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TRIple in Astma VYSOKÁ SÍLA VERSUS ICS/Laba hs a tiotRopium (TRIGGER) (TRIGGER)

4. května 2026 aktualizováno: Chiesi Farmaceutici S.p.A.

52 TÝDENNÍ, RANDOMIZOVANÁ, DVOJITÁ SLEPÁ, MULTINACIONÁLNÍ, MULTICENTROVÁ, AKTIVNĚ ŘÍZENÁ, 3-RAMENOVÁ PARALELNÍ SKUPINOVÁ ZKOUŠKA POROVNÁVAJÍCÍ CHF 5993 200/6/12,5 µg pMDI (Pevná KOMBINACE EXTRAFINE BECLOMETIONATE1 52,5 µg PMDI GUMDIUM 2 PLUSFONEFYARIMOMETIONATE15 /6 µg pMDI (Pevná KOMBINACE EXTRAFINE BECLOMETHASONE DIPROPIONATE PLUS FORMOTEROL FUMARATE) SAMOSTATNĚ NEBO NA VRCHNĚ OPEN-LABEL TIOTROPIUM 2,5 µg RESPIMAT® U PACIENTŮ S ASTmatem CO2 NEKONTROLOVANÝM PŘI VYSOKÉM KONTROLOVANÉM CORTIO-DÁVKOVÁNÍ

Účelem této studie je vyhodnotit nadřazenost CHF 5993 200/6/12,5 µg pMDI (fixní kombinace extra jemného beklometason dipropionátu plus formoterol fumarát plus glykopyrronium bromid) versus CHF 1535 200/6 µg pMDI (fixní kombinace extra jemného beklometason dipropionátu plus formoterol fumarát) a k porovnání účinku CHF0503F/0503F/92 ug pMDI vs. CHF 5993 200/6/12,5 µg plus otevřené tiotropium 2,5 µg, pokud jde o parametry plicních funkcí a četnost exacerbací, jakož i pro posouzení jeho bezpečnosti a některých zdravotně ekonomických výsledků.

Přehled studie

Postavení

Dokončeno

Podmínky

Intervence / Léčba

Detailní popis

This was a phase III, multicentre, randomised, double-blind study, with an open-label arm, active-controlled, 3-arm parallel group study to demonstrate both the superiority of CHF 5993 pMDI 200/6/12.5 μg compared with CHF 1535 pMDI 200/6 μg in terms of change from baseline in pre-dose FEV1 at Week 26 and a reduction of moderate and severe asthma exacerbation rate with CHF 5993 pMDI 200/6/12.5 μg compared to CHF 1535 pMDI 200/6 μg during the entire 52-week treatment period.

The study was performed in patients with uncontrolled asthma on high doses of inhaled corticosteroids (ICS) in combination with long acting β2-agonists LABAs). The study was conducted in accordance with the Declaration of Helsinki, Good Clinical Practice guidelines and all other requirements of local laws.

Patients completed the electronic diary (eDiary)/electronic peak flow meter (ePeakflowmeter) twice daily at home from screening to Week 52, recording asthma symptoms, treatment compliance, rescue intake and peak expiratory flow (PEF). The Asthma Control Questionnaire© (ACQ)-7 was completed at all visits from screening to Week 52. The EuroQuality of Life-5-Dimensional-3-Level (EQ-5D-3L™) questionnaire was completed at all visits from randomisation to Week 52. Health economic information was collected during the study. An independent Data Safety Monitoring Board was established for evaluation of the study and impartial safety assurance for patients. An Adjudication Committee was established to evaluate Major Adverse Cardiovascular Events.

Primary objective of the study were:

  • To demonstrate the superiority of CHF 5993 pMDI 200/6/12.5 μg compared with CHF 1535 pMDI 200/6 μg in terms of change from baseline in pre-dose forced expiratory volume in the 1st second (FEV1) at Week 26;
  • To demonstrate the reduction of moderate and severe asthma exacerbations rate with CHF 5993 pMDI 200/6/12.5 μg compared with CHF 1535 pMDI 200/6 μg during the entire 52-week treatment period.

The secondary endpoints included pooled analyse of 2 pivotal studies; this study (TRIGGER) and study (TRIMARAN). These 2 studies have similar study designs and study population.

CHF 1535 pMDI: fixed-dose combination (FDC) of BDP + FF + GB Dose: BDP 200 μg, FF 6 μg, GB 12.5 μg per actuation, 2 inhalations, BID. Total daily dose: BDP 800 μg, FF 24 μg, GB 50 μg.

BDP: Beclometasone dipropionate FF: Formoterol fumarate GB: Glycopyrronium bromide

Typ studie

Intervenční

Zápis (Aktuální)

1437

Fáze

  • Fáze 3

Kontakty a umístění

Tato část poskytuje kontaktní údaje pro ty, kteří studii provádějí, a informace o tom, kde se tato studie provádí.

