REIMAGINE 1: A research study to see how much CagriSema lowers blood sugar and body weight compared to placebo in people with type 2 diabetes treated with diet and exercise

2022-502677-42-00 Protocol NN9388-4895 Therapeutic confirmatory (Phase III) Ended

Start 24 Jul 2024 · End 22 Dec 2025 · Status Ended · 3 EU/EEA countries · 15 sites · Protocol NN9388-4895

Overview

Sponsor-declared trial summary

Phase Therapeutic confirmatory (Phase III)
Status Ended
Participants planned 180
Countries 3
Sites 15

Type 2 diabetes

To confirm superiority of CagriSema (00 mg/00 mg and 00 mg/00 mg) versus placebo on change in HbA1c in participants with T2D in inadequate glycaemic control on diet and exercise

Key facts

Sponsor
Novo Nordisk A/S
Participant type
Patients
Age range
18-64 years, 65+ years
Gender
Male and Female
Therapeutic area
Diseases [C] - Nutritional and Metabolic Diseases [C18]
Trial duration
24 Jul 2024 → 22 Dec 2025
Decision date (initial)
2024-04-11
Transition trial
No
Low-intervention
No
Rare-disease indication
No
Vulnerable population
Yes
Funding sources
Novo Nordisk A/S

External identifiers

EU CT number
2022-502677-42-00
WHO UTN
U1111-1283-0404

Trial design

CTIS Part I — objectives, methods, condition coding

Main objective

Scope: Efficacy, Safety

To confirm superiority of CagriSema (00 mg/00 mg and 00 mg/00 mg) versus placebo on change in HbA1c in participants with T2D in inadequate glycaemic control on diet and exercise

Secondary objectives 3

  1. To confirm superiority of CagriSema (00 mg/00 mg and 00 mg/00 mg) versus placebo on: Change in body weight, Achievement of ≥ 10% weight reduction, Achievement of ≥ 15% weight reduction, Other parameters of glycaemic control
  2. To compare the effect of CagriSema (00 mg/00 mg and 00 mg/00 mg) versus placebo on: Achievement of ≥ 5% weight reduction, Achievement of ≥ 20% weight reduction, Waist circumference, Blood pressure, Inflammation, Lipids, Achievement of T2D remission, Beta-cell function, Clinical outcome assessments, Leptin and soluble leptin receptor
  3. To compare the safety and tolerability of CagriSema (00 mg/00 mg and 00 mg/00 mg) versus placebo

Conditions and MedDRA coding

Type 2 diabetes

VersionLevelCodeTermSystem organ class
21.1 LLT 10045242 Type II diabetes mellitus 10027433

Regulatory references

Scientific advice from competent authorities
European Medicines Agency
Plan to share IPD
No

Eligibility criteria

Principal inclusion / exclusion criteria as submitted by sponsor

Inclusion criteria 5

  1. Male or female.
  2. Age 18 years or above at the time of signing the informed consent.
  3. Diagnosed with type 2 diabetes ≥ 30 days before screening.
  4. HbA1c 7.0-9.5% (53-80 mmol/mol) (both inclusive) as determined by central laboratory at screening.
  5. BMI ≥ 23 kg/m2 at screening. BMI will be calculated in the eCRF based on height and body weight at screening.

Exclusion criteria 5

  1. Female who is pregnant, breast-feeding or intends to become pregnant or is of childbearing potential and not using a highly effective contraceptive method.
  2. Renal impairment with estimated Glomerular Filtration Rate < 30 ml/min/1.73 m2 as determined by central laboratory at screening.
  3. Treatment with any medication for the indication of diabetes (ever) or obesity (within 90 days before screening). However, short term insulin treatment for a maximum of 14 consecutive days and prior insulin treatment for gestational diabetes are allowed.
  4. History of use of any injectable therapy for diabetes or obesity. However, short term insulin treatment for a maximum of 14 consecutive days and prior insulin treatment for gestational diabetes are allowed.
  5. Uncontrolled and potentially unstable diabetic retinopathy or maculopathy. Verified by a eye examination performed within 90 days before screening or in the period between screening and randomisation. Pharmacological pupil-dilation is a requirement unless using a digital fundus photography camera specified for non-dilated examination.

