Patient info Open main menu

Trulicity - summary of medicine characteristics

Contains active substance:

Dostupné balení:

Summary of medicine characteristics - Trulicity

NAME OF THE MEDICINAL PRODUCT

Trulicity 0.75 mg solution for injection in pre-filled pen

Trulicity 1.5 mg solution for injection in pre-filled pen

Trulicity 3 mg solution for injection in pre-filled pen

Trulicity 4.5 mg solution for injection in pre-filled pen

2. QUALITATIVE AND QUANTITATIVE COMPOSITION

Trulicity 0.75 mg solution for injection in pre-filled pen

Each pre-filled pen contains 0.75 mg of dulaglutide* in 0.5 ml solution.

Trulicity 1.5 mg solution for injection in pre-filled pen

Each pre-filled pen contains 1.5 mg of dulaglutide* in 0.5 ml solution.

Trulicity 3 mg solution for injection in pre-filled pen

Each pre-filled pen contains 3 mg of dulaglutide* in 0.5 ml solution.

Trulicity 4.5 mg solution for injection in pre-filled pen

Each pre-filled pen contains 4.5 mg of dulaglutide* in 0.5 ml solution.

  • *produced in CHO cells by recombinant DNA technology.

For the full list of excipients, see section 6.1.

3. PHARMACEUTICAL FORM

Solution for injection.

Clear, colourless solution.

4. CLINICAL PARTICULARS4.1 Therapeutic indications

Type 2 Diabetes Mellitus

Trulicity is indicated for the treatment of adults with insufficiently controlled type 2 diabetes mellitus as an adjunct to diet and exercise

  • • as monotherapy when metformin is considered inappropriate due to intolerance or contraindications
  • • in addition to other medicinal products for the treatment of diabetes.

For study results with respect to combinations, effects on glycaemic control and cardiovascular events, and the populations studied, see sections 4.4, 4.5 and 5.1.

4.2 Posology and method of administration

Posology

Monotherapy

The recommended dose is 0.75 mg once weekly.

Add-on therapy

The recommended dose is 1.5 mg once weekly.

For potentially vulnerable populations 0.75 mg once weekly can be considered as a starting dose.

For additional glycaemic control,

  • • the 1.5 mg dose may be increased after at least 4 weeks to 3 mg once weekly.
  • • the 3 mg dose may be increased after at least 4 weeks to 4.5 mg once weekly.

The maximum dose is 4.5 mg once weekly.

When Trulicity is added to existing metformin and/or pioglitazone therapy, the current dose of metformin and/or pioglitazone can be continued. When Trulicity is added to existing metformin and/or sodium-glucose co-transporter 2 inhibitor (SGLT2i) therapy, the current dose of metformin and/or SGLT2i can be continued. When it is added to existing therapy of a sulphonylurea or insulin, a reduction in the dose of sulphonylurea or insulin may be considered to reduce the risk of hypoglycaemia (see sections 4.4 and 4.8).

The use of Trulicity does not require blood glucose self-monitoring. Blood glucose self-monitoring is necessary to adjust the dose of sulphonylurea or insulin, particularly when Trulicity therapy is started and insulin is reduced. A stepwise approach to insulin dose reduction is recommended.

Missed doses

If a dose is missed, it should be administered as soon as possible if there are at least 3 days (72 hours) until the next scheduled dose. If less than 3 days (72 hours) remain before the next scheduled dose, the missed dose should be skipped and the next dose should be administered on the regularly scheduled day. In each case, patients can then resume their regular once weekly dosing schedule.

Special population

Elderly

No dose adjustment is required based on age (see section 5.2).

Renal impairment

No dose adjustment is required in patients with mild, moderate or severe renal impairment (eGFR < 90 to > 15 mL/min/1.73m2).

There is very limited experience in patients with end stage renal disease (< 15 ml/min/1.73m2), therefore Trulicity cannot be recommended in this population (see sections 5.1 and 5.2).

Hepatic impairment

No dose adjustment is required in patients with hepatic impairment.

Paediatric population

The safety and efficacy of dulaglutide in children aged less than 18 years have not yet been established. No data are available.

Method of administration

Trulicity is to be injected subcutaneously in the abdomen, thigh or upper arm. It should not be administered intravenously or intramuscularly.

The day of weekly administration can be changed if necessary, as long as the last dose was administered 3 or more days (72 hours) before.

4.3 Contraindications

Hypersensitivity to the active substance or to any of the excipients listed in section 6.1.

4.4 Special warnings and precautions for use

Traceability

In order to improve the traceability of biological medicinal products, the name and the batch number of the administered medicinal product should be clearly recorded.

Type 1 diabetes mellitus or diabetic ketoacidosis

Dulaglutide should not be used in patients with type 1 diabetes mellitus or for the treatment of diabetic ketoacidosis. Dulaglutide is not a substitute for insulin.

Diabetic ketoacidosis has been reported in insulin-dependent patients after rapid discontinuation or dose reduction of insulin (see section 4.2).

Severe gastrointestinal disease

Dulaglutide has not been studied in patients with severe gastrointestinal disease, including severe gastroparesis, and is therefore not recommended in these patients.

Dehydration

Dehydration, sometimes leading to acute renal failure or worsening renal impairment, has been reported in patients treated with dulaglutide, especially at the initiation of treatment. Many of the reported adverse renal events occurred in patients who had experienced nausea, vomiting, diarrhoea, or dehydration. Patients treated with dulaglutide should be advised of the potential risk of dehydration, particularly in relation to gastrointestinal adverse reactions and take precautions to avoid fluid depletion.

Acute pancreatitis

Use of GLP-1 receptor agonists has been associated with a risk of developing acute pancreatitis. In clinical trials, acute pancreatitis has been reported in association with dulaglutide (see section 4.8).

Patients should be informed of the characteristic symptoms of acute pancreatitis. If pancreatitis is suspected, dulaglutide should be discontinued. If pancreatitis is confirmed, dulaglutide should not be restarted. In the absence of other signs and symptoms of acute pancreatitis, elevations in pancreatic enzymes alone are not predictive of acute pancreatitis (see section 4.8).

Hypoglycaemia

Patients receiving dulaglutide in combination with sulphonylurea or insulin may have an increased risk of hypoglycaemia. The risk of hypoglycaemia may be lowered by a reduction in the dose of sulphonylurea or insulin (see sections 4.2 and 4.8).

Sodium content

This medicinal product contains less than 1 mmol sodium (23 mg) per dose, that is to say essentially ‘sodium- free’.

4.5 Interaction with other medicinal products and other forms of interaction

Dulaglutide delays gastric emptying and has the potential to impact the rate of absorption of concomitantly administered oral medicinal products. In the clinical pharmacology studies described below, dulaglutide doses up to 1.5 mg did not affect the absorption of the orally administered medicinal products tested to any clinically relevant degree. For the 4.5 mg dose, absence of major clinically relevant interactions was predicted by physiologically-based pharmacokinetic (PBPK) modelling simulations.

For patients receiving dulaglutide in combination with oral medicinal products with rapid gastrointestinal absorption or prolonged release, there is a potential for altered medicinal product exposure, particularly at the time of dulaglutide treatment initiation.

Sitagliptin

Sitagliptin exposure was unaffected when coadministered with a single 1.5 mg dose of dulaglutide. Following coadministration with 2 consecutive 1.5 mg doses of dulaglutide, sitagliptin AUC(o-t) and Cmax decreased by approximately 7.4 % and 23.1 %, respectively. Sitagliptin tmax increased approximately o.5 hours following coadministration with dulaglutide compared to sitagliptin alone.

