PMID- 20637971
OWN - NLM
STAT- MEDLINE
DCOM- 20101116
LR  - 20151119
IS  - 1879-114X (Electronic)
IS  - 0149-2918 (Linking)
VI  - 32
IP  - 6
DP  - 2010 Jun
TI  - Linagliptin, a dipeptidyl peptidase-4 inhibitor in development for the treatment 
      of type 2 diabetes mellitus: a Phase I, randomized, double-blind, 
      placebo-controlled trial of single and multiple escalating doses in healthy adult 
      male Japanese subjects.
PG  - 1188-204
LID - 10.1016/j.clinthera.2010.06.004 [doi]
AB  - BACKGROUND: The dipeptidyl peptidase-4 (DPP-4) inhibitor linagliptin is in 
      clinical development for the treatment of type 2 diabetes mellitus (T2DM). In 
      previous studies in non-Japanese populations, linagliptin showed potential as a 
      once-daily oral antidiabetic drug. OBJECTIVE: This study investigated the 
      tolerability, pharmacokinetics, and pharmacodynamics of linagliptin in healthy 
      adult male Japanese volunteers, in compliance with Japanese regulatory 
      requirements for new drugs intended for use in humans. METHODS: This was a Phase 
      I, randomized, doubleblind, placebo-controlled study in healthy volunteers. 
      Linagliptin or placebo was administered as single escalating doses of 1, 2.5, 5, 
      and 10 mg, or as multiple escalating doses of 2.5, 5, and 10 mg once daily for 12 
      days. Three quarters of subjects in each dose group were randomized to active 
      drug and one quarter to placebo. Blood and urine samples for determination of 
      pharmacokinetic parameters were obtained before administration of the first dose 
      of study drug and at regular time points after administration, with more frequent 
      blood sampling on days 1 and 12 in subjects receiving multiple doses. Inhibition 
      of DPP-4 activity and plasma concentrations of glucagon-like peptide-1 (GLP-1) 
      and glucose were also determined. Tolerability was assessed throughout the study 
      based on physical examinations, 12-lead ECGs, and standard laboratory tests. 
      RESULTS: Eight subjects were enrolled in each dose group, 6 receiving active drug 
      and 2 receiving placebo. Baseline demographic characteristics were comparable in 
      the single-dose groups (mean [SD] age, 24.5 [3.6] years; mean weight, 61.2 [6.2] 
      kg; mean height, 171.5 [5.3] cm) and multiple-dose groups (mean age, 25.4 [3.7] 
      years; mean weight, 61.6 [5.2] kg; mean height, 170.9 [4.9] cm). Linagliptin 
      displayed nonlinear pharmacokinetics. Total systemic exposure (AUC and C(max)) 
      increased in a manner that was less than dose proportional. T(max) ranged from 
      1.50 to 6.00 hours, and elimination t((1/2)) ranged from 96.9 to 175.0 hours. 
      Total CL increased with increasing dose (from 140 mL/min in the 1-mg group to 314 
      mL/min in the 10-mg group), as did apparent V(d) (from 1260 to 3060 L with doses 
      up to 10 mg). Steady state was attained within 2 to 3 days. The accumulation 
      t((1/2)) ranged from approximately 10 to 15 hours. The accumulation ratio with 
      multiple dosing was <1.5 and decreased with increasing dose (approximately 1.2 in 
      the 10-mg dose). Urinary excretion increased with increasing dose and over time 
      in all dose groups, although it did not exceed 7% in any dose group on day 12. 