Studijní místa

  • Argentina
      • Buenos Aires, Argentina
        • Chiesi Clinical Trial Site 432702
      • CABA, Argentina
        • Chiesi Clinical Trial Site 432704
      • Mar del Plata, Argentina
        • Chiesi Clinical Trial Site 432705
      • Quilmes, Argentina
        • Chiesi Clinical Trial Site 432701
      • San Miguel de Tucumán, Argentina
        • Chiesi Clinical Trial Site 432703
      • San Miguel de Tucumán, Argentina
        • Chiesi Clinical Trial Site 432706
  • Bulharsko
      • Blagoevgrad, Bulharsko
        • Chiesi Clinical Trial Site 100707
      • Burgas, Bulharsko
        • Chiesi Clinical Trial Site 100720
      • Gabrovo, Bulharsko
        • Chiesi Clinical Trial Site 100718
      • Haskovo, Bulharsko
        • Chiesi Clinical Trial Site 100713
      • Montana, Bulharsko
        • Chiesi Clinical Trial Site 100722
      • Pleven, Bulharsko
        • Chiesi Clinical Trial Site 100702
      • Plovdiv, Bulharsko
        • Chiesi Clinical Trial Site 100705
      • Plovdiv, Bulharsko
        • Chiesi Clinical Trial Site 100708
      • Plovdiv, Bulharsko
        • Chiesi Clinical Trial Site 100715
      • Rousse, Bulharsko
        • Chiesi Clinical Trial Site 100716
      • Sofia, Bulharsko
        • Chiesi Clinical Trial Site 100701
      • Sofia, Bulharsko
        • Chiesi Clinical Trial Site 100703
      • Sofia, Bulharsko
        • Chiesi Clinical Trial Site 100704
      • Sofia, Bulharsko
        • Chiesi Clinical Trial Site 100709
      • Sofia, Bulharsko
        • Chiesi Clinical Trial Site 100719
      • Stara Zagora, Bulharsko
        • Chiesi Clinical Trial Site 100706
      • Stara Zagora, Bulharsko
        • Chiesi Clinical Trial Site 100712
      • Varna, Bulharsko
        • Chiesi Clinical Trial Site 100710
      • Vidin, Bulharsko
        • Chiesi Clinical Trial Site 100711
      • Vidin, Bulharsko
        • Chiesi Clinical Trial Site 100721
  • Bělorusko
      • Homyel, Bělorusko
        • Chiesi Clinical Trial Site 112703
      • Homyel, Bělorusko
        • Chiesi Clinical Trial Site 112704
      • Minsk, Bělorusko
        • Chiesi Clinical Trial Site 112701
      • Minsk, Bělorusko
        • Chiesi Clinical Trial Site 112702
      • Minsk, Bělorusko
        • Chiesi Clinical Trial Site 112705
  • Itálie
      • Bologna, Itálie
        • Chiesi Clinical Trial Site 380704
      • Catania, Itálie
        • Chiesi Clinical Trial Site 380703
      • Genova, Itálie
        • Chiesi Clinical Trial Site 380701
      • Palermo, Itálie
        • Chiesi Clinical Trial Site 380705
      • Pavia, Itálie
        • Chiesi Clinical Trial Site 380702
      • Tradate, Itálie
        • Chiesi Clinical Trial Site 380706
  • Litva
      • Vilnius, Litva
        • Chiesi Clinical Trial Site 440702
      • Vilnius, Litva
        • Chiesi Clinical Trial Site 440703
      • Vilnius, Litva
        • Chiesi Clinical Trial Site 440705
      • Šiauliai, Litva
        • Chiesi Clinical Trial Site 440701
  • Maďarsko
      • Balassagyarmat, Maďarsko
        • Chiesi Clinical Trial Site 348707
      • Budapest, Maďarsko
        • Chiesi Clinical Trial Site 348715
      • Debrecen, Maďarsko
        • Chiesi Clinical Trial Site 348721
      • Gödöllő, Maďarsko
        • Chiesi Clinical Trial Site 348712
      • Hatvan, Maďarsko
        • Chiesi Clinical Trial Site 348718
      • Komárom, Maďarsko
        • Chiesi Clinical Trial Site 348717
      • Létavértes, Maďarsko
        • Chiesi Clinical Trial Site 348709
      • Monor, Maďarsko
        • Chiesi Clinical Trial Site 348703
      • Mórahalom, Maďarsko
        • Chiesi Clinical Trial Site 348719
      • Nyíregyháza, Maďarsko
        • Chiesi Clinical Trial Site 348704
      • Nyíregyháza, Maďarsko
        • Chiesi Clinical Trial Site 348714
      • Pécs, Maďarsko
        • Chiesi Clinical Trial Site 348713
      • Pécs, Maďarsko
        • Chiesi Clinical Trial Site 348720
      • Siófok, Maďarsko
        • Chiesi Clinical Trial Site 348702
      • Szarvas, Maďarsko
        • Chiesi Clinical Trial Site 348706
      • Szeged, Maďarsko
        • Chiesi Clinical Trial Site 348701
      • Szombathely, Maďarsko
        • Chiesi Clinical Trial Site 348705
      • Vásárosnamény, Maďarsko
        • Chiesi Clinical Trial Site 348710
      • Érd, Maďarsko
        • Chiesi Clinical Trial Site 348708
  • Německo
      • Berlin, Německo
        • Chiesi Clinical Trial Site 276709
      • Berlin, Německo
        • Chiesi Clinical Trial Site 276712
      • Bonn, Německo
        • Chiesi Clinical Trial Site 276711
      • Frankfurt am Main, Německo
        • Chiesi Clinical Trial Site 276707
      • Frankfurt am Main, Německo
        • Chiesi Clinical Trial Site 276714
      • Hamburg, Německo
        • Chiesi Clinical Trial Site 276705
      • Hanover, Německo
        • Chiesi Clinical Trial Site 276703
      • Koblenz, Německo
        • Chiesi Clinical Trial Site 276708
      • Leipzig, Německo
        • Chiesi Clinical Trial Site 276702
      • Leipzig, Německo
        • Chiesi Clinical Trial Site 276704
      • Leipzig, Německo
        • Chiesi Clinical Trial Site 276710
      • Mainz, Německo
        • Chiesi Clinical Trial Site 276715
      • München, Německo
        • Chiesi Clinical Trial Site 276701
      • Münster, Německo
        • Chiesi Clinical Trial Site 276713
      • Rosenheim, Německo
        • Chiesi Clinical Trial Site 276716
  • Polsko
      • Bialystok, Polsko
        • Chiesi Clinical Trial Site 616713
      • Bialystok, Polsko
        • Chiesi Clinical Trial Site 616718
      • Bielsko-Biala, Polsko
        • Chiesi Clinical Trial Site 616722
      • Bienkówka, Polsko
        • Chiesi Clinical Trial Site 616702
      • Bydgoszcz, Polsko
        • Chiesi Clinical Trial Site 616727