Sitagliptin can produce up to 8o % inhibition of DPP-4 over a 24-hour period. Dulaglutide (1.5 mg) coadministration with sitagliptin increased dulaglutide exposure and Cmax by approximately 38 % and 27 %, respectively, and median tmax increased approximately 24 hours. Therefore, dulaglutide does have a high degree of protection against DPP-4 inactivation (see section 5.1, Mechanism of action). The increased exposure may enhance the effects of dulaglutide on blood glucose levels.

Paracetamol

Following a first dose of 1 and 3 mg dulaglutide, paracetamol Cmax was reduced by 36 % and 5o %, respectively, and the median tmax occurred later (3 and 4 hours, respectively). After coadministration with up to 3 mg of dulaglutide at steady state, there were no statistically significant differences on AUC(o-12), Cmax or tmax of paracetamol. No dose adjustment of paracetamol is necessary when administered with dulaglutide.

Atorvastatin

Coadministration of 1.5 mg of dulaglutide with atorvastatin decreased Cmaxand AUC«,—,, up to 70 % and 21 %, respectively, for atorvastatin and its major metabolite o -hydroxyatorvas­tatin. The mean t1/2 of atorvastatin and o -hydroxyatorvastatin were increased by 17 % and 41 %, respectively, following dulaglutide administration. These observations are not clinically relevant. No dose adjustment of atorvastatin is necessary when administered with dulaglutide.

Digoxin

After coadministration of steady state digoxin with 2 consecutive 1.5 mg doses of dulaglutide, overall exposure (AUCt) and tmax of digoxin were unchanged; and Cmax decreased by up to 22 %. This change is not expected to have clinical consequences. No dose adjustment is required for digoxin when administered with dulaglutide.

Anti-hypertensives

Coadministration of multiple dulaglutide 1.5 mg doses with steady state lisinopril caused no clinically relevant changes in the AUC or Cmax of lisinopril. Statistically significant delays in lisinopril tmax of approximately 1 hour were observed on Days 3 and 24 of the study. When a single 1.5 mg dose of dulaglutide and metoprolol were coadministered, the AUC and Cmax of metoprolol increased by19 % and 32 %, respectively. While metoprolol tmax was delayed by 1 hour, this change was not statistically significant. These changes were not clinically relevant; therefore, no dose adjustment of lisinopril or metoprolol is necessary when administered with dulaglutide.

Warfarin

Following dulaglutide (1.5 mg) coadministration, S- and R-warfarin exposure and R-warfarin Cmax were unaffected, and S-warfarin Cmax decreased by 22 %. AUCINR increased by 2 %, which is unlikely to be clinically significant, and there was no effect on maximum international normalised ratio response (INRmax). The time of international normalised ratio response (tINRmax) was delayed by 6 hours, consistent with delays in tmax of approximately 4 and 6 hours for S- and R-warfarin, respectively. These changes are not clinically relevant. No dose adjustment for warfarin is necessary when given together with dulaglutide.

Oral contraceptives

Coadministration of dulaglutide (1.5 mg) with an oral contraceptive (norgestimate 0.18 mg/ethinyl estradiol 0.025 mg) did not affect the overall exposure to norelgestromin and ethinyl estradiol.

Statistically significant reductions in Cmax of 26 % and 13 % and delays in tmax of 2 and 0.30 hours were observed for norelgestromin and ethinyl estradiol, respectively. These observations are not clinically relevant. No dose adjustment for oral contraceptives is required when given together with dulaglutide.

Metformin

Following coadministration of multiple 1.5 mg doses of dulaglutide with steady state metformin (immediate release formula [IR]), metformin AUC increased up to 15 % and Cmax decreased up to 12 %, respectively, with no changes in tmax. These changes are consistent with the gastric emptying delay of dulaglutide and within the pharmacokinetic variability of metformin and thus are not clinically relevant. No dose adjustment for metformin IR is recommended when given with dulaglutide.

4.6 Fertility, pregnancy and lactation

Pregnancy

There are no or limited amount of data from the use of dulaglutide in pregnant women. Studies in animals have shown reproductive toxicity (see section 5.3). Therefore, the use of dulaglutide is not recommended during pregnancy.

Breast-feeding

It is unknown whether dulaglutide is excreted in human milk. A risk to newborns/infants cannot be excluded. Dulaglutide should not be used during breast-feeding.

Fertility

The effect of dulaglutide on fertility in humans is unknown. In the rat, there was no direct effect on mating or fertility following treatment with dulaglutide (see section 5.3).

4.7 Effects on ability to drive and use machines

Trulicity has no or negligible influence on the ability to drive or use machines. When it is used in combination with a sulphonylurea or insulin, patients should be advised to take precautions to avoid hypoglycaemia while driving and using machines (see section 4.4).

4.8 Undesirable effects

Summary of safety profile

In the completed phase 2 and phase 3 studies to support the initial registration of dulaglutide 0.75 mg and 1.5 mg, 4,006 patients were exposed to dulaglutide alone or in combination with other glucose lowering medicinal products. The most frequently reported adverse reactions in clinical trials were gastrointestinal, including nausea, vomiting and diarrhoea. In general, these reactions were mild or moderate in severity and transient in nature. Results from the long-term cardiovascular outcome study with 4,949 patients randomised to dulaglutide and followed for a median of 5.4 years were consistent with these findings.

Tabulated list of adverse reactions

The following adverse reactions have been identified based on evaluation of the full duration of the phase 2 and phase 3 clinical studies, the long-term cardiovascular outcome study and post-marketing reports. The adverse reactions are listed in Table 1 as MedDRA preferred term by system organ class and in order of decreasing incidence (very common: > 1/10; common: > 1/100 to < 1/10; uncommon: > 1/1,000 to < 1/100; rare: > 1/10,000 to < 1/1,000; very rare: < 1/10,000 and not known: cannot be estimated from available data). Within each incidence grouping, adverse reactions are presented in order of decreasing frequency. Frequencies for events have been calculated based on their incidence in the phase 2 and phase 3 registration studies.

Table 1. The frequency of adverse reactions of dulaglutide

System organ class

Very common

Common

Uncommon

Rare

Not known

Immune system disorders

Hypersensitivity

Anaphylactic reaction#

Metabolism and nutrition disorders

Hypoglycaemia* (when used in combination with insulin, glimepiride, metformin! or metformin plus glimepiride)

Hypoglycaemia* (when used as monotherapy or in combination with metformin plus pioglitazone)

Dehydration

Gastrointestinal disorders

Nausea, diarrhoea, vomiting!, abdominal pain!

Decreased appetite, dyspepsia, constipation, flatulence, abdominal distention, gastroesophageal reflux disease, eructation

Acute pancreatitis, delayed gastric emptying

Nonmechanical intestinal obstruction

Hepatobiliary disorders

Cholelithiasis, cholecystitis

Skin and subcutaneous tissue disorders

Angioedema#

General disorders and administration site conditions

Fatigue

Injection site reactions

Investigations

Sinus tachycardia, first degree atrioventricular block (AVB)

  • # From post-marketing reports.

  • * Documented, symptomatic hypoglycaemia with blood glucose < 3.9 mmol/L

fDulaglutide 1.5 mg dose only. For dulaglutide 0.75 mg, adverse reaction met frequency for next lower incidence grouping.

Description of selected adverse reactions

Hypoglycaemia

When dulaglutide 0.75 mg and 1.5 mg were used as monotherapy or in combination with metformin alone or metformin and pioglitazone, the incidences of documented symptomatic hypoglycaemia were 5.9 % to 10.9 % and the rates were 0.14 to 0.62 events/pa­tient/year, and no episodes of severe hypoglycaemia were reported.

