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First-in-human Study to Assess the Safety and Pharmacokinetics of LML134 in Healthy Volunteers (LML134)

2016. október 26. frissítette: Novartis Pharmaceuticals

A First-in-human, Randomized, Double-blind, Placebo-controlled, Single and Multiple Ascending Oral Dose Study, to Assess the Safety, Tolerability and Pharmacokinetics of LML134 in Healthy Volunteers

Phase I study to assess the safety, tolerability and pharmacokinetics of ascending single and multiple doses of the investigational medicinal product in healthy volunteers

A tanulmány áttekintése

Állapot

Befejezve

Körülmények

Beavatkozás / kezelés

Tanulmány típusa

Beavatkozó

Beiratkozás (Tényleges)

133

Fázis

  • 1. fázis

Kapcsolatok és helyek

Ez a rész a vizsgálatot végzők elérhetőségeit, valamint a vizsgálat lefolytatásának helyére vonatkozó információkat tartalmazza.

Tanulmányi helyek

  • Németország
      • Berlin, Németország, 14050
        • Novartis Investigative Site

Részvételi kritériumok

A kutatók olyan embereket keresnek, akik megfelelnek egy bizonyos leírásnak, az úgynevezett jogosultsági kritériumoknak. Néhány példa ezekre a kritériumokra a személy általános egészségi állapota vagy a korábbi kezelések.

Jogosultsági kritériumok

Tanulmányozható életkorok

18 év (Felnőtt)

Egészséges önkénteseket fogad

Nem

Tanulmányozható nemek

Összes

Leírás

Inclusion Criteria:

  • Healthy male and female subjects age 18 to 55 years of age included, and in good health as determined by medical history, physical examination, vital signs, electrocardiogram, and laboratory tests.
  • Written informed consent must be obtained before any assessment is performed.
  • Able to communicate well with the Investigator, to understand and comply with the requirements of the study.

Exclusion Criteria:

  • History or presence of epilepsy or of seizures or convulsions of any kind.
  • Any clinically relevant abnormalities identified in the resting EEG during screening, or pre-ictal signs or other clinically relevant abnormalities in the hyperventilation or intermittent photic stimulation EEG during screening.
  • History of head trauma leading to clinically significant symptoms in the past two years.
  • Applies only to subjects enrolled in Part 2 MAD. Score "yes" on item 4 or item 5 of the Suicidal Ideation section of the C-SSRS, if this ideation occurred in the past 6 months, or "yes" on any item of the Suicidal Behavior section, except for the "Non-Suicidal Self-Injurious Behavior" (item also included in the Suicidal Behavior section), if this behavior occurred in the past 2 years.
  • Significant illness including any clinically significant infectious disease which has not resolved within two (2) weeks prior to initial dosing.
  • History or presence of significant hematological abnormalities or immunodeficiency or any condition that might compromise the immune system (infection, vaccination), of any etiology as indicated by clinically significantly abnormal values of any of the following hematologic parameters: thrombocyte, RBC count, total WBC count and differentials presented as % of total white blood cell count and as absolute concentrations.
  • History or presence of any thyroid disease as indicated by any clinically relevant abnormality on thyroid stimulating hormone test (TSH).
  • History or presence of any chronic eye disease other than refractive error, strabismic amblyopia, or anisometropic amblyopia.
  • Women of child-bearing potential, defined as all women physiologically capable of becoming pregnant.

Tanulási terv

Ez a rész a vizsgálati terv részleteit tartalmazza, beleértve a vizsgálat megtervezését és a vizsgálat mérését.

Hogyan készül a tanulmány?

Tervezési részletek

  • Elsődleges cél: Kezelés
  • Beavatkozó modell: Párhuzamos hozzárendelés
  • Maszkolás: Négyszeres

Fegyverek és beavatkozások

Résztvevő csoport / kar
Beavatkozás / kezelés
Kísérleti: Single dose study part
there will be 8 cohorts of healthy volunteers dosed with single doses of LML134 (8 planned dose levels) or with placebo and 2 potential additional cohorts (also dosed with single dose of LML134 or placebo)
Drog: LML134
LML134 will be administered first as single doses and then as multiple doses
Drog: Placebo
All study cohorts (except food effect cohort) are placebo controlled
Kísérleti: Multiple dose study part
there will be 3 cohorts of healthy volunteers dosed with multiple doses of LML134 (3 planned dose levels) or placebo and one potential additional cohort (also dosed with multiple doses of LML134 or placebo)
Drog: LML134
LML134 will be administered first as single doses and then as multiple doses
Drog: Placebo
All study cohorts (except food effect cohort) are placebo controlled

Mit mér a tanulmány?