      • Giżycko, Polsko
        • Chiesi Clinical Trial Site 616704
      • Grudziądz, Polsko
        • Chiesi Clinical Trial Site 616716
      • Katowice, Polsko
        • Chiesi Clinical Trial Site 616725
      • Katowice, Polsko
        • Chiesi Clinical Trial Site 616729
      • Krakow, Polsko
        • Chiesi Clinical Trial Site 616719
      • Krakow, Polsko
        • Chiesi Clinical Trial Site 616734
      • Krakow, Polsko
        • Chiesi Clinical Trial Site 616736
      • Lodz, Polsko
        • Chiesi Clinical Trial Site 616707
      • Lodz, Polsko
        • Chiesi Clinical Trial Site 616708
      • Lodz, Polsko
        • Chiesi Clinical Trial Site 616711
      • Lodz, Polsko
        • Chiesi Clinical Trial Site 616726
      • Mrozy, Polsko
        • Chiesi Clinical Trial Site 616733
      • Ostróda, Polsko
        • Chiesi Clinical Trial Site 616717
      • Otwock, Polsko
        • Chiesi Clinical Trial Site 616731
      • Pabianice, Polsko
        • Chiesi Clinical Trial Site 616703
      • Poznan, Polsko
        • Chiesi Clinical Trial Site 616709
      • Poznan, Polsko
        • Chiesi Clinical Trial Site 616728
      • Proszowice, Polsko
        • Chiesi Clinical Trial Site 616720
      • Rzeszów, Polsko
        • Chiesi Clinical Trial Site 616723
      • Rzeszów, Polsko
        • Chiesi Clinical Trial Site 616735
      • Skierniewice, Polsko
        • Chiesi Clinical Trial Site 616721
      • Strzelce Opolskie, Polsko
        • Chiesi Clinical Trial Site 616732
      • Tarnów, Polsko
        • Chiesi Clinical Trial Site 616710
      • Warsaw, Polsko
        • Chiesi Clinical Trial Site 616701
      • Wilkowice, Polsko
        • Chiesi Clinical Trial Site 616730
      • Wroclaw, Polsko
        • Chiesi Clinical Trial Site 616705
      • Wroclaw, Polsko
        • Chiesi Clinical Trial Site 616714
      • Wroclaw, Polsko
        • Chiesi Clinical Trial Site 616715
      • Świdnik, Polsko
        • Chiesi Clinical Trial Site 616712
  • Portugalsko
      • Aveiro, Portugalsko
        • Chiesi Clinical Trial Site 620704
      • Figueira da Foz Municipality, Portugalsko
        • Chiesi Clinical Trial Site 620703
      • Lisbon, Portugalsko
        • Chiesi Clinical Trial Site 620702
      • Loures, Portugalsko
        • Chiesi Clinical Trial Site 620708
      • Vila Nova de Gaia, Portugalsko
        • Chiesi Clinical Trial Site 620707
  • Rumunsko
      • Alexandru cel Bun, Rumunsko
        • Chiesi Clinical Trial Site 642715
      • Arad, Rumunsko
        • Chiesi Clinical Trial Site 642713
      • Bacau, Rumunsko
        • Chiesi Clinical Trial Site 642722
      • Bragadiru, Rumunsko
        • Chiesi Clinical Trial Site 642717
      • Brasov, Rumunsko
        • Chiesi Clinical Trial Site 642706
      • Bucharest, Rumunsko
        • Chiesi Clinical Trial Site 642703
      • Bucharest, Rumunsko
        • Chiesi Clinical Trial Site 642707
      • Bucharest, Rumunsko
        • Chiesi Clinical Trial Site 642708
      • Bucharest, Rumunsko
        • Chiesi Clinical Trial Site 642719
      • Bucharest, Rumunsko
        • Chiesi Clinical Trial Site 642723
      • Cluj-Napoca, Rumunsko
        • Chiesi Clinical Trial Site 642709
      • Cluj-Napoca, Rumunsko
        • Chiesi Clinical Trial Site 642714
      • Cluj-Napoca, Rumunsko
        • Chiesi Clinical Trial Site 642716
      • Cluj-Napoca, Rumunsko
        • Chiesi Clinical Trial Site 642718
      • Cluj-Napoca, Rumunsko
        • Chiesi Clinical Trial Site 642726
      • Craiova, Rumunsko
        • Chiesi Clinical Trial Site 642712
      • Iași, Rumunsko
        • Chiesi Clinical Trial Site 642704
      • Iași, Rumunsko
        • Chiesi Clinical Trial Site 642710
      • Oradea, Rumunsko
        • Chiesi Clinical Trial Site 642705
      • Suceava, Rumunsko
        • Chiesi Clinical Trial Site 642711
      • Timișoara, Rumunsko
        • Chiesi Clinical Trial Site 642721
  • Rusko
      • Chelyabinsk, Rusko
        • Chiesi Clinical Trial Site 643727
      • Chelyabinsk, Rusko
        • Chiesi Clinical Trial Site 643733
      • Chelyabinsk, Rusko
        • Chiesi Clinical Trial Site 643745
      • Izhevsk, Rusko
        • Chiesi Clinical Trial Site 643754
      • Kazan', Rusko
        • Chiesi Clinical Trial Site 643713
      • Kazan', Rusko
        • Chiesi Clinical Trial Site 643719
      • Kazan', Rusko
        • Chiesi Clinical Trial Site 643741
      • Kazan', Rusko
        • Chiesi Clinical Trial Site 643746
      • Kemerovo, Rusko
        • Chiesi Clinical Trial Site 643704
      • Kemerovo, Rusko
        • Chiesi Clinical Trial Site 643731
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643702
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643705
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643706
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643718
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643722
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643735
      • Moscow, Rusko
        • Chiesi Clinical Trial Site 643743
      • Nizhny Novgorod, Rusko
        • Chiesi Clinical Trial Site 643707
      • Nizhny Novgorod, Rusko
        • Chiesi Clinical Trial Site 643723
      • Nizhny Novgorod, Rusko
        • Chiesi Clinical Trial Site 643744
      • Novosibirsk, Rusko
        • Chiesi Clinical Trial Site 643717
      • Odintsovo, Rusko
        • Chiesi Clinical Trial Site 643724
      • Orenburg, Rusko
        • Chiesi Clinical Trial Site 643729
      • Pyatigorsk, Rusko
        • Chiesi Clinical Trial Site 643711
      • Ryazan, Rusko
        • Chiesi Clinical Trial Site 643701
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643712
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643714
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643715
