Benefit–Risk Assessment of Galcanezumab Versus Placebo for the Treatment of Episodic and Chronic Migraine Using the Metrics of Number Needed to Treat and Number Needed to Harm

Leslie Citrome; Margarita Sánchez del Rio; Yan Dong; Russell M Nichols; Antje Tockhorn-Heidenreich; Shonda A Foster; Virginia L Stauffer

doi:10.1007/s12325-021-01848-x

. 2021 Jul 15;38(8):4442–4460. doi: 10.1007/s12325-021-01848-x

Benefit–Risk Assessment of Galcanezumab Versus Placebo for the Treatment of Episodic and Chronic Migraine Using the Metrics of Number Needed to Treat and Number Needed to Harm

Leslie Citrome ¹, Margarita Sánchez del Rio ², Yan Dong ³, Russell M Nichols ³, Antje Tockhorn-Heidenreich ⁴, Shonda A Foster ³, Virginia L Stauffer ^3,^✉

PMCID: PMC8342379 PMID: 34264500

Abstract

Introduction

Subcutaneous galcanezumab was an effective, well-tolerated preventive treatment for adults with episodic (EM) or chronic migraine (CM) in 4 phase 3 randomized controlled trials: EVOLVE-1, EVOLVE-2, REGAIN, and CONQUER. Number needed to treat (NNT) and to harm (NNH) are metrics of effect size used to evaluate benefit–risk profiles. This study evaluated NNT, NNH, and benefit–risk profiles (measured as likelihood to be helped or harmed, LHH) of galcanezumab 120 mg versus placebo in patients with EM or CM.

Methods

Primary efficacy outcomes were responses defined as ≥ 30%, ≥ 50%, and ≥ 75% reductions from baseline in number of monthly migraine headache days in patients with EM (EVOLVE-1; EVOLVE-2; CONQUER) and CM (REGAIN; CONQUER); corresponding NNTs to achieve respective responses; and corresponding NNHs for discontinuations due to adverse events (DCAEs) among the safety population. Secondary efficacy outcomes were responses for patients with ≥ 2 failed prior preventive treatments due to lack of efficacy and/or for tolerability reasons. All LHHs were based on ≥ 50% response and DCAEs.

Results

During double-blind treatment periods with galcanezumab 120 mg, NNT to achieve ≥ 30% and ≥ 50% responses ranged from 4 to 10 and NNT to achieve ≥ 75% responses ranged from 5 to 23 in individual trials. NNH ranged from 93 to 1000, while LHH ranged from 18.6 to 104.6. NNTs were generally more robust among patients with EM than with CM; however, in patients with failure of ≥ 2 prior preventive treatments, NNTs to achieve ≥ 30% and ≥ 50% responses were similar between patients with CM and EM. NNHs were imputed as 1000 for both migraine types. Resulting LHHs were 178.8 (EM) and 127 (CM).

Conclusion

Across 4 trials, galcanezumab 120 mg demonstrated a favorable benefit–risk profile versus placebo, based on low NNTs to achieve response and high NNHs associated with DCAEs. LHH values consistently far exceeded 1.

Trial Registration Numbers

EVOLVE-1: ClinicalTrials.gov identifier, NCT02614183; EVOLVE-2: ClinicalTrials.gov identifier, NCT02614196; REGAIN: ClinicalTrials.gov identifier, NCT02614261; CONQUER: ClinicalTrials.gov identifier, NCT03559257.

Supplementary Information

The online version contains supplementary material available at 10.1007/s12325-021-01848-x.

Keywords: Benefit–risk profile, Chronic migraine, Effect size, Galcanezumab, Episodic migraine, Likelihood of help versus harm, Number needed to treat, Number needed to harm

Key Summary Points

Why carry out this study?

Migraine carries a high disease burden, and, although analgesic use for acute treatment of migraine is common, not all patients who might benefit from preventive therapy receive it.

Number needed to treat (NNT) and number needed to harm (NNH) are metrics of effect size that can be used to evaluate benefit–risk profiles and may help guide clinical decision-making.

This study evaluated the benefit–risk profile of galcanezumab using number needed to treat (NNT), number needed to harm (NNH), and likelihood to be helped or harmed (LHH), as calculated from the phase 3 clinical trial program.

What was learned from the study?

Across 4 trials, galcanezumab treatment demonstrated robust NNTs versus placebo to achieve response and favorable NNHs versus placebo associated with discontinuations due to adverse events; in combination, these findings suggest galcanezumab is an effective preventive treatment for both chronic and episodic migraine with an excellent safety profile, where the benefits outweigh the possible risks associated with the drug.

More robust NNTs for galcanezumab versus placebo were observed for patients with episodic migraine (EM) than with chronic migraine (CM) overall; however, in patients with failure of ≥ 2 prior preventive treatments, the NNTs versus placebo to achieve ≥ 30% and ≥ 50% response were similar between patients with EM and those with CM.

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Introduction

Advances have recently been made regarding specific interventions to migraine prophylaxis which may carry efficacy and tolerability advantages over older approaches. Quantifying the benefit–risk can be challenging, particularly for novel mechanisms of action that may be unfamiliar to many practitioners. One such therapeutic target implicated in the pathogenesis of migraine is the calcitonin gene-receptor peptide (CGRP) [1]. Serum levels of CGRP are elevated during a migraine attack [2, 3]. Galcanezumab is a humanized monoclonal antibody that binds to CGRP ligand and blocks its binding to the receptor.

