Mark A. Miller
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Featured researches published by Mark A. Miller.
Circulation | 2005
Alessandro Cataliotti; John A. Schirger; Fernando L. Martin; Horng H. Chen; Paul M. McKie; Guido Boerrigter; Lisa C. Costello-Boerrigter; Gail Harty; Denise M. Heublein; Sharon M. Sandberg; Kenneth D. James; Mark A. Miller; Navdeep B. Malkar; Karen Polowy; John C. Burnett
Background—The objective of this study was to address the feasibility and the biological activity of orally administered human brain natriuretic peptide (hBNP). Proprietary technology has been developed in which short, amphiphilic oligomers are covalently attached to peptides. The conjugated peptides are intended to have an improved pharmacokinetic profile and to enable oral administration. We hypothesized that novel oral conjugated hBNP (CONJ-hBNP) increases plasma hBNP, activates cGMP, and reduces mean arterial pressure (MAP). Methods and Results—This randomized crossover-designed study tested the biological activity of oral CONJ-hBNP compared with oral native hBNP in normal conscious dogs. Measurements of MAP, plasma hBNP, and cGMP were made at baseline (BL) and repeated at 10, 30, 60, 120, 180, and 240 minutes after oral administration. Plasma hBNP was not detectable in dogs at BL. Plasma hBNP was detected after native hBNP and CONJ-HBNP administration. However, plasma hBNP concentration was significantly higher after CONJ-hBNP than after native hBNP administration (P=0.0374 between groups). Plasma cGMP increased after CONJ-hBNP for 60 minutes (from 10.8±3 to 36.8±26 pmol/mL; P<0.05), whereas it did not change after native hBNP (P=0.001 between groups). MAP decreased at 10 minutes and remained decreased for 60 minutes after CONJ-hBNP (from 113±8 to 101±12 mm Hg after 10 minutes to 97.5±10 mm Hg after 30 minutes to 99±13 mm Hg after 60 minutes) while remaining unchanged after native hBNP (P=0.0387 between groups). Conclusions—This study reports for the first time that novel conjugated oral BNP activates cGMP and significantly reduces MAP, thus implying an efficacious coupling of CONJ-hBNP to the natriuretic receptor-A. These data advance a new concept of orally administered chronic BNP therapy for cardiovascular diseases.
Archive | 2005
Balasingam Radhakrishnan; Diti Aggarwal; Michelle Ferro; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Monica Puskas; Nnochiri N. Ekwuribe
Archive | 2013
Balasingam Radhakrishnan; ラドークリスナン,バラサイアム; Diti Aggarwal; アガーウォル,ディティ; Michelle Ferro; フェロ,ミシェル; D Kenneth James; ディー. ケニース,ジェームス; Navdeep B. Malkar; マルカー,ナブディープ,ビー.; Mark A. Miller; ミラー,マーク,エー.; Leo Pavliv; パブリブ,レオ; Karen Polowy; ポロウィ,カラン; Karen Puskas; プスカシ,カラン; Nnochirii N. Ekwuribe; エクウィリベ,ノッチーリ,エヌ.
Archive | 2011
Diti Aggarwal; Nnochirii N. Ekwuribe; Michelle Ferro; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Leo Pavliv; Karen Polowy; Karen Puskas; Balasingam Radhakrishnan; アガーウォル,ディティ; エクウィリベ,ノッチーリ,エヌ.; ディー. ケニース,ジェームス; パブリブ,レオ; フェロ,ミシェル; プスカシ,カラン; ポロウィ,カラン; マルカー,ナブディープ,ビー.; ミラー,マーク,エー.; ラドークリスナン,バラサイアム
Archive | 2005
Balasingam Radhakrishnan; Diti Aggarwal; Michelle Ferro; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Leo Pavliv; Karen Polowy; Karen Puskas; Nnochirii N. Ekwuribe
Archive | 2005
Kenneth D. James; Balasingam Radhakrishnan; Navdeep B. Malkar; Mark A. Miller; Nnochiri N. Ekwuribe
Archive | 2005
Balasingam Radhakrishnan; Diti Aggarwal; Michelle Ferro; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Leo Pavliv; Karen Polowy; Karen Puskas; Nnochirii N. Ekwuribe
Archive | 2005
Kenneth D. James; Balasingam Radhakrishnan; Navdeep B. Malkar; Mark A. Miller; Nnochiri N. Ekwuribe
Archive | 2005
Balasingam Radhakrishnan; Diti Aggarwal; Michelle Ferro; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Leo Pavliv; Karen Polowy; Karen Puskas; Nnochirii N. Ekwuribe
Archive | 2005
Balasingam Radhakrishnan; Diti Aggarwal; Kenneth D. James; Navdeep B. Malkar; Mark A. Miller; Karen Polowy; Karen Puskas; Nnochirii N. Ekwuribe; Michelle Ferro; Leo Pavliv