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643716
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643725
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643730
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643732
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643737
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643739
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643752
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643757
      • Saint Petersburg, Rusko
        • Chiesi Clinical Trial Site 643758
      • Saratov, Rusko
        • Chiesi Clinical Trial Site 643703
      • Saratov, Rusko
        • Chiesi Clinical Trial Site 643736
      • Smolensk, Rusko
        • Chiesi Clinical Trial Site 643726
      • Stavropol, Rusko
        • Chiesi Clinical Trial Site 643740
      • Tomsk, Rusko
        • Chiesi Clinical Trial Site 643709
      • Tomsk, Rusko
        • Chiesi Clinical Trial Site 643728
      • Tomsk, Rusko
        • Chiesi Clinical Trial Site 643759
      • Ufa, Rusko
        • Chiesi Clinical Trial Site 643755
      • Vladikavkaz, Rusko
        • Chiesi Clinical Trial Site 643708
      • Vladimir, Rusko
        • Chiesi Clinical Trial Site 643738
      • Voronezh, Rusko
        • Chiesi Clinical Trial Site 643710
      • Yaroslavl, Rusko
        • Chiesi Clinical Trial Site 643720
      • Yaroslavl, Rusko
        • Chiesi Clinical Trial Site 643734
      • Yaroslavl, Rusko
        • Chiesi Clinical Trial Site 643742
      • Yaroslavl, Rusko
        • Chiesi Clinical Trial Site 643749
      • Yekaterinburg, Rusko
        • Chiesi Clinical Trial Site 643721
  • Slovensko
      • Bratislava, Slovensko
        • Chiesi Clinical Trial Site 703704
      • Bratislava, Slovensko
        • Chiesi Clinical Trial Site 703707
      • Ilava, Slovensko
        • Chiesi Clinical Trial Site 703702
      • Košice, Slovensko
        • Chiesi Clinical Trial Site 703705
      • Košice, Slovensko
        • Chiesi Clinical Trial Site 703706
      • Nové Zámky, Slovensko
        • Chiesi Clinical Trial Site 703701
      • Prievidza, Slovensko
        • Chiesi Clinical Trial Site 703709
      • Spišská Nová Ves, Slovensko
        • Chiesi Clinical Trial Site 703703
      • Štúrovo, Slovensko
        • Chiesi Clinical Trial Site 703708
  • Spojené království
      • Llanelli, Spojené království
        • Chiesi Clinical Trial Site 826702
      • London, Spojené království
        • Chiesi Clinical Trial Site 826703
      • Manchester, Spojené království
        • Chiesi Clinical Trial Site 826704
      • Soham, Spojené království
        • Chiesi Clinical Trial Site 826701
  • Turecko (Türkiye)
      • Ankara, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792701
      • Ankara, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792702
      • Antalya, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792703
      • Aydin, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792710
      • Istanbul, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792707
      • Kocaeli, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792706
      • Maltepe, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792705
      • Mersin, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792708
      • Yenişehir, Turecko (Türkiye)
        • Chiesi Clinical Trial Site 792709
  • Ukrajina
      • Dnipro, Ukrajina
        • Chiesi Clinical Trial Site 804701
      • Ivano-Frankivsk, Ukrajina
        • Chiesi Clinical Trial Site 804711
      • Kharkiv, Ukrajina
        • Chiesi Clinical Trial Site 804709
      • Kherson, Ukrajina
        • Chiesi Clinical Trial Site 804710
      • Kiev, Ukrajina
        • Chiesi Clinical Trial Site 804713
      • Kyiv, Ukrajina
        • Chiesi Clinical Trial Site 804705
      • Lviv, Ukrajina
        • Chiesi Clinical Trial Site 804712
      • Sumy, Ukrajina
        • Chiesi Clinical Trial Site 804715
      • Vinnytsia, Ukrajina
        • Chiesi Clinical Trial Site 804703
      • Vinnytsia, Ukrajina
        • Chiesi Clinical Trial Site 804706
      • Vinnytsia, Ukrajina
        • Chiesi Clinical Trial Site 804707
      • Vinnytsia, Ukrajina
        • Chiesi Clinical Trial Site 804714
      • Zaporizhzhya, Ukrajina
        • Chiesi Clinical Trial Site 804704
      • Zhytomyr, Ukrajina
        • Chiesi Clinical Trial Site 804708
  • Česko
      • Blansko, Česko
        • Chiesi Clinical Trial Site 203711
      • Brandýs nad Labem, Česko
        • Chiesi Clinical Trial Site 203702
      • Brno, Česko
        • Chiesi Clinical Trial Site 203708
      • Jindřichův Hradec, Česko
        • Chiesi Clinical Trial Site 203707
      • Kralupy nad Vltavou, Česko
        • Chiesi Clinical Trial Site 203705
      • Miroslav, Česko
        • Chiesi Clinical Trial Site 203709
      • Opava, Česko
        • Chiesi Clinical Trial Site 203704
      • Prague, Česko
        • Chiesi Clinical Trial Site 203701
      • Prague, Česko
        • Chiesi Clinical Trial Site 203703
      • Prague, Česko
        • Chiesi Clinical Trial Site 203710
      • Rokycany, Česko
        • Chiesi Clinical Trial Site 203713
      • Teplice, Česko
        • Chiesi Clinical Trial Site 203706
      • Varnsdorf, Česko
        • Chiesi Clinical Trial Site 203712
  • Španělsko
      • A Coruña, Španělsko
        • Chiesi Clinical Trial Site 724702
      • Badajoz, Španělsko
        • Chiesi Clinical Trial Site 724703
      • Badalona, Španělsko
        • Chiesi Clinical Trial Site 724706
      • Madrid, Španělsko
        • Chiesi Clinical Trial Site 724701
      • Madrid, Španělsko
        • Chiesi Clinical Trial Site 724704
      • Málaga, Španělsko
        • Chiesi Clinical Trial Site 724705
      • Sabadell, Španělsko
        • Chiesi Clinical Trial Site 724707

