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Dive into the research topics where James Patrick Mcdonough is active.

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Featured researches published by James Patrick Mcdonough.


Pharmaceutical Research | 2001

Oral Delivery of Biologically Active Parathyroid Hormone

Andrea Leone-Bay; Masahiko Sato; Duncan R. Paton; Ann H. Hunt; Donald J. Sarubbi; Monica Carozza; James Z. Chou; James Patrick Mcdonough; Robert A. Baughman

AbstractPurpose. Parathyroid hormone (PTH), the only drug known to stimulate bone formation, is a peptide therapeutic indicated in the treatment of osteoporosis. Unfortunately, PTH is only effective when dosed by injection because it has no oral bioavailability. Herein we report the oral absorption of PTH in rats and monkeys facilitated by the novel delivery agent, N-[8-(2-hydroxy-4-methoxy)bensoyl]amino caprylic acid (4-MOAC). Methods. 4-MOAC was selected from a group of 100 delivery agents based on in vitro chromotography studies and in vivo screening studies in rats. The PTH/4-MOAC combination was then tested in monkeys. The interaction of 4-MOAC and PTH was evaluated by nuclear magnetic resonance (NMR) spectroscopy. Results. Monkeys were administered an aqueous solution containing 4-MOAC and PTH and mean peak serum PTH concentrations of about 3000 pg/mL were obtained. The relative bioavailability of oral PTH was 2.1% relative to subcutaneous administration. The biological activity of the orally-delivered PTH was further evaluated in a rat model of osteoporosis. These studies showed that the bone formed following oral PTH/4-MOAC administration was comparable to that formed following PTH injections. The 4-MOAC mediated absorption of PTH is hypothesized to be the result of a noncovalent interaction between 4-MOAC and PTH. The preliminary evaluation of this interaction by NMR is described. Conclusions. 4-MOAC facilitates the absorption of PTH following oral administration to both rats and monkeys. The orally-absorbed PTH is biologically active as demonstrated in a rat model of osteoporosis.


Archive | 1989

Method for the reduction of heterogeneity of monoclonal antibodies

James Patrick Mcdonough; Thomas Charles Furman; Richard Mark Bartholomew; Rodney Alan Jue


Archive | 1990

Enzymatic removal of a protein amino-terminal sequence

Gerald W. Becker; Thomas Charles Furman; Warren Cameron Mackellar; James Patrick Mcdonough


Archive | 1993

Selective removal of N-terminal extensions from folded insulin precursors using dipeptidyl-aminopeptidase-1

Bruce Hill Frank; Thomas Charles Furman; James Patrick Mcdonough


Archive | 1990

ENZYMATIC PROCESS FOR PRODUCING A PRECURSOR TO HUMAN INSULIN OR A MODIFIED HUMAN INSULIN

Gerald W. Becker; Thomas Charles Furman; Warren Cameron Mackellar; James Patrick Mcdonough


Drug Information Journal | 2003

Project Management as a Discipline within Pharmaceutical Contract Research Organizations

Ellis Wilson; James Patrick Mcdonough; William Allbee; Jann Nielsen


Biopharm International | 2003

The Project Management Institute's Pharmaceutical Specific Interest Group 2002 Benchmark Survey results: Project managers and project management in the biotech industry

Ellis Wilson; James Patrick Mcdonough; William Allbee; Jann Nielsen


Archive | 1995

METHOD FOR THE SELECTIVE REMOVAL OF N-TERMINAL EXTENSIONS FROM FOLDED INSULIN PRECURSORS USING DIPEPTIDYL-AMINOPEPTIDASE-1

Bruce Hill Frank; Thomas Charles Furman; James Patrick Mcdonough


Archive | 1992

REDUCTION PROCESS OF HETEROGENEITY OF MONOCLONAL ANTIBODIES

Batholomew Richard Mark; Thomas Charles Furman; Rodney Alan Jue; James Patrick Mcdonough


Archive | 1990

Enzymatische Entfernung einer aminoterminalen Proteinsequenz. Enzymatic removal of an amino-terminal protein sequence.

Gerald W. Becker; Thomas Charles Furman; Warren Cameron Mackellar; James Patrick Mcdonough

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