The incidences of documented symptomatic hypoglycaemia when dulaglutide 0.75 mg and 1.5 mg, respectively, were used in combination with a sulphonylurea and metformin were 39.0 % and 40.3 % and the rates were 1.67 and 1.67 events/pa­tient/year. The severe hypoglycaemia event incidences were 0 % and 0.7 %, and rates were 0.00 and 0.01 events/pa­tient/year for each dose, respectively. The incidence of documented symptomatic hypoglycaemia when dulaglutide 1.5 mg was used with sulphonylurea alone was 11.3 % and the rate was 0.90 events/pa­tient/year, and there were no episodes of severe hypoglycaemia.

The incidence of documented symptomatic hypoglycaemia when dulaglutide 1.5 mg was used in combination with insulin glargine was 35.3 % and the rate was 3.38 events/pa­tient/year. The severe hypoglycaemia event incidence was 0.7 % and the rate was 0.01 events/pa­tient/year.

The incidences when dulaglutide 0.75 mg and 1.5 mg, respectively, were used in combination with prandial insulin were 85.3 % and 80.0 % and rates were 35.66 and 31.06 events/pa­tient/year. The severe hypoglycaemia event incidences were 2.4 % and 3.4 %, and rates were 0.05 and 0.06 events/pa­tient/year.

In a phase 3 study through to week 52, when dulaglutide 1.5 mg, 3 mg and 4.5 mg were used in combination with metformin, the incidences of documented symptomatic hypoglycaemia were 3.1 %, 2.4 % and 3.1 %, respectively, and rates were 0.07, 0.05 and 0.07 events/pa­tient/year; one episode of severe hypoglycaemia was reported with dulaglutide 1.5 mg and 4.5 mg, respectively.

Gastrointestinal adverse reactions

Cumulative reporting of gastrointestinal events up to 104 weeks with dulaglutide 0.75 mg and 1.5 mg, respectively, included nausea (12.9 % and 21.2 %) , diarrhoea (10.7 % and 13.7 %) and vomiting (6.9 % and 11.5 %). These were typically mild or moderate in severity and were reported to peak during the first 2 weeks of treatment and rapidly declined over the next 4 weeks, after which the rate remained relatively constant.

In a phase 3 study with 1.5 mg, 3 mg and 4.5 mg dulaglutide doses respectively, cumulative reporting of gastrointestinal events through to 52 weeks included nausea (14.2 %, 16.1 % and 17.3 %), diarrhoea (7.7 %, 12.0 % and 11.6 %) and vomiting (6.4 %, 9.1 % and 10.1 %). In clinical pharmacology studies conducted in patients with type 2 diabetes mellitus up to 6 weeks, the majority of gastrointestinal events were reported during the first 2–3 days after the initial dose and declined with subsequent doses.

Acute pancreatitis

The incidence of acute pancreatitis in phase 2 and 3 registration studies was 0.07 % for dulaglutide compared to 0.14 % for placebo and 0.19 % for comparators with or without additional background antidiabetic therapy. Acute pancreatitis and pancreatitis have also been reported in the post-marketing setting.

Pancreatic enzymes

Dulaglutide is associated with mean increases from baseline in pancreatic enzymes (lipase and/or pancreatic amylase) of 11 % to 21 % (see section 4.4). In the absence of other signs and symptoms of acute pancreatitis, elevations in pancreatic enzymes alone are not predictive of acute pancreatitis.

Heart rate increase

Small mean increases in heart rate of 2 to 4 beats per minute (bpm) and a 1.3 % and 1.4 % incidence of sinus tachycardia, with a concomitant increase from baseline > 15 bpm, were observed with dulaglutide 0.75 mg and 1.5 mg, respectively.

In a phase 3 study with 1.5 mg, 3 mg and 4.5 mg dulaglutide doses, the incidence of sinus tachycardia, with a concomitant increase from baseline > 15 bpm, was 2.6 %, 1.9 % and 2.6 % respectively. Mean increases in heart rate of 1 – 4 beats per minute (bpm) were observed.

First degree AV block/PR interval prolongation

Small mean increases from baseline in PR interval of 2 to 3 msec and a 1.5 % and 2.4 % incidence of first-degree AV block were observed with dulaglutide 0.75 mg and 1.5 mg, respectively.

In a phase 3 study with 1.5 mg, 3 mg and 4.5 mg dulaglutide doses, the incidence of first-degree AV block was 1.2 %, 3.8 % and 1.7 % respectively. Mean increases from baseline in PR interval of 3 – 5 msec were observed.

Immunogenicity

In registration studies, treatment with dulaglutide was associated with a 1.6 % incidence of treatment emergent dulaglutide anti-drug antibodies, indicating that the structural modifications in the GLP-1 and modified IgG4 parts of the dulaglutide molecule, together with high homology with native GLP-1 and native IgG4, minimise the risk of immune response against dulaglutide. Patients with dulaglutide anti-drug antibodies generally had low titres, and although the number of patients developing dulaglutide anti-drug antibodies was low, examination of the phase 3 data revealed no clear impact of dulaglutide anti-drug antibodies on changes in HbA1c. None of the patients with systemic hypersensitivity developed dulaglutide anti-drug antibodies.

Hypersensitivity

In the phase 2 and phase 3 registration studies, systemic hypersensitivity events (e.g., urticaria, edema) were reported in 0.5 % of patients receiving dulaglutide. Cases of anaphylactic reaction have been rarely reported with marketed use of dulaglutide.

Injection site reactions

Injection site adverse events were reported in 1.9 % of patients receiving dulaglutide. Potentially immune-mediated injection site adverse events (e.g., rash, erythema) were reported in 0.7 % of patients and were usually mild.

Discontinuation due to an adverse event

In studies of 26 weeks duration, the incidence of discontinuation due to adverse events was 2.6 % (0.75 mg) and 6.1 % (1.5 mg) for dulaglutide versus 3.7 % for placebo. Through the full study duration (up to 104 weeks), the incidence of discontinuation due to adverse events was 5.1 % (0.75 mg) and 8.4 % (1.5 mg) for dulaglutide. The most frequent adverse reactions leading to discontinuation for 0.75 mg and 1.5 mg dulaglutide, respectively, were nausea (1.0 %, 1.9 %), diarrhoea (0.5 %, 0.6 %), and vomiting (0.4 %, 0.6 %), and were generally reported within the first 4 – 6 weeks.

In a phase 3 study with 1.5 mg, 3 mg and 4.5 mg dulaglutide doses, the incidence of discontinuation due to adverse events through 52 weeks was 6.0 % (1.5 mg), 7.0 % (3 mg) and 8.5 % (4.5 mg). The most frequent adverse reactions leading to discontinuation for dulaglutide 1.5 mg, 3 mg and 4.5 mg, respectively, were nausea (1.3 %, 1.3 %, 1.5 %), diarrhoea (0.2 %, 1.0 %, 1.0 %), and vomiting (0.0 %, 0.8 %, 1.3 %).

Dulaglutide doses of 3 mg and 4.5 mg

The safety profile in patients treated with dulaglutide 3 mg and 4.5 mg once weekly is consistent with that described above for dulaglutide doses of 0.75 mg and 1.5 mg once weekly.

Reporting of suspected adverse reactions

Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via the national reporting system listed in

4.9 Overdose

Effects of overdose with dulaglutide in clinical studies have included gastrointestinal disorders and hypoglycaemia. In the event of overdose, appropriate supportive treatment should be initiated according to the patient’s clinical signs and symptoms.

5. PHARMACOLOGICAL PROPERTIES5.1 Pharmacodynamic properties

Pharmacotherapeutic group: Drugs used in diabetes, blood glucose lowering drugs, excl. insulins, ATC code: A10BJ05

Mechanism of action

Dulaglutide is a long-acting glucagon-like peptide 1 (GLP-1) receptor agonist. The molecule consists of 2 identical disulfide-linked chains, each containing a modified human GLP-1 analogue sequence covalently linked to a modified human immunoglobulin G4 (IgG4) heavy chain fragment (Fc) by a small peptide linker. The GLP-1 analog portion of dulaglutide is approximately 90 % homologous to native human GLP-1 (7–37). Native GLP-1 has a half-life of 1.5 – 2 minutes due to degradation by DPP-4 and renal clearance. In contrast to native GLP-1, dulaglutide is resistant to degradation by DPP-4, and has a large size that slows absorption and reduces renal clearance. These engineering features result in a soluble formulation and a prolonged half-life of 4.7 days, which makes it suitable for once-weekly subcutaneous administration. In addition, the dulaglutide molecule was engineered to prevent the Fcy receptor-dependent immune response and to reduce its immunogenic potential.