Kritéria účasti

Výzkumníci hledají lidi, kteří odpovídají určitému popisu, kterému se říká kritéria způsobilosti. Některé příklady těchto kritérií jsou celkový zdravotní stav osoby nebo předchozí léčba.

Kritéria způsobilosti

Věk způsobilý ke studiu

18 let až 75 let (Dospělý, Starší dospělý)

Přijímá zdravé dobrovolníky

Ne

Popis

Kritéria pro zařazení:

  • Anamnéza astmatu ≥ 1 rok a diagnostikovaná před 40. rokem věku
  • Nekontrolované astma s dvojitou terapií pouze vysokými dávkami inhalačního kortikosteroidu (ICS) v kombinaci s dlouhodobě působícím beta2 agonistou (LABA) s ACQ-7 (Asthma Control Questionnaire) ≥1,5
  • FEV1 před bronchodilatací < 80 % předpokládané normální hodnoty
  • Pozitivní test reverzibility
  • Alespoň 1 zdokumentovaná exacerbace astmatu v předchozím roce

Kritéria vyloučení:

  • Těhotné nebo kojící ženy
  • Diagnostika chronické obstrukční plicní nemoci (CHOPN)
  • Pacienti s jakoukoli exacerbací astmatu nebo infekcí dýchacích cest během 4 týdnů před screeningem
  • Současný kuřák nebo bývalý kuřák (>= 10 balení za rok)
  • Jakákoli změna v dávce, schématu nebo formulaci kombinace IKS + LABA během 4 týdnů před screeningem

Studijní plán

Tato část poskytuje podrobnosti o studijním plánu, včetně toho, jak je studie navržena a co studie měří.

Jak je studie koncipována?

Detaily designu

  • Primární účel: Léčba
  • Přidělení: Randomizované
  • Intervenční model: Paralelní přiřazení
  • Maskování: Čtyřnásobek

Zbraně a zásahy

Skupina účastníků / Arm
Intervence / Léčba
Experimentální: CHF 5993 200/6/12,5 ug

Léčba A:

5993 CHF 200/6/12.5 µg: 2 inhalace bid Celková denní dávka: 800/24/50 µg BDP/FF/GB
Lék: CHF 5993 200/6/12,5 ug
Aktivní komparátor: CHF 1535 200/6 ug

Léčba B:

CHF 1535 200/6 µg: 2 inhalace bid Celková denní dávka: 800/24 ​​µg BDP/FF
Lék: CHF 1535 200/6 ug
Aktivní komparátor: CHF 1535 200/6 µg + Tiotropium Respimat 2,5 µg

Léčba C (otevřená větev):

CHF 1535 200/6 µg: 2 inhalace bid

+ Tiotropium Respimat 2,5 µg: 2 inhalace od Celková denní dávka: 800/24 ​​µg BDP/FF + 5 µg Tio
Lék: CHF 1535 200/6 µg + Tiotropium Respimat 2,5 µg

Co je měření studie?

Primární výstupní opatření

Měření výsledku
Popis opatření
Časové okno
1_Change From Baseline in Pre-Dose Forced Expiratory Volume in the First Second (FEV1) at Week 26
Časové okno: Week 0 (pre-treatment, baseline) to Week 26.

Change from baseline in pre-dose FEV1, analysed at Week 26 of treatment.

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) to Week 26.
2_Moderate and Severe Asthma Exacerbation Rate Over the 52-Week Treatment Period
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Asthma exacerbation intensity: Moderate AND Severe Asthma Exacerbation

Severe: asthma worsening requiring initiation of treatment with systemic corticosteroids for at least 3 days (courses of corticosteroids separated by ≥1 week treated as separate severe exacerbations).

Moderate: ≥1 of the following criteria fulfilled and leading to a change in treatment (sustained increase of ≥1 puff of short acting beta 2-agonist [SABA] for 2 consecutive days) as shown below:

  • Nocturnal awakening(s) due to asthma requiring SABA for 2 consecutive nights/increase of ≥ 0.75 from baseline in daily symptom score on 2 consecutive days; increase from baseline in occasions of SABA use on 2 consecutive days (minimum increase 4 puffs/day);
  • ≥20% decrease in peak expiratory flow from baseline on at least 2 consecutive mornings/evenings or ≥ 20% decrease in FEV1 from baseline;
  • Visit to the ER/trial site for asthma treatment not requiring systemic corticosteroid;
Week 0 (pre-treatment, baseline) to Week 52.

Sekundární výstupní opatření

Měření výsledku
Popis opatření
Časové okno
3_Change From Baseline in Peak(0-3h) FEV1 at Week 26
Časové okno: Week 0 (pre-treatment, baseline) and Week 26.

Peak peak of forced expiratory volume in the first second (FEV1) within 3 hours post-dose.

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) and Week 26.
4_Change From Baseline in Morning Peak Expiratory Flow (PEF) Over the 26-Week Treatment
Časové okno: Week 0 (pre-treatment, baseline) to Week 26.

Change from baseline in the average morning PEF (Litre/min), measured by patients at home over the 26-week treatment period (i.e., up to Week 26).

PEF=Peak Expiratory Flow; is the maximal airflow forcefully expelled from the lungs in one quick exhalation.
Week 0 (pre-treatment, baseline) to Week 26.
5_Severe Asthma Exacerbation Rate Over the 52-Week Treatment Period - Pooled Analysis
Časové okno: The entire treatment period; up to Week 52.

Severe asthma exacerbation rate over the 52-Week treatment period in a pre-specified pooled analysis of 2 pivotal studies CCD-05993AB1-03 (TRIMARAN) and CCD-05993AB2-02 (TRIGGER).