Endpoints

Primary and secondary outcome measures (English text)

Primary endpoints 1

  1. Change in HbA1c from baseline (week 0) to end of treatment (week 40)

Secondary endpoints 23

  1. Relative change in body weight from baseline (week 0) to end of treatment (week 40)
  2. Achievement of ≥ 10 % weight reduction from baseline (week 0) to end of treatment (week 40)
  3. Achievement of ≥ 15 % weight reduction from baseline (week 0) to end of treatment (week 40)
  4. Achievement of HbA1c target values of <7.0% (<53 mmol/mol) at end of treatment (week 40)
  5. Achievement of HbA1c target values of ≤6.5% (≤48 mmol/mol) at end of treatment (week 40)
  6. Change in Fasting Plasma Glucose (FPG) from baseline (week 0) to end of treatment (week 40)
  7. Achievement of ≥ 5% weight reduction from baseline (week 0) to end of treatment (week 40)
  8. Achievement of ≥ 20% weight reduction from baseline (week 0) to end of treatment (week 40)
  9. Change in waist circumference from baseline (week 0) to end of treatment (week 40)
  10. Change in systolic blood pressure (SBP) from baseline (week 0) to end of treatment (week 40)
  11. Change in diastolic blood pressure (DBP) from baseline (week 0) to end of treatment (week 40)
  12. Ratio to baseline in high sensitivity C-reactive protein (hsCRP) from baseline (week 0) to end of treatment (week 40)
  13. Ratio to baseline in lipids: Total cholesterol, High-density lipoprotein (HDL) cholesterol, Low-density lipoprotein (LDL) cholesterol, Very low-density lipoprotein (VLDL) cholesterol, Triglycerides, Free fatty acids, Non-HDL cholesterol from baseline (week 0) to end of treatment (week 40)
  14. Achievement of T2D remission (HbA1c<6.5% and no antidiabetic medication) at end of study (end of treatment + 12 weeks)
  15. Ratio to baseline in OGTT based oral glucose disposition index (DIo) from baseline (week 0) to end of treatment (week 40)
  16. Change in experienced level of energy, as measured by the SF-36v2 Vitality score from baseline (week 0) to end of treatment (week 40)
  17. Change in SF-36v2 score: Physical Component Summary score, Mental Component Summary score from baseline (week 0) to end of treatment (week 40)
  18. Change in Diabetes Treatment Satisfaction Questionnaire (DTSQ) score from baseline (week 0) to end of treatment (week 40)
  19. Change in leptin from baseline (week 0) to end of treatment (week 40)
  20. Change in soluble leptin receptor from baseline (week 0) to end of treatment (week 40)
  21. Number of Treatment Emergent Adverse Events (TEAEs) from baseline (week 0) to end of treatment + 7 weeks
  22. Number of clinically significant hypoglycaemic episodes (level 2) (<3.0 mmol/L (54 mg/dL), confirmed by BG meter) from baseline (week 0) to end of treatment + 7 weeks
  23. Number of severe hypoglycaemic episodes (level 3): hypoglycaemia associated with severe cognitive impairment requiring external assistance for recovery, with no specific glucose threshold from baseline (week 0) to end of treatment + 7 weeks

Investigational products

Investigational medicinal products (IMPs), comparators, placebo, auxiliary

Test 5

cagrilintide semaglutide

PRD8977528 · Product

Active substance
Cagrilintide
Substance synonyms
NNC0174-0833, NN9838, N-alfa-[(S)-4-Carboxy-4-(19-carboxynonadecanoylamino)butyryl]-[Glu14,Arg17,Pro25,Pro28,Pro29,Pro37]-human amylin
Pharmaceutical form
SOLUTION FOR INJECTION
Route of administration
SUBCUTANEOUS
Max daily dose
0 mg milligram(s)
Max total dose
0 mg milligram(s)
Max treatment duration
4 Week(s)
Authorisation status
Not Authorised
MA holder
NOVO NORDISK A/S
Paediatric formulation
No
Orphan designation
No

cagrilintide semaglutide

PRD8977529 · Product

Active substance
Cagrilintide
Substance synonyms
NNC0174-0833, NN9838, N-alfa-[(S)-4-Carboxy-4-(19-carboxynonadecanoylamino)butyryl]-[Glu14,Arg17,Pro25,Pro28,Pro29,Pro37]-human amylin
Pharmaceutical form
SOLUTION FOR INJECTION
Route of administration
SUBCUTANEOUS
Max daily dose
0 mg milligram(s)
Max total dose
0 mg milligram(s)
Max treatment duration
32 Week(s)
Authorisation status
Not Authorised
MA holder
NOVO NORDISK A/S
Paediatric formulation
No
Orphan designation
No