Initially, phase 2 studies of galcanezumab were conducted in patients with episodic migraine (EM) to establish proof of concept and dose finding. Preliminary efficacy results from the proof-of-concept study (vs. placebo, a significant mean change from baseline in the frequency of migraine headache days per 28-day period when assessed at 9–12 weeks) supported the likelihood of a role for CGRP in the pathogenesis of migraine, as well as support for more in-depth study of galcanezumab [4]. A later phase 2b dose-finding study established that the once-monthly administration of 120 mg galcanezumab significantly reduced the number of migraine headache days compared with placebo in patients with a history of migraine who completed treatment, with good tolerability and without any emergent safety issues [5].

Phase 3, double-blind, placebo-controlled studies have shown that the CGRP monoclonal antibodies approved in the United States and other countries (erenumab [6–8], fremanezumab [9, 10], galcanezumab [11–13], and eptinezumab [14, 15]) are efficacious in decreasing the frequency of monthly migraine headache days. Galcanezumab administered via subcutaneous injection (a single 240-mg loading dose, followed by 120-mg monthly doses) has been effective and well tolerated for the preventive treatment of EM and chronic migraine (CM) in 4 phase 3 studies: EVOLVE-1 (NCT02614183), EVOLVE-2 (NCT02614196), REGAIN (NCT02614261), and CONQUER (phase 3b, NCT03559257) [16–19]. In all 4 studies, the most common treatment-emergent adverse events (AEs) included injection site-related AEs (pain, erythema, pruritus, or swelling at the injection site), nasopharyngitis, sinusitis, upper respiratory tract infection, and influenza.

The objective of this study was to evaluate the benefit–risk profile of galcanezumab using number needed to treat (NNT), number needed to harm (NNH), and likelihood to be helped or harmed (LHH) [20, 21], as calculated from the phase 3 clinical trial program.

Methods

Data Sources

EVOLVE-1, EVOLVE-2, REGAIN, and CONQUER were 4 phase 3, multicenter, randomized, double-blind, placebo-controlled studies of adult patients with migraine [16–19]. The EM studies (EVOLVE-1 [19] and EVOLVE-2 [18]) examined whether galcanezumab 120 mg or 240 mg per month was superior to placebo in the preventive treatment of EM. In the CM study, REGAIN [16], galcanezumab was examined at doses of 120 mg per month or 240 mg per month, to see if it was superior to placebo in the preventive treatment of CM. The CONQUER study [17] examined whether galcanezumab 120 mg was superior to placebo in patients with treatment-resistant EM or CM. Additional details related to these clinical trials are provided in the published manuscripts for these trials [16–19]. Key study design characteristics and results from all 4 studies are summarized in Table 1. The primary outcome of all 4 studies was the overall mean change from baseline in the number of monthly migraine headache days during the double-blind treatment period (6 months for EVOLVE-1 and -2, and 3 months for REGAIN and CONQUER).

Table 1.