Elsődleges eredményintézkedések

Eredménymérő
Intézkedés leírása
Időkeret
Nemkívánatos események értékelése egyszeri és többszöri növekvő dózis beadása után a kiinduláskor és a vizsgálat befejezéséig ismételten
Időkeret: Körülbelül 24 órával az adagolás előtt kezdeni, és az utolsó adag után körülbelül 7-14 napig folytatni
Ez a biztonsági eredmény egyesíti a nemkívánatos eseményeket (AE) tapasztaló alanyok számának mértékét, ezen nemkívánatos események természetét és súlyosságát, valamint a vizsgálati kezelésekkel való kapcsolatukat.
Körülbelül 24 órával az adagolás előtt kezdeni, és az utolsó adag után körülbelül 7-14 napig folytatni
Cardiovascular safety assessments after single and multiple ascending dose administration at baseline and repeatedly until study completion
Időkeret: Starting about 24 hours before dosing and continued until about 7-14 days after last dose
This safety outcome combines the measure of a set of cardiovascular safety parameters extracted from ECGs, 25 hours-Holter ECGs and from vital signs assessments
Starting about 24 hours before dosing and continued until about 7-14 days after last dose
Central nervous system safety assessments after single and multiple ascending dose administration at baseline and repeatedly until study completion
Időkeret: Starting about 24 hours before dosing and continued until about 7-14 days after last dose
This safety outcome combines the measure of a set of central nervous system safety parameters extracted from EEGs and neurological examinations
Starting about 24 hours before dosing and continued until about 7-14 days after last dose
Ocular safety assessments after single and multiple ascending dose administration at baseline and repeatedly until study completion
Időkeret: Starting about 24 hours before dosing and continued until about 7-14 days after last dose
This safety outcome combined the measure of a set of ocular parameters including best corrected visual acuity and other parameters assessed by the mean of slit lamp biomicroscopy and dilated ophthalmoscopy examinations and by optical coherence tomography and electroretinography
Starting about 24 hours before dosing and continued until about 7-14 days after last dose
General safety assessments after single and multiple ascending dose administration at baseline and repeatedly until study completion
Időkeret: Starting about 24 hours before dosing and continued until about 7-14 days after last dose
This general safety outcome combines the measure of blood laboratory parameters and the outcome of physical examinations
Starting about 24 hours before dosing and continued until about 7-14 days after last dose

Másodlagos eredményintézkedések

Eredménymérő
Intézkedés leírása
Időkeret
Pharmacokinetics (PK) of LML134: time to reach the maximum concentration after a single drug administration (Tmax) in Part 1 and in Part 3
Időkeret: Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)

Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h and 36h post dose, on Day 3: 48h and 60h post dose and on Day 4: 72h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above, in Parts 1 and 3.

In Part 3, the outcome measure is done once without food intake and once after the intake of a high fat breakfast (in 2 different periods). Both outcomes (with and without breakfast intake) will be compared to assess the effect of a high fast breakfast on LML134 Tmax
Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)
PK of LML134: Observed maximum serum concentration following single drug administration (Cmax) in Part 1 and Part 3
Időkeret: Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)

Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h and 36h post dose, on Day 3: 48h and 60h post dose and on Day 4: 72h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above, in Parts 1 and 3.

