JE Foley scite author profile

1 The effect of single oral doses of six P-receptor antagonists on exercise-induced changes in double product (systolic blood pressure x heart rate) were studied in 25 human volunteers. 2 Three doses of propranolol, nadolol, oxprenolol, pindolol, timolol and atenolol were selected for study on the basis of in vivo P-blocking potency. 3 Although all P-blockers studied reduced the double product response to exercise, the pharmacodynamics of this effect differed markedly. 4 Pharmacodynamic half-lives, estimated for the drugs tested, were 39 h for nadolol, atenolol 21 h, timolol 15 h, oxprenolol 13 h, propranolol 11 and pindolol 8 h. 5 These results suggest that the clinical choice of a1-blocker with the least problems of compliance can be made on the basis of pharmacodynamics as well as pharmacological profile.

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Nateglinide, but not glyburide, selectively enhances early insulin release and more effectively controls post-meal glucose excursions with less total insulin exposure

Hollander¹,

Schwartz²,

Gatlin³

et al. 2000

Diabetes Research and Clinical Practice

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Quantifizierung des Inkretineffekts bei Patienten mit Typ 2-Diabetes unter Therapie mit dem DPP-4-Inhibitor („Inkretin-Verstärker“) Vildagliptin bzw. Plazebo

Vardarli¹,

Becker²,

Koethe³

et al. 2010

Diabetologie und Stoffwechsel

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JE Foley

Adverse effects of dipeptidyl peptidases 8 and 9 inhibition in rodents revisited

Effect of beta‐blockers on exercise double product (systolic blood pressure x heart rate).

Nateglinide, but not glyburide, selectively enhances early insulin release and more effectively controls post-meal glucose excursions with less total insulin exposure

Quantifizierung des Inkretineffekts bei Patienten mit Typ 2-Diabetes unter Therapie mit dem DPP-4-Inhibitor („Inkretin-Verstärker“) Vildagliptin bzw. Plazebo

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