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RSC Drug Discovery Series | 2015

CHAPTER 6:The Molecular Diversity of Conoidean Venom Peptides and their Targets: From Basic Research to Therapeutic Applications

Russell W. Teichert; Baldomero M. Olivera; J. Michael McIntosh; Grzegorz Bulaj; Martin P. Horvath

The >10 000 species of venomous marine snails (superfamily Conoidea) have evolved sophisticated chemical strategies to interact with other animals in their environment. A conoidean venom typically contains 50–200 peptides unique to that species, each honed by natural selection to interact with a specific molecular target in the prey, predators or competitors of the snail. The diversity and molecular targeting specificity of conoidean venom peptides has provided sets of ligands that allow the pharmacological differentiation of different subtypes in large ion channel/receptor families (such as Na channels and nicotinic receptors). Conoidean venoms contain multiple sets of peptides, known as “cabals”, acting in concert on functionally linked molecular targets to achieve a specific physiological end-point, such as paralysis or excitotoxic shock. Each cabal targets a cognate “constellation” of receptors and ion channels in a physiological circuit. For example, the “motor cabal” causes neuromuscular paralysis, with different peptides of the cabal targeting specific motor constellation components, including Ca channels in motor neurons, Na channels and nAChRs in muscle. The elucidation of venom-peptide cabals and receptor/ion-channel constellations has inspired a new pharmacological paradigm called “Constellation Pharmacology” with the potential to transform both the discovery of novel pharmacological agents and the development of therapeutic drugs.


Journal of Biological Chemistry | 1996

A new alpha-conotoxin which targets alpha3beta2 nicotinic acetylcholine receptors.

G.E Cartier; Doju Yoshikami; William R. Gray; Siqin Luo; Baldomero M. Olivera; J M McIntosh


Journal of Biological Chemistry | 1987

Neuronal calcium channel inhibitors. Synthesis of omega-conotoxin GVIA and effects on 45Ca uptake by synaptosomes.

Jean Rivier; Robert Galyean; W R Gray; A Azimi-Zonooz; J M McIntosh; Lourdes J. Cruz; Baldomero M. Olivera


Archive | 1996

A new a-conotoxin which targets a3b2 nicotinic acetylcholine receptors

G. Edward Cartier; Doju Yoshikami; William R. Gray; Shujun Luo; Baldomero M. Olivera; J. Michael McIntosh


Journal of Biological Chemistry | 1981

The pyridine nucleotide cycle. Studies in Escherichia coli and the human cell line D98/AH2.

David R. Hillyard; Martin Rechsteiner; P Manlapaz-Ramos; Julita S. Imperial; Lourdes J. Cruz; Baldomero M. Olivera


Journal of Biological Chemistry | 2000

Nuclear Magnetic Resonance Solution Conformation of α-Conotoxin AuIB, an α3β4 Subtype-selective Neuronal Nicotinic Acetylcholine Receptor Antagonist

Jee Hyun Cho; K. Hun Mok; Baldomero M. Olivera; J. Michael McIntosh; Kyu Hwan Park; Kyou Hoon Han


Philippine science letters | 2010

THE INDO-PACIFIC GEMMULA SPECIES IN THE SUBFAMILY TURRINAE: ASPECTS OF FIELD DISTRIBUTION, MOLECULAR PHYLOGENY, RADULAR ANATOMY AND FEEDING ECOLOGY

Francisco M. Heralde; Yuri I. Kantor; Mary Anne Q. Astilla; Arturo O. Lluisma; Rollan Geronimo; Porfirio M. Aliño; Maren Watkins; Patrice Showers Corneli; Baldomero M. Olivera; Ameurfina D. Santos; Gisela P. Concepcion


Archive | 1997

USE OF CONOTOXIN PEPTIDES ImI AND MII AS CARDIOVASCULAR AGENTS

J. Michael McIntosh; Baldomero M. Olivera; Doju Yoshikami


Archive | 2015

Conopeptides, Marine Natural Products from Venoms: Biomedical Applications and Future Research Applications

Baldomero M. Olivera; Helena Safavi-­Hemami; Martin P. Horvath; Russell W. Teichert


Archive | 1999

Kappa-A conopeptides and uses therefor

Richard T. Layer; Karen Pemberton; Robert N. Jones; James E. Garrett; Baldomero M. Olivera; John A. McIntosh; David R. Hillyard; Michelle Grilley; Maren Watkins; Ameurfina D. Santos; Glenn C. Zafaralla; A. Craig

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Lourdes J. Cruz

University of the Philippines Diliman

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