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
The entire treatment period; up to Week 52.
6_Change From Baseline in Peak FEV1 (0-3h) at All Clinical Visits
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

The peak (0-3h) FEV1 at baseline and at all subsequent visits, and the respective changes from baseline are presented by treatment group for all clinical visits.

Baseline for pre-dose FEV1 was calculated as average of the FEV1 measurements (L) from the visit 2 (V2) Pre45min & V2 Pre15min. If one of the two pre-dose values was missing, the baseline was equal to the available pre-dose value.

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) to Week 52.
7_Change From Baseline in Pre-Dose FEV1 at All Clinical Visits
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Results show the change from baseline in pre-dose FEV1 at all clinical visits.

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) to Week 52.
8_FEV1 Response (FEV1 ≥ 100 mL) at Week 26 and Week 52
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Results show the percentage of patients classified as FEV1 responders at Week 26 and at Week 52.

The FEV1 response was defined as: Change from baseline in pre-dose morning FEV1 ≥ 100 mL.

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
9_Change From Baseline in FEV1 Area Under the Curve (AUC) (0-3h) Normalised by Time at All Clinical Visits
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Baseline definition: mean of two pre-dose FEV1 measurements at visit 2 (V2).

Results show the change from baseline in FEV1 area under the curve [AUC] (0-3h) at all subsequent visits (i.e. change from baseline of the AUC of the serial post-dose spirometry assessments till 3h post-dose).

FEV1=Forced expiratory volume in the first second
Week 0 (pre-treatment, baseline) to Week 52.
10_Change From Baseline in the Asthma Control Questionnaire-7 (ACQ-7) Score at All Clinical Visits
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

ACQ-7 Questionnaire.

ACQ-7 allows assessment of asthma control in individual patients.

The ACQ-7 measured asthma symptom control and consists of 7 items: 5 on symptom assessment, 1 on rescue medication use and 1 on lung function (FEV1 % predicted). All seven items are scored on a 7-point Likert scale, with 0 indicating total control (no impairment) and 6 indicating poor control (maximum impairment). The questions are equally weighted and the total score is the mean of the seven items. The first 6 questions of the ACQ-7 were completed by the participant while the last question was completed by the study investigator using data from the Master Scope spirometer.

Baseline for ACQ-7 was the total score recorded at Visit 2 (Week 0) of the study. The change from Baseline was calculated by subtracting the Baseline values from the individual post-randomization values. A negative change from baseline indicates improvement in lung function.
Week 0 (pre-treatment, baseline) to Week 52.
11_Asthma Control Questionnaire©-7 Response at Week 26 and Week 52
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Asthma Control Questionnaire (ACQ) and Asthma Control Questionnaire-7 (QAC-7) are defined in the description of Outcome measure 10 above.

An ACQ-7 response was defined as change from baseline (Week 0, pre-dose) in ACQ-7 score ≤ -0.5; non-response was defined as change from baseline in ACQ-7 score >-0.5 or missing data.

Results represent responders (i.e. change from baseline in ACQ-7 Score ≤ -0.5) at Week 26 and at Week 52.
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
12_Change From Baseline in Average Morning PEF (L/Min) Over 52 Weeks of Treatment
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Change from baseline in average MORNING PEF (L/min) over 52 weeks of treatment.

PEF=Peak Expiratory Flow; is the maximal airflow forcefully expelled from the lungs in one quick exhalation.
Week 0 (pre-treatment, baseline) to Week 52.
12a_Change From Baseline in Average Evening PEF (L/Min) Over 26 and 52 Weeks of Treatment
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Change from baseline in average EVENING PEF (L/min) over 26 and 52 weeks of treatment.

PEF=Peak Expiratory Flow; is the maximal airflow forcefully expelled from the lungs in one quick exhalation.
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
13_Number of Patients at Risk of Moderate or Severe Asthma Exacerbation Over 52 Weeks
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Number of patients at risk of a moderate or severe asthma exacerbation.

Results show the number of patients who had moderate or severe asthma exacerbation over the 52 weeks treatment period.
Week 0 (pre-treatment, baseline) to Week 52.
14_Number of Patients at Risk of Severe Asthma Exacerbation in the Pooled Analysis of the Two Pivotal Studies CCD-05993AB1-03 and CCD-05993AB2-02
Časové okno: Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.

Number of patients at risk of a SEVERE asthma exacerbation in the pooled analysis of the two pivotal studies CCD-05993AB1-03 (TRIMARAN) and CCD-05993AB2-02 (TRIGGER), over the 52 weeks treatment period.

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.
15_Moderate Asthma Exacerbation Rate Over the 52-Week Treatment Period in the Pooled Analysis of the 2 Pivotal Studies CCD-05993AB1-03 and CCD-055993AB2-02.
Časové okno: Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.

MODERATE asthma exacerbation rate over the 52-Week treatment period in the pooled analysis of the 2 pivotal studies CCD-05993AB1-03 (TRIMARAN) and CCD-055993AB2-02 (TRIGGER).

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.
16_Number of Patients at Risk of MODERATE Asthma Exacerbation in the Pooled Analysis of the Two Pivotal Studies CCD-05993AB1-03 and CCD-05993AB2-02
Časové okno: Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.

Number of Patients at Risk of MODERATE Asthma Exacerbation in the Pooled Analysis of the Two Pivotal Studies CCD-05993AB1-03 and CCD-05993AB2-02.

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.
17_Moderate and Severe Asthma Exacerbation Rate Over the 52-Week Treatment Period in the Pooled Analysis of the 2 Pivotal Studies CCD-05993AB1-03 and CCD-055993AB2-02
Časové okno: Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.

Moderate AND severe asthma exacerbation rate over the 52-Week treatment period in the pooled analysis of the 2 pivotal studies CCD-05993AB1-03 (TRIMARAN) and CCD-05993AB2-02 (TRIGGER).

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.
18_Number of Patients at Risk of Moderate OR Severe Asthma Exacerbation in the Pooled Analysis of the Two Pivotal Studies CCD-05993AB1-03 and CCD-05993AB2-02
Časové okno: Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.