Dulaglutide exhibits several antihyperglycaemic actions of GLP-1. In the presence of elevated glucose concentrations, dulaglutide increases intracellular cyclic AMP (cAMP) in pancreatic beta cells leading to insulin release. Dulaglutide suppresses glucagon secretion which is known to be inappropriately elevated in patients with type 2 diabetes. Lower glucagon concentrations lead to decreased hepatic glucose output. Dulaglutide also slows gastric emptying.

Pharmacodynamic effects

Dulaglutide improves glycaemic control through the sustained effects of lowering fasting, pre-meal and postprandial glucose concentrations in patients with type 2 diabetes starting after the first dulaglutide administration and is sustained throughout the once weekly dosing interval.

A pharmacodynamic study with dulaglutide demonstrated, in patients with type 2 diabetes, a restoration of first phase insulin secretion to a level that exceeded levels observed in healthy subjects on placebo and improved second phase insulin secretion in response to an intravenous bolus of glucose. In the same study, a single 1.5 mg dose of dulaglutide appeared to increase maximal insulin secretion from the P—cells, and to enhance p—cell function in subjects with type 2 diabetes mellitus as compared with placebo.

Consistent with the pharmacokinetic profile, dulaglutide has a pharmacodynamic profile suitable for once weekly administration (see section 5.2).

Clinical efficacy and safety

Glycaemic control

The safety and efficacy of dulaglutide were evaluated in ten randomised, controlled, phase 3 trials involving 8,035 patients with type 2 diabetes. Of these, 1,644 were > 65 years of which 174 were > 75 years. These studies included 5,650 dulaglutide treated patients, of whom 1,558 were treated with Trulicity 0.75 mg weekly, 2,862 were treated with Trulicity 1.5 mg weekly, 616 were treated with Trulicity 3 mg weekly and 614 were treated with Trulicity 4.5 mg weekly. In all studies, dulaglutide produced clinically significant improvements in glycaemic control as measured by glycosylated haemoglobin A1c (HbA1c).

Monotherapy

Dulaglutide was studied in a 52—week active controlled monotherapy study in comparison to metformin. Trulicity 1.5 mg and 0.75 mg were superior to metformin (1500 — 2000 mg/day) in the reduction in HbA1c and a significantly greater proportion of patients reached an HbA1c target of < 7.0 % and < 6.5 % with Trulicity 1.5 mg and Trulicity 0.75 mg compared to metformin at 26 weeks.

Table 2. Results of a 52-week active controlled monotherapy study with two doses of dulaglutide in comparison to metformin

Baseline    Mean      Patients at target    Change in Change in

HbAlc change in        HbAlc          FBG    body weight

HbAlc

(%)       (%)     < 7.0 %   < 6.5 % (mmol/L)      (kg)

(%)      (%)

26 weeks

Dulaglutide 1.5 mg once weekly (n = 269)

7.63

–0.781'1'

61.5#

46.0##

–1.61

–2.29

Dulaglutide 0.75 mg once weekly (n = 270)

7.58

–0.711'1'

62.6#

40.0#

–1.46

–1.36#

Metformin

1500 – 2000 mg/day (n = 268)

7.60

–0.56

53.6

29.8

–1.34

–2.22

52 weeks

Dulaglutide 1.5 mg once weekly (n = 269)

7.63

–0.701'1'

60.0#

42.3##

–1.56#

–1.93

Dulaglutide 0.75 mg once weekly (n = 270)

7.58

–0.551

53.2

34.7

–1.00

–1.09#

Metformin

1500 – 2000 mg/day (n = 268)

7.60

–0.51

48.3

28.3

–1.15

–2.20

^ multiplicity adjusted 1-sided p-va p-value < 0.025, for superiority o

# p < 0.05, ##p < 0.001 dulaglutide

FBG = fasting blood glucose

ue < 0.025, dulaglutide treatment gro

or noninferiority; multiplicity adjusted 1-sided to metformin, assessed for HbA1c only up compared to metformin

The rate of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and 0.75 mg, and metformin were 0.62, 0.15, and 0.09 episodes/pa­tient/year, respectively. No cases of severe hypoglycaemia were observed.

Combination therapy with metformin

The safety and efficacy of dulaglutide was investigated in a placebo and active controlled (sitagliptin 100 mg daily) study of 104 weeks duration, all in combination with metformin. Treatment with Trulicity 1.5 mg and 0.75 mg resulted in a superior reduction in HbA1c compared to sitagliptin at 52 weeks, accompanied by a significantly greater proportion of patients achieving HbA1c targets of < 7.0 % and < 6.5 %. These effects were sustained to the end of the study (104 weeks).

Table 3. Results of a 104-week placebo and active controlled study with two doses of dulaglutide in comparison to sitagliptin

Baseline HbA1c

(%)

Mean change in HbA1c (%)

Patients at target HbA1c

Change in FBG

(mmol/L)

Change in body weight (kg)

< 7.0 %

(%)

< 6.5 % (%)

26 weeks

Dulaglutide 1.5 mg once weekly (n=304)

8.12

–1.22,##

60.9,##

46.7,##

–2.38,##

–3.18,##

Dulaglutide 0.75 mg once weekly (n=302)

8.19

–1.01,##

55.2,##

31.0,##

–1.97,##

–2.63,##

Placebo (n = 177)

8.10

0.03

21.0

12.5

–0.49

–1.47

Sitagliptin 100 mg once daily

(n=315)

8.09

–0.61

37.8

21.8

–0.97

–1.46

52 weeks

Dulaglutide 1.5 mg once weekly (n=304)

8.12

–1.10

57.6##

41.7##

–2.38##

–3.03##

Dulaglutide 0.75 mg once weekly (n=302)

8.19

–0.87

48.8##

29.0##

–1.63##

–2.60##

Sitagliptin 100 mg once daily (n = 315)

8.09

–0.39

33.0

19.2

–0.90

–1.53

104 weeks

Dulaglutide 1.5 mg once weekly (n=304)

8.12

–0.99

54.3##

39.1##

–1.99##

–2.88##

Dulaglutide 0.75 mg once weekly (n=302)

8.19

–0.71

44.8##

24.2##

–1.39##

–2.39

Sitagliptin 100 mg once daily (n = 315)

8.09

–0.32

31.1

14.1

–0.47

–1.75

** multiplicity adjusted

1-sided p-val

ue < 0.025, f

or superiority of dulaglutide compared to sitagliptin,

assessed only for HbA1c at 52 and 104 weeks

** multiplicity adjusted 1-sided p-value < 0.001 for superiority of dulaglutide compared to placebo,

assessed for HbA1c only

  • ** p < 0.001 dulaglutide treatment group compared to placebo

  • ## p < 0.001 dulaglutide treatment group compared to sitagliptin

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and 0.75 mg, and sitagliptin were 0.19, 0.18, and 0.17 episodes/pa­tient/year, respectively. No cases of severe hypoglycaemia with dulaglutide were observed.

The safety and efficacy of dulaglutide was also investigated in an active controlled study (liraglutide 1.8 mg daily) of 26 weeks duration, both in combination with metformin. Treatment with Trulicity 1.5 mg resulted in similar lowering of HbA1c and patients achieving HbA1c targets of < 7.0 % and < 6.5 % compared to liraglutide.