Summary of EVOLVE-1, EVOLVE-2, REGAIN, and CONQUER trials

Study title and identifiers	EM or CM	Key design characteristics	Primary outcome	Summary of results
A Phase 3, Randomized, Double-blind, Placebo-controlled Study of LY2951742 in Patients with EM (EVOLVE-1) NCT02614183 [19]	EM	Adults aged 18–65 years with at least a 1-year history of migraine. Patients received subcutaneous injection treatments once monthly for 6 months and were followed-up for 5 months after last injection. Patients were randomized 2:1:1 to receive placebo or monthly subcutaneous galcanezumab 120 mg or galcanezumab 240 mg	Overall mean change from baseline in the number of monthly migraine headache days during the treatment period	Enrolled: 862 Study start date: 11/2015 Study completion date: 3/2017 Primary outcome met for both galcanezumab doses (p < 0.001) Treatment with galcanezumab significantly reduced monthly migraine headache days (both p < 0.001) by 4.7 days (120 mg) and 4.6 days (240 mg) compared with placebo (2.8 days). All key secondary measures (reduction in monthly migraine headache days, migraine headache days with acute medication use, and scores from the Migraine-Specific Quality of Life questionnaire, Patient Global Impression of Severity, MIDAS) were also significant after multiplicity adjustment. There were no meaningful differences between 120-mg and 240-mg doses of galcanezumab on measures of efficacy
A Phase 3, Randomized, Double-Blind, Placebo-Controlled Study of LY2951742 in Patients With EM (EVOLVE-2) NCT02614196 [18]	EM	Adults aged 18–65 years with a diagnosis of migraine with or without aura, and at least a 1-year history of migraine. Patients received subcutaneous injection treatments once monthly for 6 months and were followed up for 4 months after last injection. Patients were randomized 2:1:1 to receive placebo, galcanezumab 120 mg, or galcanezumab 240 mg	Overall mean change from baseline in monthly migraine headache days	Enrolled: 922 Study start date: 12/2015 Study completion date: 3/2017 Primary outcome met for both galcanezumab doses (p < 0.001) Mean monthly migraine headache days were reduced by 4.3 and 4.2 days for galcanezumab 120 and 240 mg, respectively, and 2.3 days for placebo. The group differences (95% CIs) versus placebo were 2.0 (− 2.6, − 1.5) and 1.9 (− 2.4, − 1.4), respectively. Both doses were superior to placebo for all key secondary endpoints (≥ 50%, ≥ 75%, 100% response rates; monthly migraine headache days with acute migraine medication use; Patient Global Impression of Severity rating; the Role Function-Restrictive score of the Migraine-Specific Quality of Life Questionnaire). Injection site pain was the most common treatment-emergent AE, reported at similar rates in all treatment groups. Both galcanezumab doses had significantly more injection site reactions and injection site pruritus, and the 240-mg group had significantly more injection site erythema versus placebo
A Phase 3, Randomized, Double-Blind, Placebo-Controlled Study of LY2951742 in Patients With CM (REGAIN) NCT02614261 [16]	CM	Adults aged 18–65 years, with a diagnosis of CM as defined by the International Classification of Headache Disorders, 3rd edn, beta version (ICHD-3 beta) guidelines and migraine onset before 50 years of age. Patients received subcutaneous injection treatments once monthly for 6 months (3 months double-blind, placebo-controlled treatment, and 3 months open-label treatment). Patients received subcutaneous injection treatments once monthly for 12 months (3 months double-blind, placebo-controlled treatment, and 9 months open-label treatment), and were followed up for 4 months posttreatment. Patients were randomized 2:1:1 to receive placebo, galcanezumab 120 mg, or galcanezumab 240 mg	The overall mean change from baseline in the number of monthly migraine headache days during the 3-month double-blind treatment phase	Enrolled: 1117 Study start date: 11/2015 Study completion date: 3/2017 Primary outcome met for both galcanezumab doses (p < 0.001) Mean number of monthly headache days at baseline was 19.4 for the total sample. Both galcanezumab dose groups demonstrated greater overall mean reduction in the number of monthly migraine headache days compared to placebo (placebo − 2.7, galcanezumab 120 mg − 4.8, galcanezumab 240 mg − 4.6). There were no clinically meaningful differences between galcanezumab doses and placebo on any safety or tolerability outcome except for a higher incidence of treatment-emergent injection-site reaction (p < 0.01), injection-site erythema (p < 0.001), injection-site pruritus (p < 0.01), and sinusitis (p < 0.05) in the galcanezumab 240-mg group relative to placebo
A Randomized, Double-Blind, Placebo-Controlled Study of Galcanezumab in Adults With Treatment-Resistant Migraine (CONQUER) NCT03559257 [17]	EM or CM	Adults aged 18–75 years, with EM (58%) or CM (42%), with migraine onset before the age of 50 years, who had a documented failure of preventive medications from two to four drug treatments in the past 10 years owing to lack of efficacy or tolerability, or both. Patients received subcutaneous injection treatments once monthly for 6 months (3 months double-blind, placebo-controlled treatment, and 3 months open-label treatment). Patients were randomized 1:1 to receive placebo or galcanezumab 120 mg (with a loading dose of 240 mg)	Overall mean change from baseline in number of monthly migraine headache days during the 3-month treatment period in all patients who were randomly assigned and received at least one dose of study drug	Enrolled: 462 Study start date: 7/2018 Study completion date: 6/2019 Primary outcome met for 120-mg galcanezumab dose (p < 0.0001) Galcanezumab-treated patients had significantly greater reduction in migraine headache days versus placebo across months 1–3. The galcanezumab group had on average 4·1 fewer monthly migraine headache days compared with baseline (13·4), while the placebo group had on average 1·0 fewer than at baseline (13·0; between-group difference − 3·1 [95% CI − 3·9 to − 2·3]; p < 0·0001; effect size = 0·72). Types and number of treatment-emergent AEs were similar between galcanezumab and placebo. Treatment-emergent AEs were reported in 122 (53%) of 230 patients in the placebo group and 119 (51%) of 232 patients in the galcanezumab group. There were 4 serious AEs during the study, 2 (1%) reported in the placebo group and 2 (1%) reported in the galcanezumab group

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AE adverse event, CM chronic migraine, EM episodic migraine, MIDAS Migraine Disability Assessment

The protocols for each study were reviewed and approved by the appropriate institutional or ethical review board (IRB) for each site. All studies described were conducted according to Good Clinical Practice and the Declaration of Helsinki guidelines. Patients provided written informed consent before undergoing study procedures. Adverse outcomes such as serious AEs were reported to the sponsor, IRB, and appropriate regulatory authority.

Outcome Measures

Primary efficacy outcomes for the present study were the observed ≥ 30%, ≥ 50%, and ≥ 75% response rates based on reductions from baseline in the number of monthly migraine headache days in patients with EM (EVOLVE-1, EVOLVE-2, and CONQUER) and patients with CM (REGAIN and CONQUER); estimation of corresponding NNTs to achieve ≥ 30%, ≥ 50%, and ≥ 75% response rates, respectively; and estimation of corresponding NNHs for discontinuations due to AEs among the safety population. Secondary efficacy outcomes were the estimation of ≥ 30%, ≥ 50%, and ≥ 75% response rates, as well as corresponding NNT values to achieve the respective response rates, and estimation of corresponding NNH values for discontinuations due to AEs in patients in all 4 clinical trials who had failure of ≥ 2 prior preventive treatments versus placebo due to lack of efficacy and/or for tolerability reasons. LHH was defined as the ratio of NNH to NNT and was calculated using raw (unrounded) NNT and NNH values. The patient was considered more likely to be helped than harmed if the LHH was > 1, and more likely to be harmed than helped if the LHH was < 1.

Statistical Analysis

Patients’ demographic and disease characteristics at baseline were reported using descriptive statistics. Treatment comparisons were performed using analysis of variance model for continuous parameters and Fisher’s exact test for categorical parameters at baseline.

