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1. Molecular Determinants of Human Rhinovirus Infection, Assembly, and Conformational Stability at Capsid Protein Interfaces.

2. Thermostability of the Foot-and-Mouth Disease Virus Capsid Is Modulated by Lethal and Viability-Restoring Compensatory Amino Acid Substitutions.

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3. A single amino acid substitution in the capsid of foot-and-mouth disease virus can increase acid resistance.

4. A single amino acid substitution in the capsid of foot-and-mouth disease virus can increase acid lability and confer resistance to acid-dependent uncoating inhibition.

5. Systematic study of the genetic response of a variable virus to the introduction of deleterious mutations in a functional capsid region.

6. Engineering viable foot-and-mouth disease viruses with increased thermostability as a step in the development of improved vaccines.

7. Minute virus of mice, a parvovirus, in complex with the Fab fragment of a neutralizing monoclonal antibody.

8. Deterministic, compensatory mutational events in the capsid of foot-and-mouth disease virus in response to the introduction of mutations found in viruses from persistent infections.

9. Effect of macromolecular crowding agents on human immunodeficiency virus type 1 capsid protein assembly in vitro.

10. High mutant frequency in populations of a DNA virus allows evasion from antibody therapy in an immunodeficient host.

11. A similar pattern of interaction for different antibodies with a major antigenic site of foot-and-mouth disease virus: implications for intratypic antigenic variation.

12. Efficient neutralization of foot-and-mouth disease virus by monovalent antibody binding.

13. A large-scale evaluation of peptide vaccines against foot-and-mouth disease: lack of solid protection in cattle and isolation of escape mutants.

14. Antigenic heterogeneity of a foot-and-mouth disease virus serotype in the field is mediated by very limited sequence variation at several antigenic sites.

15. Evolution of the capsid protein genes of foot-and-mouth disease virus: antigenic variation without accumulation of amino acid substitutions over six decades.

16. Unique amino acid substitutions in the capsid proteins of foot-and-mouth disease virus from a persistent infection in cell culture.

17. Rapid selection of genetic and antigenic variants of foot-and-mouth disease virus during persistence in cattle.