Table 4. Results of a 26-week active controlled study of one dose of dulaglutide in comparison to liraglutide

Baseline Mean      Patients at target     Change in Change in

HbAlc change        HbAlc          FBG      body

in                                           ­weight

HbAlc

(%)      (%)     < 7.0 %    < 6.5 % (mmol/L)     (kg)

(%)       (%)

26 weeks

Dulaglutide 1.5 mg once weekly (n = 299)

8.06

–1.42*

68.3

54.6

–1.93

–2.90#

Liraglutide+ 1.8 mg daily (n = 300)

8.05

–1.36

67.9

50.9

–1.90

–3.61

* 1-sided p-value p < 0.001, for noninferiority of dulaglutide compared to liraglutide, assessed only for HbA1c.

# p < 0.05 dulaglutide treatment group compared to liraglutide.

+ Patients randomised to liraglutide were initiated at a dose of 0.6 mg/day. After Week 1, patients were up-titrated to 1.2 mg/day and then at Week 2 to 1.8 mg/day.

The rate of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg was 0.12 episodes/pa­tient/year and with liraglutide was 0.29 episodes/pa­tient/year. No cases of severe hypoglycaemia were observed.

Combination therapy with metformin and sulphonylurea

In an active controlled study of 78 weeks duration, dulaglutide was compared to insulin glargine, both on a background of metformin and a sulphonylurea. At 52 weeks, Trulicity 1.5 mg demonstrated superior lowering in HbA1c to insulin glargine which was maintained at 78 weeks; whereas lowering in HbA1c with Trulicity 0.75 mg was non-inferior to insulin glargine. With Trulicity 1.5 mg a significantly higher percentage of patients reached a target HbAlc of < 7.0 % or < 6.5 % at 52 and 78 weeks compared to insulin glargine.

Table 5. Results of a 78-week active controlled study with two doses of dulaglutide in comparison to insulin glargine

Baseline Mean      Patients at target     Change in Change in

HbAlc change        HbAlc          FBG      body

in                                           ­weight

HbAlc

(%)      (%)     < 7.0 %    < 6.5 % (mmol/L)     (kg)

(%)       (%)

52 weeks

Dulaglutide 1.5 mg once weekly (n = 273)

8.18

–1.081'1'

53.2##

27.0##

–1.50

–1.87##

Dulaglutide 0.75 mg once weekly (n = 272)

8.13

–0.761'

37.1

22.5#

–0.87##

–1.33##

Insulin glargine+ once daily (n = 262)

8.10

–0.63

30.9

13.5

–1.76

1.44

78 weeks

Dulaglutide 1.5 mg once weekly (n = 273)

8.18

–0.90tt

49.0##

28.1##

–1.10#

–1.96##

Dulaglutide 0.75 mg once weekly (n = 272)

8.13

–0.62f

34.1

22.1

–0.58##

–1.54##

Insulin glargine+ once daily (n = 262)

8.10

–0.59

30.5

16.6

–1.58

1.28

^ multiplicity adjusted 1-sided p-va p-value < 0.025, for superiority o # p < 0.05, ##p < 0.001 dulaglutide + Insulin glargine doses were adjust

ue < 0.025, for noninferiority; multiplicity adjusted dulaglutide to insulin glargine, assessed for HbA1c o treatment group compared to insulin glargine ed utilising an algorithm with a fasting plasma glucos

1-sided nly

e target of

< 5.6 mmol/L

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and 0.75 mg, and insulin glargine were 1.67, 1.67, and 3.02 episodes/pa­tient/year, respectively. Two cases of severe hypoglycaemia were observed with dulaglutide 1.5 mg and two cases of severe hypoglycaemia were observed with insulin glargine.

Combination therapy with sulphonylurea

The safety and efficacy of dulaglutide as add-on to a sulphonylurea was investigated in a placebo controlled study of 24 weeks duration. Treatment with Trulicity 1.5 mg in combination with glimepiride resulted in a statistically significant reduction in HbA1c compared to placebo with glimepiride at 24 weeks. With Trulicity 1.5 mg, a significantly higher percentage of patients reached a target HbAlc of < 7.0 % and < 6.5 % at 24 weeks compared to placebo.

Table 6. Results of a 24-week placebo controlled study of dulaglutide as add-on to glimepiride

Baseline Mean      Patients at target     Change in Change in

HbAlc change        HbAlc          FBG      body

in                                           ­weight

HbAlc

(%)      (%)     < 7.0 %    < 6.5 % (mmol/L)     (kg)

(%)       (%)

24 weeks

Dulaglutide 1.5 mg once weekly (n = 239)

8.39

–1.38

55.3

40.0

–1.70

–0.91

Placebo (n = 60)

8.39

–0.11

18.9

9.4

0.16

–0.24

** p < 0.001 for superiority of dulaglutide compared to placebo, with overall type I error controlled

** p < 0.001 for dulaglutide treatment group compared to placebo

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and placebo were 0.90 and 0.04 episodes/pa­tient/year, respectively. No cases of severe hypoglycaemia were observed for dulaglutide or placebo.

Combination therapy with SGLT2 inhibitor with or without metformin

The safety and efficacy of dulaglutide as add-on to sodium-glucose co-transporter 2 inhibitor (SGLT2i) therapy (96 % with and 4 % without metformin) were investigated in a placebo controlled study of 24 weeks duration. Treatment with Trulicity 0.75 mg or Trulicity 1.5 mg in combination with SGLT2i therapy resulted in a statistically significant reduction in HbA1c compared to placebo with SGLT2i therapy at 24 weeks. With both Trulicity 0.75 mg and 1.5 mg, a significantly higher percentage of patients reached a target HbAlc of < 7.0 % and < 6.5 % at 24 weeks compared to placebo.

Table 7. Results of a 24-week placebo controlled study of dulaglutide as add-on to SGLT2i therapy

Baseline Mean      Patients at target     Change in Change in

HbAlc change        HbAlc          FBG      body

in                                           ­weight

HbAlc

(%)      (%)    < 7. 0% a   < 6.5 % (mmol/L)     (kg)

(%)       (%)

24 weeks

Dulaglutide 0.75 mg once weekly (n = 141)

8.05

–1.19

58.8

38.9

–1.44

–2.6

Dulaglutide 1.5 mg once weekly (n=142)

8.04

–1.33

67.4

50.8

–1.77

–3.1

Placebo (n = 140)

8.05

–0.51

31.2

14.6

–0.29

–2.3

** p < 0.001 for superiority of dulaglutide compared to placebo, with overall type I error controlled

** p < 0.001 for dulaglutide treatment group compared to placebo

A Patients who withdrew from randomised treatment before 24 weeks were considered as not meeting the target

The rates of documented symptomatic hypoglycaemia with dulaglutide 0.75 mg, dulaglutide 1.5 mg, and placebo were 0.15, 0.16 and 0.12 episodes/pa­tient/year, respectively. One patient reported severe hypoglycaemia with dulaglutide 0.75 mg in combination with SGLT2i therapy and none with dulaglutide 1.5 mg or placebo.