cagrilintide semaglutide

PRD8977527 · Product

Active substance
Cagrilintide
Substance synonyms
NNC0174-0833, NN9838, N-alfa-[(S)-4-Carboxy-4-(19-carboxynonadecanoylamino)butyryl]-[Glu14,Arg17,Pro25,Pro28,Pro29,Pro37]-human amylin
Pharmaceutical form
SOLUTION FOR INJECTION
Route of administration
SUBCUTANEOUS
Max daily dose
0 mg milligram(s)
Max total dose
0 mg milligram(s)
Max treatment duration
4 Week(s)
Authorisation status
Not Authorised
MA holder
NOVO NORDISK A/S
Paediatric formulation
No
Orphan designation
No

cagrilintide semaglutide

PRD8977531 · Product

Active substance
Cagrilintide
Substance synonyms
NNC0174-0833, NN9838, N-alfa-[(S)-4-Carboxy-4-(19-carboxynonadecanoylamino)butyryl]-[Glu14,Arg17,Pro25,Pro28,Pro29,Pro37]-human amylin
Pharmaceutical form
SOLUTION FOR INJECTION
Route of administration
SUBCUTANEOUS
Max daily dose
0 mg milligram(s)
Max total dose
0 mg milligram(s)
Max treatment duration
24 Week(s)
Authorisation status
Not Authorised
MA holder
NOVO NORDISK A/S
Paediatric formulation
No
Orphan designation
No

cagrilintide semaglutide

PRD8977530 · Product

Active substance
Cagrilintide
Substance synonyms
NNC0174-0833, NN9838, N-alfa-[(S)-4-Carboxy-4-(19-carboxynonadecanoylamino)butyryl]-[Glu14,Arg17,Pro25,Pro28,Pro29,Pro37]-human amylin
Pharmaceutical form
SOLUTION FOR INJECTION
Route of administration
SUBCUTANEOUS
Max daily dose
0 mg milligram(s)
Max total dose
0 mg milligram(s)
Max treatment duration
4 Week(s)
Authorisation status
Not Authorised
MA holder
NOVO NORDISK A/S
Paediatric formulation
No
Orphan designation
No

Placebo 1

Placebo + Placebo

N/A · Product

Other product name
N/A
Pharmaceutical form
N/A
ATC code
N/A — N/A
Marketing authorisation
N/A
MA holder
N/A
MA country
Iceland
Paediatric formulation
No

Sponsors and contacts

Sponsor organisations, regulatory contacts, third parties

Novo Nordisk A/S

107 Total trials 29 Recruiting 72 Ended
Commercial
Sponsor organisation
Novo Nordisk A/S
Address
Novo Alle 1
City
Bagsvaerd
Postcode
2880
Country
Denmark

Scientific contact point

Organisation
Novo Nordisk A/S
Contact name
EU Submission Hub

Public contact point

Organisation
Novo Nordisk A/S
Contact name
EU Submission Hub

Third parties 11

OrganisationCity, countryDuties
Eresearchtechnology Inc.
ORG-100013039
 Philadelphia, United States Other
Oracle America Inc.
ORG-100039874
 Redwood City, United States Other
Antaros Medical AB
ORG-100039055
 Molndal, Sweden Other
SYRINX Bioanalytics Oy
ORG-100021026
 Turku, Finland Laboratory analysis
Celerion Inc.
ORG-100029202
 Lincoln, United States Laboratory analysis
Abbott GmbH
ORG-100000219
 Wiesbaden, Germany Other
Accellacare Limited
ORG-100044508
 Dublin 18, Ireland Other
Icon Clinical Research Limited
ORG-100008322
 Dublin 18, Ireland Other
Andrea Mari
ORL-000013382
 Padova, Italy Laboratory analysis
Icon Clinical Research Limited
ORG-100008322
 Dublin 18, Ireland Laboratory analysis
4G Clinical B.V.
ORG-100044721
 Amsterdam, Netherlands Other