Time to first MODERATE OR SEVERE asthma exacerbation in the Pooled Analysis of the 2 Pivotal Studies CCD-05993AB1-03 (TRIMARAN) and CCD-05993AB2-02 (TRIGGER).

The pooled analysis of pivotal studies TRIMARAN and TRIGGER was a pre-specified secondary outcome measure for this study. Both studies have identical design, duration, endpoints, data collection, and statistical methodology for analyses. TRIMARAN and TRIGGER enrolled patients under medium dose and high dose ICS/LABA, respectively. Both studies were designed to assess the effect of the LAMA on ICS/LABA and showed homogeneity in terms of baseline characteristics, thus confirming the appropriateness of the pooling.
Week 0 (Baseline) to 52 weeks for both studies in the pooled analysis.
19_Moderate Asthma Exacerbation Rate Over the 52-Week Treatment Period
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

MODERATE asthma exacerbation rate over the 52-Week treatment period.

Asthma exacerbation intensity: Moderate: ≥1 of the following criteria fulfilled and leading to a change in treatment (sustained increase of ≥1 puff of short acting beta 2-agonist [SABA] for 2 consecutive days) as shown below:

  • Nocturnal awakening(s) due to asthma requiring SABA for 2 consecutive nights/increase of ≥ 0.75 from baseline in daily symptom score on 2 consecutive days; increase from baseline in occasions of SABA use on 2 consecutive days (minimum increase 4 puffs/day);
  • ≥20% decrease in peak expiratory flow from baseline on at least 2 consecutive mornings/evenings or ≥ 20% decrease in FEV1 from baseline;
  • Visit to the ER/trial site for asthma treatment not requiring systemic corticosteroid;
Week 0 (pre-treatment, baseline) to Week 52.
20_Number of Patients at Risk of a MODERATE Asthma Exacerbation
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.
Data were analysed for the number of patients at risk of a MODERATE asthma exacerbation.
Week 0 (pre-treatment, baseline) to Week 52.
21_Change From Baseline in the Average Use of Rescue Medication Over the 26- and 52-Week Treatment Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Change from baseline in the average use of rescue medication over the 26- and 52-Week treatment periods.

Data was collected through an electronic daily diary from screening to the end of the study.
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
21a_Change From Baseline in the Average Use of Rescue Medication in Each Inter-Visit Period
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Results show the change from baseline in the average use (puffs/day) of rescue medication in each inter-visit period.

Data was collected through an electronic daily diary from screening to the end of the study.
Week 0 (pre-treatment, baseline) to Week 52.
22_Change From Baseline in the Percentage of Rescue Medication-Free Days Over the 26- and 52-Week Treatment Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Change from baseline in the percentage of rescue medication-free days over the 26- and 52-Week treatment periods.

Data was collected using an electronic daily diary, from screening to the end of the study.
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
22a_Change From Baseline in the Percentage of Rescue Medication-Free Days in Each Inter-Visit Period Over the Treatment
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Results show the change from baseline in the percentage of rescue medication-free days in each inter-visit period over the entire treatment.

Data was collected through an electronic daily diary from screening to the end of the study.
Week 0 (pre-treatment, baseline) to Week 52.
23_Change From Baseline in the Average Total Daily Asthma Symptom Scores Over the 26- and 52-Week Treatment Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Results show the change from baseline in the average total daily asthma symptom scores over the 26- and 52-Weeks of treatment. A day represents data recorded in the evening session of that day plus the data recorded in the morning session of the next day.

Symptoms considered: cough, wheeze, chest tightness, breathlessness.

Morning (night-time asthma symptom score):

  • 0 No symptoms;
  • 1 Mild = Symptoms not causing awakening;
  • 2 Moderate = Discomfort enough to cause awakenings;
  • 3 Severe = Causing awakenings for most of the night/did not sleep at all.

Evening (daytime asthma symptom score):

  • 0 No symptoms;
  • 1 Mild = Aware of symptoms, which could be easily tolerated;
  • 2 Moderate = Discomfort enough to cause interference with daily activity;
  • 3 Severe = Incapacitating
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
23a_Change From Baseline in the Average Daily Asthma Symptom Scores in Each Inter-Visit Period
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Results show the change from baseline in the average total daily asthma symptom scores over the 26- and 52-Weeks of treatment. A day represents data recorded in the evening session of that day plus the data recorded in the morning session of the next day.

Symptoms considered: cough, wheeze, chest tightness, breathlessness.

Morning (night-time asthma symptom score):

  • 0 No symptoms;
  • 1 Mild = Symptoms not causing awakening;
  • 2 Moderate = Discomfort enough to cause awakenings;
  • 3 Severe = Causing awakenings for most of the night/did not sleep at all.

Evening (daytime asthma symptom score):

  • 0 No symptoms;
  • 1 Mild = Aware of symptoms, which could be easily tolerated;
  • 2 Moderate = Discomfort enough to cause interference with daily activity;
  • 3 Severe = Incapacitating
Week 0 (pre-treatment, baseline) to Week 52.
24_Change From Baseline in the Percentage of Asthma Symptom-Free Days Over the 26- and 52-Week Treatment Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Change from baseline in the percentage of asthma symptom-free days over the 26- and 52-Week treatment periods.

Data was collected through an electronic daily diary from screening to the end of the study.

Results show the change from baseline in the average daily asthma symptom scores over the 26- and 52-Week treatment periods. A day represents data recorded in the evening session of that day plus the data recorded in the morning session of the next day.

Symptoms considered by the questionnaire: cough, wheeze, chest tightness, breathlessness.

An asthma symptom-free day is a day with total daily asthma symptom score = 0. For a description of the score see outcome measure number 23.
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
24a_Change From Baseline in the Percentage of Asthma Symptom-Free Days in Each Inter-Visit Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

Results show the change from baseline in the percentage of asthma symptom-free days in each inter-visit periods over the entire treatment.

Data was collected through an electronic daily diary from screening to end of the study.

A day represents data recorded in the evening session of that day plus the data recorded in the morning session of the next day.