      Linagliptin inhibited plasma DPP-4 activity in a dose-dependent manner. Mean 
      DPP-4 inhibition was >or=80% over 24 hours after a single dose of 10 mg and after 
      multiple doses of 5 and 10 mg for 12 days. Postprandial plasma GLP-1 
      concentrations increased from preprandial concentrations by 2- to 4-fold after 
      administration of single doses and by 2- to 2.5-fold on day 12 after 
      administration of multiple doses. Baseline (premeal) plasma GLP-1 concentrations 
      were higher on day 12 than on day 1 in all linagliptin groups. A total of 3 
      adverse events were reported in 1 subject each: an increase in histamine 
      concentration in a subject receiving a single dose of linagliptin 5 mg, vasovagal 
      syncope in a subject receiving a single dose of linagliptin 10 mg, and 
      pharyngitis in a subject receiving multiple doses of linagliptin 10 mg. None of 
      these events was considered drug related. No episodes of hypoglycemia occurred 
      during the study. CONCLUSIONS: In this short-term study in healthy adult male 
      Japanese volunteers, multiple oral doses of linagliptin inhibited plasma DPP-4 
      activity and elevated active GLP-1 concentrations in a dose-dependent manner, 
      with no episodes of hypoglycemia. Multiple dosing of linagliptin for 12 days was 
      well tolerated and exhibited a pharmacokinetic/pharmacodynamic profile consistent 
      with a once-daily regimen. Clinical studies in Japanese patients with T2DM appear 
      to be warranted.
FAU - Sarashina, Akiko
AU  - Sarashina A
AD  - Pharmacokinetics and Non-clinical Safety Department, Nippon Boehringer Ingelheim 
      Co., Ltd., Kobe, Hyogo, Japan. sarasina@kaw.boehringeringelheim.com
FAU - Sesoko, Shogo
AU  - Sesoko S
FAU - Nakashima, Mitsuyoshi
AU  - Nakashima M
FAU - Hayashi, Naoyuki
AU  - Hayashi N
FAU - Taniguchi, Atsushi
AU  - Taniguchi A
FAU - Horie, Yoshiharu
AU  - Horie Y
FAU - Graefe-Mody, Eva U
AU  - Graefe-Mody EU
FAU - Woerle, Hans-Juergen
AU  - Woerle HJ
FAU - Dugi, Klaus A
AU  - Dugi KA
LA  - eng
PT  - Clinical Trial, Phase I
PT  - Journal Article
PT  - Randomized Controlled Trial
PT  - Research Support, Non-U.S. Gov't
PL  - United States
TA  - Clin Ther
JT  - Clinical therapeutics
JID - 7706726
RN  - 0 (Dipeptidyl-Peptidase IV Inhibitors)
RN  - 0 (Hypoglycemic Agents)
RN  - 0 (Purines)
RN  - 0 (Quinazolines)
RN  - 3X29ZEJ4R2 (Linagliptin)
SB  - IM
MH  - Adult
MH  - Area Under Curve
MH  - Diabetes Mellitus, Type 2/*drug therapy
MH  - Dipeptidyl-Peptidase IV Inhibitors/adverse effects/*pharmacokinetics/pharmacology
MH  - Dose-Response Relationship, Drug
MH  - Double-Blind Method
MH  - Half-Life
MH  - Humans
MH  - Hypoglycemic Agents/adverse effects/*pharmacokinetics/pharmacology
MH  - Japan
MH  - Linagliptin
MH  - Male
MH  - Metabolic Clearance Rate
MH  - Purines/adverse effects/*pharmacokinetics/pharmacology
MH  - Quinazolines/adverse effects/*pharmacokinetics/pharmacology
EDAT- 2010/07/20 06:00
MHDA- 2010/11/17 06:00
CRDT- 2010/07/20 06:00
PHST- 2010/04/20 00:00 [accepted]
PHST- 2010/07/20 06:00 [entrez]
PHST- 2010/07/20 06:00 [pubmed]
PHST- 2010/11/17 06:00 [medline]
AID - S0149-2918(10)00195-5 [pii]
AID - 10.1016/j.clinthera.2010.06.004 [doi]
PST - ppublish
SO  - Clin Ther. 2010 Jun;32(6):1188-204. doi: 10.1016/j.clinthera.2010.06.004.