Locations

3 EU/EEA countries · 15 investigational sites

By country

CountryMS statusPlanned subjectsSites
Hungary Ended 25 4
Italy Ended 10 4
Poland Ended 25 7
Rest of world
Serbia, China, United States
 120

Investigational sites

Hungary

4 sites · Ended
PVN Kutato Kft.
N/A, Halom Utca 10, 1102, Budapest X
Borbanya Praxis Egeszsegugyi Kft.
NA, Bazsalikom Utca 1/1, Borbanya, Nyiregyhaza
Szent Margit Rendelointezet Nonprofit Kft.
N/A, Vorosvari Ut 88-96/III, III Kerulet, Budapest III
Belinus Bt.
NA, Erzsebet Utca 11-13, 4025, Debrecen

Italy

4 sites · Ended
Ospedale San Raffaele S.r.l.
NA, Via Olgettina 60, 20132, Milan
Azienda Ospedaliero-Universitaria Policlinico Umberto I
NA, Viale Del Policlinico 155, 00161, Rome
Azienda Ospedaliera Universitaria Mater Domini
NA, Viale Tommaso Campanella 115, 88100, Catanzaro
Azienda Ospedaliera Papa Giovanni XXIII
NA, Piazza Oms 1, 24127, Bergamo

Poland

7 sites · Ended
Renew Clinic Sp. z o.o.
NA, Ul Gen Gustawa Orlicz Dreszera 1/8, 15-797, Bialystok
Velocity Nova Sp. z o.o.
N/A, Ul. Peowiakow 1, 22-400, Zamosc
Osteo-Medic s.c. A. Racewicz, J. Supronik
N/A, ul Wiejska 81, 15-351, Bialystok
Centrum Medyczne Medyk Sp. z o.o.
NA, Ul. Fryderyka Szopena 1, 35-055, Rzeszow
Panstwowy Instytut Medyczny Ministerstwa Spraw Wewnetrznych I Administracji
N/A, Ul. Woloska 137, 02-507, Warsaw
NBR Polska Tomasz Klodawski
NA, Aleja Witosa 31, 00-710, Warsaw
Centrum Terapii Wspolczesnej J.M. Jasnorzewska S.K.A.
NA, Ul. Przedzalniana 66, 90-338, Lodz

Country notifications

Trial-start, recruitment-start, end and early-termination notifications submitted per Member State

Country Trial startTrial end Recruitment startRecruitment end Early termination
Hungary 2024-08-02 2025-12-16 2024-09-10 2024-12-19
Italy 2024-08-28 2025-12-11 2024-09-13 2024-12-19
Poland 2024-07-24 2025-12-18 2024-07-24 2024-12-27

Results and documents

Annex IV summary of results, Annex V layperson summary, and all documents registered in CTIS for this trial

Documents 40 files

Public protocol annexes, IB summaries, regulatory submissions and post-authorisation documents registered in CTIS.