Combination therapy with metformin and pioglitazone

In a placebo and active (exenatide twice daily) controlled study, both in combination with metformin and pioglitazone, Trulicity 1.5 mg and 0.75 mg demonstrated superiority for HbA1c reduction in comparison to placebo and exenatide, accompanied by a significantly a greater percentage of patients achieving HbAlc targets of < 7.0 % or < 6.5 %

Table 8. Results of a 52-week active controlled study with two doses of dulaglutide in comparison to exenatide

Baseline    Mean      Patients at target     Change in Change in

HbAlc change in       HbAlc          FBG      body

HbAlc                                   ­weight

(%)       (%)     < 7.0 %   < 6.5 % (mmol/L)     (kg)

(%)      (%)

26 weeks

Dulaglutide 1.5 mg once weekly (n = 279)

8.10

–1.51«,"

78.2,##

62.7,##

–2.36,##

–1.30

Dulaglutide 0.75 mg once weekly (n = 280)

8.05

–1.30Ji/tt

65.8/##

53.2/##

–1.90/##

0.20 /##

Placebo (n = 141)

8.06

–0.46

42.9

24.4

–0.26

1.24

Exenatide+

10 mcg twice daily (n = 276)

8.07

–0.99

52.3

38.0

–1.35

–1.07

52 weeks

Dulaglutide 1.5 mg once weekly (n = 279)

8.10

–1.36"

70.8##

57.2##

–2.04##

–1.10

Dulaglutide 0.75 mg once weekly (n = 280)

8.05

–1.07"

59.1#

48.3##

–1.58#

0.44#

Exenatide+

10 mcg twice daily (n = 276)

8.07

–0.80

49.2

34.6

–1.03

–0.80

" multiplicity adjusted 1-sided p-va for HbA1c only

" multiplicity adjusted 1-sided p-va assessed for HbA1c only

p < 0.05, p < 0.001 dulaglutide # p < 0.05, ##p < 0.001 dulaglutide t + Exenatide dose was 5 mcg twice d

lue < 0.025,

lue < 0.001 f

treatment gr reatment gro aily for first

for superiority of dulaglutide to exenatide, assessed

or superiority of dulaglutide compared to placebo,

oup compared to placebo

up compared to exenatide

4 weeks and 10 mcg twice daily thereafter

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and 0.75 mg, and exenatide twice daily were 0.19, 0.14, and 0.75 episodes/pa­tient/year, respectively. No cases of severe hypoglycaemia were observed for dulaglutide and two cases of severe hypoglycaemia were observed with exenatide twice daily.

Combination therapy with titrated basal insulin, with or without metformin

In a 28-week placebo controlled study, Trulicity1.5 mg was compared to placebo as add-on to titrated basal insulin glargine (88 % with and 12 % without metformin) to evaluate the effect on glycaemic control and safety. To optimise the insulin glargine dose, both groups were titrated to a target fasting serum glucose of < 5.6 mmol/L. The mean baseline dose of insulin glargine was 37 units/day for patients receiving placebo and 41 units/day for patients receiving Trulicity 1.5 mg. The initial insulin glargine doses in patients with HbA1c < 8.0 % were reduced by 20 %. At the end of the 28-week treatment period the dose was 65 units/day and 51 units/day, for patients receiving placebo and Trulicity 1.5 mg, respectively. At 28 weeks, treatment with once weekly Trulicity 1.5 mg resulted in a statistically significant reduction in HbA1c compared to placebo and a significantly greater percentage of patients achieving HbAlc targets of < 7.0 % and < 6.5 % (Table 9).

Table 9. Results of a 28-week study of dulaglutide compared to placebo as add-on to titrated insulin glargine

Baseline     Mean       Patients at target     Change in Change in

HbAlc change in         HbAlc          FBG      body

HbAlc                                     ­weight

(%)       (%)      < 7.0 %    < 6.5 % (mmol/L)     (kg)

(%)       (%)

28 weeks

Dulaglutide 1.5 mg once weekly and insulin glargine (n = 150)

8.41

–1.44

66.7

50.0

–2.48

–1.91

Placebo once weekly and insulin glargine (n = 150)

8.32

–0.67

33.3

16.7

–1.55

0.50

« p < 0.001 for superiority of dulaglutide compared to placebo, overall type I error controlled

p < 0.001 dulaglutide treatment group compared to placebo

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and insulin glargine were 3.38 episodes/pa­tient/year compared to placebo and insulin glargine 4.38 episodes/pa­tient/year. One patient reported severe hypoglycaemia with dulaglutide 1.5 mg in combination with insulin glargine and none with placebo.

Combination therapy with prandial insulin with or without metformin

In this study, patients on 1 or 2 insulin injections per day prior to study entry, discontinued their prestudy insulin regimen and were randomised to dulaglutide once weekly or insulin glargine once daily, both in combination with prandial insulin lispro three times daily, with or without metformin. At 26 weeks, both Trulicity 1.5 mg and 0.75 mg were superior to insulin glargine in lowering of HbA1c and this effect was sustained at 52 weeks. A greater percentage of patients achieved HbA1c targets of < 7.0 % or < 6.5 % at 26 weeks and < 7.0 % at 52 weeks than with insulin glargine.

Table 10. Results of a 52-week active controlled study with two doses of dulaglutide in comparison to insulin glargine

Baseline    Mean      Patients at target     Change in Change in

HbAlc change in       HbAlc          FBG      body

HbAlc                                   ­weight

(%)       (%)      < 7.0 %   < 6.5 % (mmol/L)     (kg)

(%)      (%)

26 weeks

Dulaglutide 1.5 mg once weekly (n = 295)

8.46

–1.64"

67.6#

48.0#

–0.27##

–0.87##

Dulaglutide 0.75 mg once weekly (n = 293)

8.40

–1.59"

69.0#

43.0

0.22##

0.18##

Insulin glargine+ once daily (n = 296)

8.53

–1.41

56.8

37.5

–1.58

2.33

52 weeks

Dulaglutide 1.5 mg once weekly (n = 295)

8.46

–1.48"

58.5#

36.7

0.08##

–0.35##

Dulaglutide 0.75 mg once weekly (n = 293)

8.40

–1.42"

56.3

34.7

0.41##

0.86##

Insulin glargine+ once daily (n = 296)

8.53

–1.23

49.3

30.4

–1.01

2.89

" multiplicity adjusted 1-sided p-va assessed for HbA1c only

# p < 0.05, ##p < 0.001 dulaglutide

+ Insulin glargine doses were adjust

lue < 0.025,

treatment gro ed utilizing a

for superiority of dulaglutide to insulin g

up compared to insulin glargine n algorithm with a fasting plasma glucos

largine,

e target of

< 5.6 mmol/L

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg and 0.75 mg, and insulin glargine were 31.06, 35.66, and 40.95 episodes/pa­tient/year, respectively. Ten patients reported severe hypoglycaemia with dulaglutide 1.5 mg, seven with dulaglutide 0.75 mg, and fifteen with insulin glargine.

Fasting blood glucose

Treatment with dulaglutide resulted in significant reductions from baseline in fasting blood glucose. The majority of the effect on fasting blood glucose concentrations occurred by 2 weeks. The improvement in fasting glucose was sustained through the longest study duration of 104 weeks.

Postprandial glucose

Treatment with dulaglutide resulted in significant reductions in mean post prandial glucose from baseline (changes from baseline to primary time point –1.95 mmol/L to –4.23 mmol/L).

Beta-cell function

Clinical studies with dulaglutide have indicated enhanced beta-cell function as measured by homeostasis model assessment (HOMA2-%B). The durability of effect on beta-cell function was maintained through the longest study duration of 104 weeks.

Body weight

Trulicity 1.5 mg was associated with sustained weight reduction over the duration of studies (from baseline to final time point –0.35 kg to –2.90 kg). Changes in body weight with Trulicity 0.75 mg ranged from 0.86 kg to –2.63 kg. Reduction in body weight was observed in patients treated with dulaglutide irrespective of nausea, though the reduction was numerically larger in the group with nausea.

Patient reported outcomes

Dulaglutide significantly improved total treatment satisfaction compared to exenatide twice daily. In addition, there was significantly lower perceived frequency of hyperglycaemia and hypoglycaemia compared to exenatide twice daily.

Blood pressure

The effect of dulaglutide on blood pressure as assessed by Ambulatory Blood Pressure Monitoring was evaluated in a study of 755 patients with type 2 diabetes. Treatment with dulaglutide provided reductions in systolic blood pressure (SBP) (-2.8 mmHg difference compared to placebo) at 16 weeks. There was no difference in diastolic blood pressure (DBP). Similar results for SBP and DBP were demonstrated at the final 26 week time point of the study.

