Your search keyword '"Demicco M"' showing total 8 results

1. A randomized, placebo-controlled study of the NS5B inhibitor beclabuvir with peginterferon/ribavirin for HCV genotype 1.

Author

Tatum, H., Thuluvath, P. J., Lawitz, E., Martorell, C., DeMicco, M., Cohen, S., Rustgi, V., Ravendhran, N., Ghalib, R., Hanson, J., Zamparo, J., Zhao, J., Cooney, E., Treitel, M., and Hughes, E.

Subjects

*GENOTYPE-environment interaction, *ANTIMETABOLITES, *HEPATITIS C, *VIRAL hepatitis, *FLAVIVIRAL diseases, *LIVER diseases, *VIRUS diseases

Abstract

Beclabuvir is a potent, non-nucleoside inhibitor of the HCV NS5B RNA polymerase, with nanomolar activity against HCV genotypes 1, 3, 4, 5 and 6 in vitro. This study evaluated the efficacy and safety of beclabuvir, in combination with peginterferon alfa-2a (pegIFN) and ribavirin (RBV), in HCV genotype 1. In this randomized (1:1:1), double-blinded, placebo-controlled, dose-ranging phase 2a study, 39 treatment-naive patients chronically infected with HCV genotype 1 were treated for 48 weeks with beclabuvir (75 mg or 150 mg) plus pegIFN (180 lg) and RBV (1000 mg/day [<75 kg] or 1200 mg/day [≥75 kg]) vs pegIFN/RBV alone. The primary efficacy endpoint of extended rapid virologic response (undetectable HCV RNA at treatment weeks 4 and 12) was achieved by 76.9% (10/13) of patients receiving beclabuvir 75 mg and 38.5% (5/13) receiving beclabuvir 150 mg vs 0% receiving pegIFN/RBV alone. Higher response rates were observed among patients receiving beclabuvir 75 mg for all secondary efficacy endpoints, including sustained virologic response at follow-up weeks 12 or 24. Three patients experienced virologic breakthrough on treatment, all in the beclabuvir 150-mg treatment group. Beclabuvir was well tolerated at both doses, with the most commonly observed adverse events (headache, fatigue, nausea, decreased appetite, irritability, depression and insomnia) consistent with those observed with pegIFN/RBV. In conclusion, beclabuvir was both effective and well tolerated when administered in combination with pegIFN/RBV for the treatment of chronic HCV GT 1, supporting the study of beclabuvir as part of an all-oral regimen for HCV GT1. [ABSTRACT FROM AUTHOR]

Published

2015

2. 1055 ANTIVIRAL ACTIVITY OF ANA598, A POTENT NON- NUCLEOSIDE POLYMERASE INHIBITOR, IN CHRONIC HEPATITIS C PATIENTS

Author

Lawitz, E., Rodriguez-Torres, M., DeMicco, M., Nguyen, T., Godofsky, E., Appleman, J., Rahimy, M., Crowley, C., and Freddo, J.

Published

2009

3. P1–055PHARMACOKINETICS (PK) OF THE PAN-HER INHIBITOR DACOMITINIB (D) IN SUBJECTS WITH MILD OR MODERATE HEPATIC IMPAIRMENT.

Author

O'Connell, J., Plotka, A., Liang, Y., Boutros, T., Ni, G., Masters, J., DeMicco, M., Pardo, P., Bello, C., and Giri, N.

Subjects

*LIVER cancer, *PROTEIN-tyrosine kinase inhibitors, *PHARMACOKINETICS, *ELECTROCARDIOGRAPHY, *PROTEIN binding, *PERIODIC health examinations

Published

2013

4. 847 ACH-2684 DEMONSTRATES POTENT VIRAL SUPPRESSION IN GENOTYPE 1 HEPATITIS C PATIENTS WITH AND WITHOUT CIRRHOSIS: SAFETY, PHARMACOKINETIC, AND VIRAL KINETIC ANALYSIS.

Author

Lawitz, E., Hill, J., Vince, B., Murillo, A., Gruener, D., Marbury, T., Demicco, M., Agarwal, A., Robison, H., Huang, M., Robarge, L., Hui, J., Olek, E., Deshpande, M., and Kocinsky, H.

Published

2013

5. 1163 A PHASE 2A STUDY OF BMS-791325, AN NS5B POLYMERASE INHIBITOR, WITH PEGINTERFERON ALFA-2A AND RIBAVIRIN IN TREATMENT-NAIVE PATIENTS WITH GENOTYPE 1 CHRONIC HEPATITIS C INFECTION

Author

Tatum, H., Thuluvath, P., Lawitz, E., Martorell, C.T., Demicco, M., Cohen, S., Rustgi, V., Ravendhran, N., Ghalib, R., Hanson, J., Zamparo, J., Yang, R., Hughes, E., and Cooney, E.

Published

2012

6. 1120 PSI-7977 400 MG QD SAFETY AND TOLERABILITY IN THE FIRST 450 PATIENTS TREATED FOR 12 WEEKS

Author

Jacobson, I., Lawitz, E., Lalezari, J., Crespo, I., Davis, M., Hassanein, T., DeMicco, M., Arora, S., Gitlin, N., Herring, R., Nelson, D.R., Anderson, J.K., Hyland, R.H., Mader, M., Hindes, R., Albanis, E., Symonds, W.T., and Berrey, M.M.

Published

2012

7. 1 ATOMIC: 97% RVR FOR PSI-7977 + PEG/RBV × 12 WEEK REGIMEN IN HCV GT1: AN END TO RESPONSE-GUIDED THERAPY?

Author

Kowdlev, K.V., Läwitz, E., Crespo, I., Hassanein, T., Davis, M., DeMicco, M., Nelson, D.R., Bernstein, D., Afdhal, N.H., Jacobson, I., Vierling, J., Gordon, S., Anderson, J.K., Hyland, R.H., Hindes, R.G., Baker, C., Sorensen, R., Albanis, E., Symonds, W.T., and Berrey, M.M.

Published

2012

8. 1219 THREE-DAY, DOSE-RANGING STUDY OF THE HCV NS5A INHIBITOR GS-5885

Author

Lawitz, E., Gruener, D., Hill, J., Marbury, T., Komjathy, S., DeMicco, M., Murillo, A., Jenkin, F., Kim, K., Simpson, J., Aycock, M., Mathias, A., Yang, C., Dowdy, E., Liles, M., Cheng, G., Mondou, E., Link, J., Brainard, D., and McHutchison, J.

Published

2011