In Part 3, the outcome measure is done once without food intake and once after the intake of a high fat breakfast (in 2 different periods). Both outcomes (with and without breakfast intake) will be compared to assess the effect of a high fast breakfast on LML134 Cmax.
Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)
PK of LML134: Area under the serum concentration-time curve from time zero to the time of last quantifiable concentration (AUClast) in Part 1 and Part 3
Időkeret: Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h and 36h post dose, on Day 3: 48h and 60h post dose and on Day 4: 72h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above, in Parts 1 and 3. In Part 3, the outcome measure is done once without food intake and once after the intake of a high fat breakfast (in 2 different periods). Both outcomes (with and without breakfast intake) will be compared to assess the effect of a high fast breakfast on LML134 AUClast.
Starting 1hour prior to dosing on Day 1 and until 72 hours after dosing (Day 4)
PK of LML134: time to reach the maximum concentration after the first drug administration (Tmax) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose and on Day 2: 24h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
PK of LML134: time to reach the maximum concentration after the last drug administration (Tmax) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
PK of LML134: Observed maximum serum concentration following the first drug administration (Cmax) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose and on Day 2: 24h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
PK of LML134: Observed maximum serum concentration following drug administration at steady state (Cmax,ss) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
PK of LML134: Area under the serum concentration-time curve from time zero to the time of last quantifiable concentration (AUClast) after the first dose administration in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose and on Day 2: 24h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 24hr after the first dose administration on Day 2
PK of LML134: The area under the serum concentration-time curve from time zero to the end of the dosing interval tau at steady state (AUCtau,ss) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
PK of LML134: The average steady state serum concentration during multiple dosing (Cav,ss) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
PK of LML134: The effective half-life based on drug accumulation at steady state (T1/2,acc) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
PK of LML134: The accumulation ratio (Racc) in Part 2
Időkeret: Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)
Serum samples will be collected on Day 1: 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 2: 24h post dose, on Day 3: 1hr prior the second dose administration, on Days 4, 5, 6, 8, 10, 12, 13, 14: 1hr prior dosing, on Day 15 (last time the drug is administered): 1hr predose; 0,25h; 0,5h; 1h; 1,5h; 2h; 3h; 4h; 6h; 8h; 12h; 16h post dose, on Day 16: 24h post dose and Day 17: 48h post dose. This outcome measure shows the mean of all subject values resulting from each time point specified above.
Starting 1hour prior the first dose administration (Day 1) until 48hour after the last dose administration (Day 17)

Együttműködők és nyomozók

Itt találhatja meg a tanulmányban érintett személyeket és szervezeteket.

Szponzor

Novartis Pharmaceuticals

Nyomozók

  • Tanulmányi igazgató: Study Director, Novartis Pharmceuticals

Tanulmányi rekorddátumok

Ezek a dátumok nyomon követik a ClinicalTrials.gov webhelyre benyújtott vizsgálati rekordok és összefoglaló eredmények benyújtásának folyamatát. A vizsgálati feljegyzéseket és a jelentett eredményeket a Nemzeti Orvostudományi Könyvtár (NLM) felülvizsgálja, hogy megbizonyosodjon arról, hogy megfelelnek-e az adott minőség-ellenőrzési szabványoknak, mielőtt közzéteszik őket a nyilvános weboldalon.

Tanulmány főbb dátumok

Tanulmány kezdete

2015. február 1.

Elsődleges befejezés (Tényleges)

2016. február 1.

A tanulmány befejezése (Tényleges)

2016. február 1.

Tanulmányi regisztráció dátumai

Először benyújtva

2014. november 14.

Először nyújtották be, amely megfelel a minőségbiztosítási kritériumoknak

2015. január 6.

Első közzététel (Becslés)

2015. január 8.

Tanulmányi rekordok frissítései

Utolsó frissítés közzétéve (Becslés)

2016. október 27.

Az utolsó frissítés elküldve, amely megfelel a minőségbiztosítási kritériumoknak

2016. október 26.

Utolsó ellenőrzés

2016. október 1.

Több információ

A tanulmányhoz kapcsolódó kifejezések

Kulcsszavak

Egyéb vizsgálati azonosító számok

  • CLML134X2101
  • 2014-000937-22 (EudraCT szám)

Ezt az információt közvetlenül a clinicaltrials.gov webhelyről szereztük be, változtatás nélkül. Ha bármilyen kérése van vizsgálati adatainak módosítására, eltávolítására vagy frissítésére, kérjük, írjon a következő címre: register@clinicaltrials.gov. Amint a változás bevezetésre kerül a clinicaltrials.gov oldalon, ez a webhelyünkön is automatikusan frissül. .

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