In this post hoc analysis, NNT for efficacy outcomes, ≥ 30%, ≥ 50%, and ≥ 75% response rates, NNH for tolerability outcome, and discontinuations due to AEs were calculated for galcanezumab 120 mg and 240 mg versus placebo. The NNT or NNH is the inverse of the absolute difference in the incidence of outcomes between a given active treatment relative to placebo group. NNT and NNH were each rounded up to the next whole value. The precision around NNT and NNH was measured with 95% confidence intervals (CIs) calculated using the modified Wilson score method without continuity correction [22]. If the lower bound (LB) and upper bound (UB) of the 95% CI for the incidence difference had the same positive or negative sign (excluding 0), the 95% CI of the NNT or NNH was the inverse of the UB and LB of incidence difference. Otherwise, a 95% CI for the NNT or NNH was the union of less than 1/LB and greater than 1/UB; in other words (− ∞, − 1/LB) ∪ (1/UB, + ∞). In instances where the rate of the AE or discontinuation because of an AE was greater with placebo than with galcanezumab, resulting in a “negative” NNH, the NNH was redefined as having a value of 1000 (representing an absolute risk increase of 0.001, and with an incalculable 95% CI) when determining the LHH, as has been done in other reports of a similar nature [23].

The 95% CI for LHH was calculated using a Bayesian approach with study summary data treated as the observations and a non-informative prior. The observed number of patients that achieved a response and the number of patients that discontinued treatment due to an AE from active treatment and placebo groups were assumed to follow 4 distinct binomial distributions. The posterior distribution of the incidence rate of an outcome from different treatment groups were beta distributions. LHH, a 2.5% LB and a UB of 95% CI were estimated using Monte Carlo random sampling distributions. The 95% CIs of LHH were wide and included zero because the incidence of discontinuations due to AEs between galcanezumab doses and the placebo group were very small positive percentages and close to zero. Therefore, the LHH value was reported but the corresponding 95% CI of LHH was not presented.

In this analysis, NNT for each specific efficacy outcome and NNH for tolerability outcome, and the respective 95% CIs, were calculated for galcanezumab 120 mg versus placebo (for galcanezumab 240 mg vs. placebo, see Supplementary Material) for the individual study for the overall population. The data were also reported among patients with at least 2 prior preventive medication failures due to inadequate efficacy or safety/tolerability in 6-month pooled EVOLVE-1 and -2, 3-month REGAIN, or 3-month CONQUER, respectively. In addition, the analysis was performed for pooled EM data at month 3 for EVOLVE-1, EVOLVE-2, and CONQUER studies, as well as the pooled CM data from REGAIN and CONQUER studies. This is a post hoc exploratory analysis and no formal hypothesis comparison or test was conducted. A two-sided significance level of 0.05 was considered. Statistical analyses were conducted using SAS v.7.1 (SAS Institute, Cary, NC, USA) and R v.3.6.3.

Results

Patient Demographics and Disease Characteristics

Baseline demographics and disease characteristics were similar among patients with EM versus those with CM (Table 2). Among the most common pre-existing conditions (≥ 10% of patients in EVOLVE-1 and/or CONQUER) were hypertension, anxiety, depression, seasonal allergy, drug hypersensitivity, back pain, gastroesophageal reflux disease, insomnia, and myopia. Across all 4 studies, migraine burden measured as the number of monthly migraine headache days and disability scores measured using the Migraine Disability Assessment (MIDAS) were greater among CM patients. Patients in the REGAIN trial and patients with CM in the CONQUER trial treated with galcanezumab 120 mg had 19.4 (4.3) and 19.2 (4.7) mean (SD) monthly migraine headache days, respectively; in comparison, all patients in EVOLVE-1, all patients in EVOLVE-2, and patients with EM in CONQUER treated with galcanezumab 120 mg had 9.2 (3.1), 9.1 (2.9), and 9.5 (3.0) mean monthly migraine headache days, respectively. Mean (SD) MIDAS scores among REGAIN patients and CONQUER patients with CM treated with galcanezumab 120 mg were 62.5 (49.5) and 64.7 (56.2), respectively; in comparison, mean MIDAS scores among all patients in EVOLVE-1, all patients in EVOLVE-2, and patients with EM in CONQUER were 32.9 (28.2), 30.9 (27.9), and 41.3 (34.3), respectively.

Table 2.