Cardiovascular Evaluation

Meta-analysis of phase 2 and 3 studies

In a meta-analysis of phase 2 and 3 registration studies, a total of 51 patients (dulaglutide:

26 [N = 3,885]; all comparators: 25 [N = 2,125]) experienced at least one cardiovascular (CV) event (death due to CV causes, nonfatal MI, nonfatal stroke, or hospitalisation for unstable angina). The results showed that there was no increase in CV risk with dulaglutide compared with control therapies (HR: 0.57; CI: [0.30, 1.10] ).

Cardiovascular outcome study

The Trulicity long-term cardiovascular outcome study was a placebo-controlled, double-blind clinical trial. Type 2 diabetes patients were randomly allocated to either Trulicity 1.5 mg (4,949) or placebo (4,952) both in addition to standards of care for type 2 diabetes (the 0.75 mg dose was not administered in this study). The median study follow-up time was 5.4 years.

The mean age was 66.2 years, the mean BMI was 32.3 kg/m2, and 46.3 % of patients were female. There were 3,114 (31.5 %) patients with established CV disease. The median baseline HbA1c was 7.2 %. The Trulicity treatment arm included patients > 65 years (n = 2,619) and > 75 years (n = 484), and patients with mild (n = 2,435), moderate (n = 1,031) or severe (n = 50) renal impairment.

The primary endpoint was the time from randomisation to first occurrence of any major adverse cardiovascular events (MACE): CV death, non-fatal myocardial infarction, or non-fatal stroke.

Trulicity was superior in preventing MACE compared to placebo (Figure 1). Each MACE component contributed to the reduction of MACE, as shown in Figure 2.

Figure 1. Kaplan-Meier plot of time to first occurrence of the composite outcome: CV death, non-fatal myocardial infarction or non-fatal stroke, in the dulaglutide long-term cardiovascular outcome study

Hazard Ratio Dulaglutide, Placebo, (95% Cl)          n (%)        n (%)

Primary CV Endpoints

0.88           594        663

(0.79,0.99)        (12.0)        (13.4)

Components of CV Endpoints

  • Nonfatal Stroke            -------•---------

0.76           135         175

(0.61,0.95)         (2.7)         (3.5)

CV Death

0.91           317        346

(0.78, 1.06}          (6.4)          (7.0)

Nonfatal Ml

0.96           205        212

(0.79, 1.16)          (4.1)          (4.3)

All Death

.                           ­0.90           536     592

(0.80, 1.01)        (10.8)        (12.0)

Subgroup Analysis

CVD

No Prior CVD

0.87           277        317

(0.74, 1.02)         (9.0)         (10.1)

Prior CVD

0.87           280        315

(0.74, 1.02)        (17.9)        (20.3)

Baseline HbAlc

>Median (7.2%)

0.86           328        373

(0.74, 1.00)        (12.6)        (14.3)

<Median (7.2%)

0.90           263        289

(0.76, 1.06)        (11.3)        (12.4)

Gender

Male

0.90           376        414

(0.79, 1.04)        (14.2)        (15.5)

Female

0.85           218        249

(0.71, 1.02)         (9.5)         (10.9)

Duration of Diabetes

<5 years

0.84           128        146

(0.66, 1.06)        (10.4)        (12.2)

>5 years and <10 years

0.89           174         196

(0.72, 1.09)        (12.0)        (13.3)

>10 years

0.90           292        321

(0.77, 1.06)        (12.8)        (14.1)

4

0

Cl – confidence interval CV – cardiovascular

6 0.7 0.8 0.9 1

Favours Dulaglutide

0 1.1 1.2 1.3 1.

Favours Placebo

CVD – cardiovascular disease HbAlc – glycated haemoglobin Ml – myocardial infarction

Figure 2. Forest plot of analyses of individual cardiovascular event types, all cause death, and consistency of effect across subgroups for the primary endpoint

A significant and sustained reduction in HbA1c levels from baseline to month 60 was observed with Trulicity vs placebo, in addition to standard of care (-0.29 % vs 0.22 %; estimated treatment difference –0.51 % [-0.57; –0.45]; p < 0.001). There were significantly fewer patients in the Trulicity group who received an additional glycaemic intervention compared to placebo (Trulicity: 2,086 [42.2 %]; placebo: 2,825 [57.0 %]; p < 0.001).

Combination of dulaglutide 4.5 mg, 3 mg and 1.5 mg therapy with metformin

The safety and efficacy of dulaglutide 3 mg and 4.5 mg once weekly compared to dulaglutide 1.5 mg once weekly as add-on to metformin were investigated in a 52 weeks study. At 36 weeks, both Trulicity 3 mg and 4.5 mg were superior to Trulicity 1.5 mg in lowering of HbA1c and body weight.

A greater percentage of patients achieved HbAlc targets of < 7.0 % or < 6.5 % at 36 weeks with Trulicity 3 mg and Trulicity 4.5 mg. The proportions of patients that achieved > 5 % body weight reduction from baseline were 31 %, 40 % and 49 % for Trulicity 1.5 mg, 3 mg and 4.5 mg respectively. These effects were sustained through 52 weeks.

Table 11. Results of an active controlled study comparing three doses of dulaglutide

Baseline HbA1c

(%)

Mean change in HbAlc (%)

Patients at target HbAlc

Change in FBG

(mmol/L)

Change in body weight (kg)

< 7.0 % (%)

< 6.5 % (%)

36 weeks

Dulaglutide 1.5 mg once weekly (n=612)

8.64

–1.53

57.0

38.1

–2.45

–3.1

Dulaglutide 3 mg once weekly (n = 616)

8.63

–1.71#

64.7#

48.4

–2.66

–4.0#

Dulaglutide 4.5 mg once weekly (n=614)

8.64

–1.87##

71.5#

51.7

–2.90#

–4.7##

52 weeks

Dulaglutide 1.5 mg once weekly (n=612)

8.64

–1.52

58.6

40.4

–2.39

–3.5

Dulaglutide 3 mg once weekly (n=616)

8.63

–1.71*

65.4*

49.2*

–2.70*

–4.3*

Dulaglutide 4.5 mg once weekly (n=614)

8.64

–1.83«

71.7

51.3

–2.92

–5.0

# p < 0.05, ##p < 0.001 for superiority compared to dulaglutide 1.5 mg, adjusted p-values with overall type I error controlled

*p < 0.05, «p < 0.001 compared to dulaglutide 1.5 mg

Results target the on-treatment effect (analysis is based on mixed models for repeated measurements or longitudinal logistic regression).

Figure 3. Mean change in HbA1c (%) and body weight (kg) from baseline to week 52

The rates of documented symptomatic hypoglycaemia with dulaglutide 1.5 mg, 3 mg and 4.5 mg were 0.07, 0.05 and 0.07 episodes/pa­tient/year respectively. One patient reported severe hypoglycaemia with dulaglutide 1.5 mg, no patient with dulaglutide 3 mg, and one patient with dulaglutide 4.5 mg.

Special populations

Use in patients with renal impairment

In a 52 week study, Trulicity 1.5 mg and 0.75 mg were compared to titrated insulin glargine as add-on to prandial insulin lispro to evaluate the effect on glycaemic control and safety of patients with moderate to severe chronic kidney disease (eGFR [by CKD-EPI] < 60 and > 15 mL/min/1.73 m2).

Patients discontinued their pre-study insulin regimen at randomisation. At baseline, overall mean eGFR was 38 mL/min/1.73 m2, 30 % of patients had eGFR < 30 mL/min/1.73 m2.