TypeTitleVersion
Protocol (for publication) d1_nn9388-4895-protocol-2022-502677-42-english_for-publication 6
Protocol (for publication) D4_NN9388-4895_Subject Diary-Low blood sugar episode-EN-master version-for publication 1.0
Protocol (for publication) D4_NN9388-4895_Subject Diary-Low blood sugar episode-HU-for publication 1.0
Protocol (for publication) D4_NN9388-4895_Subject Diary-Low blood sugar episode-IT-for publication 1.0
Protocol (for publication) d4_nn9388-4895-patient-facing-material-with-copyright-english_for-publication 1
Recruitment arrangements (for publication) K1_HU NN9388-4895 SI-IC recruitment and Informed consent procedure_For Publication 1
Recruitment arrangements (for publication) K1_IT_NN9388-4895 Recruitment and Informed consent_For publication 1
Recruitment arrangements (for publication) K1_PL NN9388-4895 Recruitment and Informed consent_For publication 1.0
Recruitment arrangements (for publication) K2_HU NN9388-4895 Advertisement Poster_For Publication 2
Recruitment arrangements (for publication) K2_IT_NN9388-4895 Recruitment material Advertisement Call Guide_For publication 2.0
Recruitment arrangements (for publication) K2_IT_NN9388-4895 Recruitment material Advertisement Digital Recruitment Campaign_For publication 1
Recruitment arrangements (for publication) K2_IT_NN9388-4895 Recruitment material Advertisement recruitment Poster_For Publication 1
Recruitment arrangements (for publication) K2_IT_NN9388-4895 Recruitment material Advertisement Social Media Content Assets_For publication 2.0
Recruitment arrangements (for publication) k2_it_nn9388-4895-recruitment-material-reimagine1-website-flow_for-publication 2
Recruitment arrangements (for publication) K2_PL NN9388-4895 Advertisement recruitment Poster_For Publication 1
Subject information and informed consent form (for publication) L1_HU NN9388-4895 SI-IC Future Research_For publication 3.0
Subject information and informed consent form (for publication) L1_HU NN9388-4895 SI-IC Male Partner_For publication 2
Subject information and informed consent form (for publication) l1_hu-nn9388-4895-piic-additional-_for-publication 3
Subject information and informed consent form (for publication) l1_hu-nn9388-4895-piic-additional-for-healthy-volunteers-_for-publication 3
Subject information and informed consent form (for publication) l1_hu-nn9388-4895-piic-adult-_for-publication 5
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Future Research_For publication 1
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Male partner_For publication 1
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Privacy Adult_For publication 2.0
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Privacy Future Research_For publication 1
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Privacy Male partner_For publication 1
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Privacy MRI healthy volunteer_For publication 1
Subject information and informed consent form (for publication) L1_IT_NN9388-4895 SI-IC Privacy MRI_For publication 1
Subject information and informed consent form (for publication) l1_it-nn9388-4895-piic-additional-_for-publication 2
Subject information and informed consent form (for publication) l1_it-nn9388-4895-piic-additional-for-healthy-volunteers-_for-publication 2
Subject information and informed consent form (for publication) l1_it-nn9388-4895-piic-adult-_for-publication 3
Subject information and informed consent form (for publication) L1_PL NN9388-4895 SI-IC future research_For publication 2.0
Subject information and informed consent form (for publication) L1_PL NN9388-4895 SI-IC male partner_For publication 2.0
Subject information and informed consent form (for publication) l1_pl-nn9388-4895-piic-additional-_for-publication 3
Subject information and informed consent form (for publication) l1_pl-nn9388-4895-piic-additional-for-healthy-volunteers-_for-publication 3
Subject information and informed consent form (for publication) l1_pl-nn9388-4895-piic-main-_for-publication 4
Subject information and informed consent form (for publication) L2_HU NN9388-4895- Patient Card- For publication 2
Synopsis of the protocol (for publication) d1_hu_nn9388-4895-protocol-synopsis-2022-502677-42-hungarian-_for-publication 1
Synopsis of the protocol (for publication) d1_it_nn9388-4895-protocol-synopsis-2022-502677-42-italian-_for-publication 1
Synopsis of the protocol (for publication) d1_nn9388-4895-protocol-synopsis-2022-502677-42-english_for-publication 1
Synopsis of the protocol (for publication) d1_pl_nn9388-4895-protocol-synopsis-2022-502677-42-polish-_for-publication 1

Application history

9 submissions — initial application plus substantial / non-substantial modifications

#TypeCodeSubmittedReference MSConclusionDecision date
1 INITIAL IN 2023-11-30 Poland Acceptable with conditions
2024-04-09
 2024-04-10
2 SUBSTANTIAL MODIFICATION SM-1 2024-04-29 Poland Acceptable
2024-07-03
 2024-07-05
3 SUBSTANTIAL MODIFICATION SM-2 2024-07-23 Poland Acceptable 2024-09-16
4 SUBSTANTIAL MODIFICATION SM-3 2024-07-23 Acceptable 2024-09-09
5 NON SUBSTANTIAL MODIFICATION NSM-1 2024-09-17 Acceptable 2024-09-17
6 SUBSTANTIAL MODIFICATION SM-4 2024-09-30 Poland Acceptable
2024-11-19
 2024-11-19
7 SUBSTANTIAL MODIFICATION SM-5 2025-02-13 Poland Acceptable
2025-03-31
 2025-04-04
8 SUBSTANTIAL MODIFICATION SM-6 2025-08-18 Poland Acceptable
2025-10-06
 2025-10-10
9 NON SUBSTANTIAL MODIFICATION NSM-2 2026-01-28 Poland Acceptable
2025-10-06
 2026-01-28

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