Baseline demographics and disease characteristics in the individual trials

	EVOLVE-1^a		EVOLVE-2^a		REGAIN^b		CONQUER^c EM		CONQUER^c CM
	PBO (N = 433)	GMB 120 mg (N = 213)	PBO (N = 461)	GMB 120 mg (N = 231)	PBO (N = 558)	GMB 120 mg (N = 278)	PBO (N = 132)	GMB 120 mg (N = 137)	PBO (N = 98)	GMB 120 mg (N = 95)
Age, years, mean (SD)	41.3 (11.4)	40.9 (11.9)	42.3 (11.3)	40.9 (11.2)	41.6 (12.1)	39.7 (11.9)^d	46.3 (11.8)	45.9 (11.2)	44.8 (13.1)	45.8 (11.6)
Female, n (%)	362 (83.6)	181 (85.0)	393 (85.3)	197 (85.3)	483 (86.6)	237 (85.3)	117 (88.6)	112 (81.8)	85 (86.7)	83 (87.4)
Number of comorbidities, mean (SD)	4.8 (3.6)	4.7 (3.8)	3.7 (3.1)	3.6 (3.4)	4.4 (3.7)	4.1 (3.3)	4.1 (3.9)^e	4.0 (3.7)^f	4.3 (3.5)^g	4.4 (3.7)^h
Migraine illness duration, years, mean (SD)	19.9 (12.3)	21.1 (13.0)	21.2 (12.8)	19.9 (11.7)	21.9 (12.9)	20.4 (12.7)	22.9 (13.1)	21.7 (12.7)	24.9 (14.9)	24.2 (13.9)
Number of monthly migraine headache days, mean (SD)	9.1 (3.0)	9.2 (3.1)	9.2 (3.0)	9.1 (2.9)	19.6 (4.6)	19.4 (4.3)	9.2 (2.7)	9.5 (3.0)	18.1 (4.7)	19.2 (4.7)
Patients with failure of ≥ 2 prior preventive treatments, n (%)	22 (5.1)	10 (4.7)	63 (13.7)	34 (14.7)	177 (31.7)	74 (26.6)	132 (100)	137 (100)	98 (100)	95 (100)
MIDAS total score, mean (SD)	31.8 (27.3)	32.9 (28.2)	34.3 (31.0)	30.9 (27.9)	68.7 (57.4)	62.5 (49.5)	37.1 (26.2)	41.3 (34.3)	69.6 (57.9)	64.7 (56.2)

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CM chronic migraine, EM episodic migraine, GMB galcanezumab, MIDAS Migraine Disability Assessment, N number of patients in the analysis treatment group, n number of patients with each respective outcome, PBO placebo, SD standard deviation

^aIncluded patient population with EM

^bIncluded patient population with CM

^cIncluded patient population with EM (58%) and CM (42%)

^dp ≤ 0.05 versus placebo based on analysis of variance model for continuous parameters

^eN = 95

^fN = 108

^gN = 92

^hN = 84

A greater proportion of patients in REGAIN (CM) than patients in EVOLVE-1 and -2 (EM) also had treatment failure of ≥ 2 prior preventive treatments (Table 2). In CONQUER, the entire patient population had treatment failure of ≥ 2 prior preventive treatments, 78% of which were due to inadequate or no response.

Primary Analysis

Over the durations of the 4 trials (months 1–6 for EVOLVE-1/-2 and months 1–3 for REGAIN and CONQUER), significantly higher percentages of patients treated with galcanezumab 120 mg achieved ≥ 30%, ≥ 50%, and ≥ 75% responses versus patients who received placebo [16–19].

The NNTs to achieve responses during the double-blind treatment periods with galcanezumab 120 mg were generally robust (i.e., low values) in the individual trials (Table 3). NNT (95% CI) values at month 6 in EVOLVE-1 and -2 ranged from 5 (4, 7) to 8 (5, 18). In REGAIN, NNTs to achieve ≥ 30% and ≥ 50% response at month 3 were 8 (5, 20) and 10 (6, 30), respectively; however, the NNT value to achieve ≥ 75% response at month 3 was 23 (− ∞, − 134) ∪ (12, + ∞). In CONQUER, NNTs to achieve ≥ 30%, ≥ 50%, and ≥ 75% responses at month 3 were 4 (3, 5), 5 (4, 8), and 12 (8, 38), respectively, for the overall study population (Table 3).

Table 3.

The NNTs to achieve ≥ 30%, ≥ 50%, and ≥ 75% response rates and the NNHs for discontinuations due to aes in the individual trials

Outcome	GMB 120 mg			PBO			NNT or NNH (95%CI) vs PBO
	n	N	%	n	N	%
EVOLVE-1,^a Month 6
Efficacy							NNT
≥ 30% response rate	143	177	80.8%	226	342	66.1%	7 (5, 14)
≥ 50% response rate	119	177	67.2%	161	342	47.1%	5 (4, 9)
≥ 75% response rate	87	177	49.2%	88	342	25.7%	5 (4, 7)
Tolerability							NNH
Discontinuations due to AEs, all patients	7	206	3.4%	10	432	2.3%	93 (–∞, –67) $\cup$ (22, + ∞)
EVOLVE-2,^a Month 6
Efficacy							NNT
≥ 30% response rate	155	196	79.1%	220	382	57.6%	5 (4, 7)
≥ 50% response rate	127	196	64.8%	163	382	42.7%	5 (4, 8)
≥ 75% response rate	76	196	38.8%	95	382	24.9%	8 (5, 18)
Tolerability							NNH
Discontinuations due to AEs, all patients	5	226	2.2%	8	461	1.7%	210 (–∞, –62) $\cup$ (29, + ∞)
REGAIN,^b Month 3
Efficacy							NNT
≥ 30% response rate	136	256	53.1%	202	498	40.6%	8 (5, 20)
≥ 50% response rate	90	256	35.2%	123	498	24.7%	10 (6, 30)
≥ 75% response rate	34	256	13.3%	44	498	8.8%	23 (–∞, –134) $\cup$ (12, + ∞)
Tolerability							NNH
Discontinuations due to AEs, all patients	1	273	0.4%	6	558	1.1%	1000 (NE, NE)
CONQUER,^c Month 3
Efficacy							NNT
≥ 30% response rate	136	224	60.7%	72	224	32.1%	4 (3, 5)
≥ 50% response rate	87	224	38.8%	39	224	17.4%	5 (4, 8)
≥ 75% response rate	33	224	14.7%	14	224	6.3%	12 (8, 38)
Tolerability							NNH
Discontinuations due to AEs, all patients	1	232	0.4%	0	230	0%	232 (–∞, –80) $\cup$ (42, + ∞)