At 26 weeks, both Trulicity 1.5 mg and 0.75 mg were non-inferior to insulin glargine in lowering of HbA1c and this effect was sustained at 52 weeks. A similar percentage of patients achieved HbA1c targets of < 8.0 % at 26 and 52 weeks with both dulaglutide doses as well as insulin glargine.

Table 12. Results of a 52-week active controlled study with two doses of dulaglutide in comparison to insulin glargine (in patients with moderate to severe chronic kidney disease)

Baseline     Mean      Patients at    Change in Change in

HbA1c change in      target        FBG     body weight

HbA1c     HbA1c

(%)       (%)     < 8.0 % (%) (mmol/L)      (kg)

26 weeks

Dulaglutide 1.5 mg once weekly (n = 192)

8.60

–1.19f

78.3

1.28##

–2.81##

Dulaglutide 0.75 mg once weekly (n = 190)

8.58

–1.12f

72.6

0.98##

–2.02##

Insulin glargine+ once daily (n = 194)

8.56

–1.13

75.3

–1.06

1.11

52 weeks

Dulaglutide 1.5 mg once weekly (n = 192)

8.60

–1.10t

69.1

1.57##

–2.66##

Dulaglutide 0.75 mg once weekly (n = 190)

8.58

–1.10t

69.5

1.15##

–1.71##

Insulin glargine+ once daily (n = 194)

8.56

–1.00

70.3

–0.35

1.57

^ 1-sided p-value < 0.025, for non-inferiority of dulaglutide to insu

in glargine

  • ## p < 0.001 dulaglutide treatment group compared to insulin glargine

  • + Insulin glargine doses were adjusted utilizing an algorithm with a fasting plasma glucose target of < 8.3 mmol/L

5.2 Pharmacokinetic properties

Absorption

Following subcutaneous administration to patients with type 2 diabetes, dulaglutide reaches peak plasma concentrations in 48 hours. The mean peak (Cmax) and total (AUC) exposures were approximately 114 ng/ml and 14,000 ngh/ml, respectively, after multiple subcutaneous 1.5 mg doses of dulaglutide in patients with type 2 diabetes. Steady-state plasma concentrations were achieved between 2 to 4 weeks of once-weekly administration of dulaglutide (1.5 mg). Exposures after subcutaneous administration of single dulaglutide (1.5 mg) doses in the abdomen, thigh, or upper arm were comparable. The mean absolute bioavailability of dulaglutide following single-dose subcutaneous administration of single 1.5 mg and 0.75 mg doses was 47 % and 65 %, respectively.

Absolute bioavailabilities for 3 mg and 4.5 mg doses were estimated to be similar to 1.5 mg although they have not been specifically studied. Over the dose range 0.75 mg to 4.5 mg, the increase in dulaglutide concentration is approximately proportional.

Distribution

The apparent population mean central volume of distribution was 3.09 L and the apparent population mean peripheral volume of distribution was 5.98 L.

Biotransformation

Dulaglutide is presumed to be degraded into its component amino acids by general protein catabolism pathways.

Elimination

Apparent population mean clearance of dulaglutide was 0.142 L/h. and the elimination half-life was approximately 5 days.

Special populations

Elderly

Age had no clinically relevant effect on the pharmacokinetic and pharmacodynamic properties of dulaglutide.

Gender and race

Gender and race had no clinically meaningful effect on the pharmacokinetics of dulaglutide.

Body weight or body mass index

Pharmacokinetic analyses have demonstrated a statistically significant inverse relationship between body weight or body mass index (BMI) and dulaglutide exposure, although there was no clinically relevant impact of weight or BMI on glycaemic control.

Renal impairment

The pharmacokinetics of dulaglutide were evaluated in a clinical pharmacology study and were generally similar between healthy subjects and patients with mild to severe renal impairment (CrCl < 30 ml/min), including end stage renal disease (requiring dialysis). Additionally, in a 52 week clinical study in patients with type 2 diabetes and moderate to severe renal impairment (eGFR [by CKD-EPI] < 60 and > 15 mL/min/1.73 m2), the pharmacokinetic profile of Trulicity 0.75 mg and 1.5 mg once weekly was similar to that demonstrated in previous clinical studies. This clinical study did not include patients with end stage renal disease.

Hepatic impairment

The pharmacokinetics of dulaglutide were evaluated in a clinical pharmacology study, where subjects with hepatic impairment had statistically significant decreases in dulaglutide exposure of up to 30 % to 33 % for mean Cmax and AUC, respectively, compared to healthy controls. There was a general increase in tmax of dulaglutide with increased hepatic impairment. However, no trend in dulaglutide exposure was observed relative to the degree of hepatic impairment. These effects were not considered to be clinically relevant.

Paediatric population

Studies characterising the pharmacokinetics of dulaglutide in paediatric patients have not been performed.

5.3 Preclinical safety data

Non-clinical data reveal no special hazards for humans based on conventional studies of safety pharmacology or repeat-dose toxicity.

In a 6 month carcinogenicity study in transgenic mice, there was no tumorigenic response. In a 2 year carcinogenicity study in rats, at > 3 times the human clinical exposure following 4.5 mg dulaglutide per week, dulaglutide caused statistically significant, dose-related increases in the incidence of thyroid C-cell tumours (adenomas and carcinomas combined). The clinical relevance of these findings is currently unknown.

During the fertility studies, a reduction in the number of corpora lutea and prolonged oestrous cycle were observed at dose levels that were associated with decreased food intake and body weight gain in maternal animals; however, no effects on indices of fertility and conception or embryonic development were observed. In reproductive toxicology studies, skeletal effects and a reduction in foetal growth were observed in the rat and rabbit at exposures of dulaglutide 5– to 18-fold higher than those proposed clinically, but no foetal malformations were observed. Treatment of rats throughout pregnancy and lactation produced memory deficits in female offspring at exposures that were 7-fold higher than those proposed clinically. Dulaglutide dosing of male and female juvenile rats did not produce memory deficits at 38-fold the highest human exposure.

6. PHARMACEUTICAL PARTICULARS6.1 List of excipients

Sodium citrate

Citric acid

Mannitol

Polysorbate 80

Water for injections

6.2 Incompatibilities

In the absence of compatibility studies this medicinal product must not be mixed with other medicinal products.

6.3 Shelf life

2 years

6.4 Special precautions for storage

Store in a refrigerator (2 °C – 8 °C).

Do not freeze.

Store in original package in order to protect from light.

In-use

Trulicity may be stored unrefrigerated for up to 14 days at a temperature not above 30 °C.

6.5 Nature and contents of container

Glass syringe (type I) encased in a disposable pen.

Each pre-filled pen contains 0.5 ml of solution.

Packs of 2 and 4 pre-filled pens and multipack of 12 (3 packs of 4) pre-filled pens. Not all pack sizes may be marketed.

6.6 Special precautions for disposal and other handling

Any unused medicinal product or waste material should be disposed of in accordance with local requirements.

Instructions for use

The pre-filled pen is for single-use only.

The instructions for using the pen, included with the package leaflet, must be followed carefully. Trulicity should not be used if particles appear or if the solution is cloudy and/or discoloured. Trulicity that has been frozen must not be used.

7. MARKETING AUTHORISATION HOLDER

Eli Lilly Nederland B.V., Papendorpseweg 83, 3528 BJ Utrecht, The Netherlands.

8. MARKETING AUTHORISATION NUMBER

EU/1/14/956/001

EU/1/14/956/002

EU/1/14/956/003

EU/1/14/956/006

EU/1/14/956/007

EU/1/14/956/008

EU/1/14/956/011

EU/1/14/956/012

EU/1/14/956/013

EU/1/14/956/014

EU/1/14/956/015

EU/1/14/956/016

9. DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION

Date of first authorisation: 21 November 2014

Date of latest renewal: 23 August 2019