonanilido-1,2-diarylethylamines were prepared and evaluated for their human beta(3) adrenergic receptor agonist activity. SAR studies led to the identification of BMS-196085 (25), a potent beta(3) full agonist (K(i)=21 nM, 95% activation) with partial agonist (45%) activity at the beta(1) receptor. Based on its desirable in vitro and in vivo properties, BMS-196085 was chosen for clinical evaluation.

Bioorganic & Medicinal Chemistry Letters | 2008

Aglycone exploration of C-arylglucoside inhibitors of renal sodium-dependent glucose transporter SGLT2.

Bruce A. Ellsworth; Wei Meng; Manorama Patel; Ravindar N Girotra; Gang Wu; Philip M. Sher; Deborah Hagan; Mary T. Obermeier; William G. Humphreys; James G. Robertson; Aiying Wang; Songping Han; Thomas L. Waldron; Nathan Morgan; Jean M. Whaley; William N. Washburn

Bioorganic & Medicinal Chemistry Letters | 2004

BMS-201620: a selective beta 3 agonist

William N. Washburn; Chongqing Sun; Gregory S. Bisacchi; Ginger Wu; Peter T. W. Cheng; Philip M. Sher; Denis E. Ryono; Ashvinikumar V. Gavai; K.M. Poss; Ravindar N Girotra; P.J. McCann; Amarendra B. Mikkilineni; Tamara Dejneka; Tammy C. Wang; Z. Merchant; M. Morella; C.M. Arbeeny; Timothy W. Harper; Dorothy Slusarchyk; S. Skwish; Anita D. Russell; G.T. Allen; B. Tesfamariam; B.H. Frohlich; B.E. Abboa-Offei; Michael Cap; Thomas L. Waldron; R.J. George; D.A. Young; Kenneth E.J. Dickinson

Bioorganic & Medicinal Chemistry Letters | 2007

Arylpropanolamines: Selective β3 agonists arising from strategies to mitigate phase I metabolic transformations

William N. Washburn; Timothy W. Harper; Ginger Wu; J.D. Godfrey; P.J. McCann; Ravindar N Girotra; C. Shao; Hongjian Zhang; Ashvinikumar V. Gavai; Amarendra B. Mikkilineni; Tamara Dejneka; Syed Z. Ahmed; Yolanda Caringal; Jon J. Hangeland; Mingzhu Zhang; Peter T. W. Cheng; Anita D. Russell; S. Skwish; Dorothy Slusarchyk; G.T. Allen; B.H. Frohlich; B.E. Abboa-Offei; Michael Cap; Thomas L. Waldron; R.J. George; B. Tesfamariam; Kenneth E.J. Dickinson; A.A. Seymour; Philip M. Sher

Archive | 1997

1-[(3-ARYL)ALKYLSULPHONYLAMINOPHENYL]-2-(N-PHENYLALKYLAMINO) ETHANOL DERIVATIVES INTERMEDIATES AND PHARMACEUTICAL COMPOSITIONS

Washburn William N; Ravindar N Girotra; Sher Philip M; Mikkilineni Amarendra B; Poss Kathleen M; Arvind Mathur; Ashvinikumar V. Gavai; Bisacchi Gregory S

Archive | 1994

Catecholaminersatz-Verbindungen, nützlich als beta 3 Agonisten

William N. Washburn; Ravindar N Girotra; Philip M. Sher; Amarendra B. Mikkilineni; Kathleen M. Poss; Arvind Mathur; Ashvinikumar V. Gavai; Gregory S. Bisacchi

Archive | 1994

Subrogantes de catecolamina utiles como agonistas de beta 3.

William N. Washburn; Ravindar N Girotra; Philip M. Sher; Amarendra B. Mikkilineni; Kathleen M. Poss; Arvind Mathur

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Philip M. Sher

Bristol-Myers Squibb

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William N. Washburn

Columbia University

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Amarendra B. Mikkilineni

Bristol-Myers Squibb

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Ashvinikumar V. Gavai

Bristol-Myers Squibb

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Arvind Mathur

Bristol-Myers Squibb

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Thomas L. Waldron

Bristol-Myers Squibb

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B. Tesfamariam

Bristol-Myers Squibb

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B.E. Abboa-Offei

Bristol-Myers Squibb

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B.H. Frohlich

Bristol-Myers Squibb

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Dorothy Slusarchyk

Bristol-Myers Squibb

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