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AE adverse event, CI confidence intervals, CM chronic migraine, EM episodic migraine, GMB galcanezumab, N number of patients in the analysis treatment group, n number of patients with each respective outcome, NE not evaluable, NNH number needed to harm, NNT number needed to treat, PBO placebo

^aIncluded patient population with EM; based on data from Month 6

^bIncluded patients with CM; based on data from Month 3

^cIncluded patient population with EM (58%) and CM (42%); based on data from Month 3

NNH values based on discontinuations due to AEs were high for galcanezumab 120 mg across all 4 trials (Table 3). The NNH (95% CI) values in EVOLVE-1 and EVOLVE-2 (patients with EM) were 93 (− ∞, − 67) ∪ (22, + ∞) and 210 (− ∞, − 62) ∪ (29, + ∞), respectively. In REGAIN (patients with CM), the NNH was 1000 (not evaluable [NE], NE). The overall NNH for CONQUER was 232 (− ∞, − 80) ∪ (42, + ∞) (Table 3).

All LHH values presented were based on ≥ 50% response and discontinuations due to AEs. The LHH values for patients treated with galcanezumab 120 mg were as follows: EVOLVE-1: 18.6; EVOLVE-2: 46.4; REGAIN: 104.6; and CONQUER: 49.7.

Secondary Analysis

In all 4 trials, responses were achieved among galcanezumab-treated patients with failures of ≥ 2 prior treatments due to lack of efficacy or tolerability. Over the duration of each trial, greater percentages of galcanezumab-treated patients achieved ≥ 30%, ≥ 50%, and ≥ 75% responses versus patients who received placebo (Table 4). Additionally, higher percentages of patients with EM (EVOLVE-1 and -2 pooled; CONQUER EM) than with CM (REGAIN; CONQUER CM) achieved ≥ 30%, ≥ 50%, and ≥ 75% responses (Table 5).

Table 4.

The NNTs to achieve ≥ 30%, ≥ 50%, and ≥ 75% response rates in patients with failure of ≥ 2 prior preventive treatments due to lack of efficacy and/or tolerability

Outcome	GMB 120 mg			PBO			NNT or NNH (95%CI) vs PBO
	n	N	%	n	N	%
Pooled EVOLVE-1 and EVOLVE-2,^a month 6
Efficacy							NNT
≥ 30% response rate	31	49	63.3%	32	75	42.7%	5 (3, 22)
≥ 50% response rate	28	49	57.1%	20	75	26.7%	4 (3, 7)
≥ 75% response rate	18	49	36.7%	8	75	10.7%	4 (3, 9)
TOLERABILITY							NNH
DCAE, all patients	0	51	0%	1	92	0.01%	1000 (NE, NE)
REGAIN,^b month 3
Efficacy							NNT
≥ 30% response rate	32	69	46.4%	40	167	24.0%	5 (3, 11)
≥ 50% response rate	21	69	30.4%	24	167	14.4%	7 (4, 29)
≥ 75% response rate	6	69	8.7%	5	167	3.0%	18 (–∞, –28) $\cup$ (9, + ∞)
Tolerability							NNH
DCAE, all patients	0	73	0%	2	177	1.1%	1000 (NE, NE)
CONQUER EM,^a month 3
Efficacy							NNT
≥ 30% response rate	85	136	62.5%	45	129	34.9%	4 (3, 6)
≥ 50% response rate	55	136	40.4%	27	129	20.9%	6 (4, 11)
≥ 75% response rate	22	136	16.2%	12	129	9.3%	15 (–∞, –81) $\cup$ (7, + ∞)
Tolerability							NNH
DCAE, all patients	0	137	0%	0	132	0%	NE
CONQUER CM,^b month 3
Efficacy							NNT
≥ 30% response rate	51	88	58.0%	27	95	28.4%	4 (3, 6)
≥ 50% response rate	32	88	36.4%	12	95	12.6%	5 (3, 9)
≥ 75% response rate	11	88	12.5%	2	95	2.1%	10 (6, 58)
Tolerability							NNH
DCAE, all patients	1	95	1.1%	0	98	0%	95 (–∞, –35) $\cup$ (18, + ∞)

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CI confidence intervals, CM chronic migraine, DCAEs discontinuations due to adverse events, EM episodic migraine, GMB galcanezumab, N number of patients in the analysis treatment group, n number of patients with each respective outcome, NE not evaluable, NNH number needed to harm, NNT number needed to treat, PBO placebo

^aIncluded patients with EM

^bIncluded patients with CM

Table 5.