Symptoms considered by the questionnaire: cough, wheeze, chest tightness, breathlessness.

An asthma symptom-free day is a day with total daily asthma symptom score = 0. For a description of the score see outcome measure number 23.
Week 0 (pre-treatment, baseline) to Week 52.
25_Change From Baseline in the Percentage of Asthma Control Days Over the 26- and 52-Week Treatment Periods
Časové okno: Week 0 (pre-treatment, baseline) to Week 26 and Week 52.

Results show the change from baseline in the percentage of asthma control days over the 26- and 52-Week treatment periods.

Data was collected through an electronic daily diary from screening to the end of the study.

Scoring of asthma symptoms (overall symptoms, cough, wheeze, chest tightness and breathlessness):

Morning (night-time asthma symptoms): 0 (no symptoms), 1 (mild - symptoms not causing awakening), 2 (moderate - discomfort enough to cause awakenings) and 3 (severe - causing awakenings for most of the night/did not sleep at all).

Evening (daytime asthma symptoms): 0 (no symptoms), 1 (mild: aware of symptoms that could be easily tolerated), 2 (moderate: discomfort enough to cause interference with daily activity), 3 (severe: incapacitating with inability to work/take part in usual activity).
Week 0 (pre-treatment, baseline) to Week 26 and Week 52.
25a_Change From Baseline in the Percentage of Asthma Control Days in Each Inter-Visit Period
Časové okno: Week 0 (pre-treatment, baseline) to Week 52.

A day represents data recorded in the evening session of that day plus the data recorded in the morning session of the next day.

Data was collected through an electronic daily diary from screening to the end of the study.

Scoring of asthma symptoms (overall symptoms, cough, wheeze, chest tightness and breathlessness):

Morning (night-time asthma symptoms): 0 (no symptoms), 1 (mild - symptoms not causing awakening), 2 (moderate - discomfort enough to cause awakenings) and 3 (severe - causing awakenings for most of the night/did not sleep at all).

Evening (daytime asthma symptoms): 0 (no symptoms), 1 (mild: aware of symptoms that could be easily tolerated), 2 (moderate: discomfort enough to cause interference with daily activity), 3 (severe: incapacitating with inability to work/ take part in usual activity).
Week 0 (pre-treatment, baseline) to Week 52.

Další výstupní opatření

Měření výsledku
Popis opatření
Časové okno
Nežádoucí účinky a nežádoucí reakce na léky
Časové okno: Až do 52. týdne
Až do 52. týdne
Sborník výstupů Health Economics
Časové okno: Týden 0 až 52
Úplné využití zdrojů zdravotní péče a nepřítomnost v práci
Týden 0 až 52

Spolupracovníci a vyšetřovatelé

Zde najdete lidi a organizace zapojené do této studie.

Sponzor

Chiesi Farmaceutici S.p.A.

Vyšetřovatelé

  • Vrchní vyšetřovatel: Georgio Walter Canonica, MD, University of Medicine, Genoa, Italy

Publikace a užitečné odkazy

Osoba odpovědná za zadávání informací o studiu tyto publikace poskytuje dobrovolně. Mohou se týkat čehokoli, co souvisí se studiem.

Obecné publikace

Užitečné odkazy

Termíny studijních záznamů

Tato data sledují průběh záznamů studie a předkládání souhrnných výsledků na ClinicalTrials.gov. Záznamy ze studií a hlášené výsledky jsou před zveřejněním na veřejné webové stránce přezkoumány Národní lékařskou knihovnou (NLM), aby se ujistily, že splňují specifické standardy kontroly kvality.

Hlavní termíny studia

Začátek studia (Aktuální)

6. dubna 2016

Primární dokončení (Aktuální)

28. května 2018

Dokončení studie (Aktuální)

28. května 2018

Termíny zápisu do studia

První předloženo

3. února 2016

První předloženo, které splnilo kritéria kontroly kvality

3. února 2016

První zveřejněno (Odhadovaný)

8. února 2016

Aktualizace studijních záznamů

Poslední zveřejněná aktualizace (Aktuální)

29. května 2026

Odeslaná poslední aktualizace, která splnila kritéria kontroly kvality

4. května 2026

Naposledy ověřeno

1. května 2026

Více informací

Termíny související s touto studií

Klíčová slova

Další relevantní podmínky MeSH

Další identifikační čísla studie

  • CCD-05993AB2-02
  • 2015-000717-40 (Číslo EudraCT)

Plán pro data jednotlivých účastníků (IPD)

Plánujete sdílet data jednotlivých účastníků (IPD)?

ANO

Popis plánu IPD

Chiesi se zavazuje sdílet s kvalifikovanými vědeckými a lékařskými výzkumníky, provádět legitimní výzkum, údaje na úrovni pacienta, údaje na úrovni studie, klinický protokol a úplné CSR, poskytovat přístup k informacím z klinických studií v souladu se zásadou ochrany komerčně důvěrných informací a informací o pacientovi Soukromí. Jakákoli sdílená data na úrovni pacienta jsou anonymizována, aby byly chráněny osobní údaje.

Přístupová kritéria Chiesi a kompletní proces sdílení klinických dat jsou k dispozici na webových stránkách Chiesi Group.

Časový rámec sdílení IPD

See information above in Plan Description regarding Chiesi's commitment to share information with qualified scientific and medical researchers, conducting legitimate research

Chiesi access criteria and complete process for clinical data sharing is available on the Chiesi Group website.

Kritéria přístupu pro sdílení IPD

Přístupová kritéria Chiesi a kompletní proces sdílení klinických dat jsou k dispozici na webových stránkách Chiesi Group.

Tyto informace byly beze změn načteny přímo z webu clinicaltrials.gov. Máte-li jakékoli požadavky na změnu, odstranění nebo aktualizaci podrobností studie, kontaktujte prosím register@clinicaltrials.gov. Jakmile bude změna implementována na clinicaltrials.gov, bude automaticky aktualizována i na našem webu .

Klinické studie na CHF 5993 200/6/12,5 ug

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