The NNTs to achieve ≥ 30%, ≥ 50%, and ≥ 75% response in migraine headache days and the NNHs for DCAEs from pooled 3-month data from patients with episodic migraine (From EVOLVE-1/-2 and CONQUER) and chronic migraine (From REGAIN and CONQUER)

Outcome	GMB 120 mg			PBO			NNT or NNH (95%CI) vs PBO
Outcome	n	N	%	n	N	%	NNT or NNH (95%CI) vs PBO
Episodic migraine: pooled EVOLVE-1, EVOLVE-2 and CONQUER EM, month 3
Efficacy							NNT
≥ 30% response rate	370	543	68.1%	465	912	51.0%	6 (5, 9)
≥ 50% response rate	290	543	53.4%	324	912	35.5%	6 (5, 8)
≥ 75% response rate	160	543	29.5	168	912	18.4	10 (7, 16)
Tolerability							NNH
DCAE, all patients	7	569	1.2%	14	1025	1.4%	1000 (NE, NE)
Chronic migraine: pooled REGAIN and CONQUER CM, month 3
EFFICACY							NNT
≥ 30% response rate	187	344	54.4%	229	593	38.6%	7 (5, 11)
≥ 50% response rate	122	344	35.5%	135	593	22.8%	8 (6, 16)
≥ 75% response rate	45	344	13.1%	46	593	7.8%	19 (11, 109)
Tolerability							NNH
DCAE, all patients	2	368	0.5%	6	656	0.9%	1000 (NE, NE)

Open in a new tab

Effect Sizes Among Patients with Failure of ≥ 2 Prior Preventive Treatments due to Reasons of Efficacy and/or Tolerability

A subgroup analysis of patients who had experienced failure of ≥ 2 prior preventive treatments due to reasons of efficacy and/or tolerability was conducted; this analysis focused on subgroups of the patient populations in EVOLVE-1 and -2 and REGAIN, while still including the entire patient population from CONQUER. Similarities in NNT values were noted between patients with EM versus CM. In the 2 pooled EVOLVE trials (EM patients), NNT values for galcanezumab 120 mg to achieve ≥ 30%, ≥ 50%, and ≥ 75% responses ranged from 4 (3, 7) to 5 (3, 22) (Table 4). NNT values for galcanezumab 120 mg to achieve ≥ 30% and ≥ 50% responses were similarly low for patients with EM from the CONQUER trial; however, the NNT value for galcanezumab 120 mg to achieve ≥ 75% response in CONQUER was 15 (− ∞, − 81) ∪ (7, + ∞). Among patients with CM treated with galcanezumab 120 mg in REGAIN and CONQUER, NNT values were generally low and the values to achieve each level of response were similar, although they were higher for the ≥ 75% response in each trial than for the ≥ 30% and ≥ 50% responses (Table 4). When patients in CONQUER were stratified by migraine type, NNT values to achieve ≥ 30% and ≥ 50% responses at month 3 were 4 (3, 6) and 6 (4, 11), respectively, for patients with EM and 4 (3, 6) and 5 (3, 9), respectively, for patients with CM; NNT values to achieve ≥ 75% response were 15 (− ∞, − 81) ∪ (7, + ∞) and 10 (6, 58) for patients with EM and CM, respectively (Table 4).

In both pooled EVOLVE-1 and -2 (patients with EM, month 6) and REGAIN (patients with CM, month 3), NNH values based on ≥ 50% response and discontinuations due to AEs were imputed as 1000 (NE, NE) for each, suggesting galcanezumab 120 mg is highly tolerable for patients with either migraine type. These findings were further supported by the results of the subanalysis of patients in CONQUER (all patients with EM or CM who had failure of ≥ 2 prior preventive treatments) at month 3: NNH was not evaluable for patients with EM, and was 95 (− ∞, − 35) ∪ (18, + ∞) in patients with CM (Table 4). Based on ≥ 50% responses and discontinuations due to AEs, these findings resulted in overall LHH values of 304.8 in EVOLVE-1 and -2 pooled, 160.6 in REGAIN, and 49.7 in CONQUER.

3-Month Data from all 4 Trials Stratified by Migraine Type (EM vs CM)

Overall NNTs for all tested response groups were relatively low for all migraine patients; however, they were generally higher among patients with CM than among those with EM (Table 5). NNTs to achieve ≥ 75% response were greatest for patients with each migraine type (EM: 10 [7, 16]; CM: 19 [11, 109]). NNH values based on ≥ 50% response and discontinuations due to AEs were similarly high for both migraine types, and were imputed as 1000 (NE, NE) for each. Based on ≥ 50% response and discontinuations due to AEs, these findings resulted in overall LHH values of 178.8 for patients with EM and 127 for patients with CM.

Pooled 6-Month Data for EVOLVE-1 and EVOLVE-2

In the pooled EVOLVE-1 and EVOLVE-2 trials, the NNT (95% CI) value for galcanezumab 120 mg to achieve ≥ 50% response at month 6 was 4 (3, 7), and the NNH (95% CI) value was imputed as 1000 (NE, NE) (Table 4). Based on ≥ 50% response and discontinuations due to AEs, these findings resulted in an overall LHH value of 304.8 across the 2 pooled trials at month 6.

Discussion

This analysis adds support to ongoing assertions that NNT and NNH can be used to evaluate benefit–risk profiles and help guide clinical decision-making across a variety of specialty areas and scenarios [24–29]. Although NNT and NNH estimates are calculated by comparing groups, ultimately the information is applied when treating individuals, including the communication of benefits and risks [30]. The philosophy of evidence-based medicine/practice is to integrate clinical data/judgment with relevant scientific evidence and the patient's own individual values and preferences [31]. NNT and NNH can inform the clinician about the propensity for an agent to have a large or small effect size on the outcome of interest, but it cannot be taken out of context, such as patient baseline, patient history, and patient preference.

Across all 4 trials, galcanezumab demonstrated a favorable benefit–risk profile compared with placebo, as assessed by low NNT values to achieve responses and high NNH values associated with discontinuations due to AEs, and thus LHH values far exceeding 1. Overall, more robust (i.e., lower) NNT values were observed for patients with EM (all patients in EVOLVE-1 and -2 and patients with EM in CONQUER) than for those with CM (all patients in REGAIN and patients with CM in CONQUER). NNT values to achieve ≥ 30% and ≥ 50% responses in patients with failure of ≥ 2 prior preventive treatments were similar between patients with CM and EM for the galcanezumab 120-mg dose group. Although the single discontinuation due to an AE in CONQUER precluded the calculation of meaningful NNH (and therefore LHH) values when patients were stratified by migraine type, the low NNT values and the low number of discontinuations due to AEs observed in CONQUER do support positive benefit–risk profiles for both migraine types.

The variation among NNT values may have been due to differences in disease burden at baseline (i.e., migraine headache days), and differences among both NNT and NNH values may have been due to the shorter treatment duration associated with patients with CM versus those with EM (i.e., 3 vs. 6 months). In addition, the percentages of patients who discontinued trials due to AEs were not significantly higher for galcanezumab versus placebo in any of the 4 trials, which makes the difference in NNH estimates highly variable.

LHH values based on ≥ 50% response and discontinuations due to AEs ranged from 18.6 to 104.6 across all individual studies. The highest LHH value for galcanezumab 120 mg was observed in REGAIN, a potential artifact of the shorter double-blind study period (3 vs. 6 months in EVOLVE-1 and -2).

A benefit–risk assessment of several current preventive treatments for migraine (erenumab, topiramate, onabotulinumtoxinA, and propranolol) found that each of these four drugs were more likely to help than harm migraine patients, and the benefit–risk profile for erenumab was orders of magnitude more positive than those calculated for topiramate, onabotulinumtoxinA, and propranolol [23]. The differences observed in LHH between erenumab and topiramate, onabotulinumtoxinA, and propranolol were primarily supported by large differences in NNH; in other words, the tolerability of erenumab appeared to be better than the tolerability of topiramate, onabotulinumtoxin A, and propranolol [23, reviewed in 32].

Drellia et al. recently conducted an LHH analysis of anti-CGRP antibodies and frequently used preventives for migraine [33]. Because there are no head-to-head comparisons with established treatments, their analysis helps to compare the absolute differences in benefit–risk ratios between drugs. Anti-CGRP antibodies at all tested doses had higher LHH values than propranolol or topiramate for EM prevention and onabotulinumtoxinA or topiramate for CM prevention [33]. These findings predict patient satisfaction and a better adherence profile for anti-CGRP antibodies. The results we describe here are in line with the findings of Drellia et al. regarding the NNT and NNH to achieve ≥ 50% response (≥ 50% reduction in migraine headache days) and the resulting LHH of galcanezumab in EVOLVE-1/2 and REGAIN [33], and we build on those findings by also evaluating pooled EVOLVE-1/-2 results, CONQUER results stratified by migraine type (EM vs. CM), and pooled 3-month results from all 4 galcanezumab studies stratified by migraine type. In addition, we have included analogous calculations for the NNT values to achieve ≥ 30% and ≥ 75% responses, and found that the NNTs required to achieve all tested response levels were similarly low, with the notable exception of the NNT to achieve ≥ 75% response in REGAIN (patients with CM; NNT = 23).

Limitations

NNT and NNH values are subject to limitations. Values can vary with baseline risk, length of treatment, response threshold definitions, and length of follow-up. In addition, regarding NNH, if the treatment arm has a lower rate of discontinuation than the placebo arm, it yields a negative absolute risk reduction, and hence results in a difficult to interpret “negative” NNH value; arbitrarily assigning an NNH value of 1000 under these circumstances is a workaround in order to estimate the LHH. Moreover, for small event rate differences, 95% CI values generally span infinity, and thus inherently the NNH estimate would be imprecise. Because of these limitations, NNT and NNH values (and the LHH values calculated from them) should be interpreted with caution, particularly across trials and interventions. In the absence of direct head-to-head studies, no definitive conclusions regarding one treatment being better than another should be drawn from reports of NNT and NNH values across various studies. Analyses are post hoc. Due to the nature of NNT/NNH analysis, the data analyzed in this study are limited to dichotomous outcomes. The results may not be generalizable to patients outside the confines of a clinical trial; this is always a concern for results of randomized controlled trials because of the strict inclusion/exclusion criteria that these studies require. Reasons for clinical trial discontinuation can be complex, so the NNH for discontinuations due to AEs in the study may not always generalize to overall tolerability in clinical practice. The brief durations of the available controlled studies limit the sensitivity of calculating NNH for delayed adverse outcomes beyond 3–6 months, and the relatively small sample sizes of the studies limit sensitivity of calculating NNH for uncommon adverse outcomes and sub-population effects.

Conclusions

Across 4 trials, in comparison to placebo galcanezumab showed robust NNTs to achieve response rates and favorable NNHs associated with discontinuations due to AEs. These findings suggest galcanezumab is associated with an advantageous benefit–risk profile. In patients with failure of ≥ 2 prior preventive treatments, the NNTs to achieve ≥ 30% and ≥ 50% response rates were similar between patients with CM (REGAIN and CONQUER CM) and those with EM (EVOLVE-1/2 and CONQUER EM) who received a single loading dose of 240 mg galcanezumab followed by 120 mg monthly thereafter (Table 4). More robust (i.e., lower) NNTs were observed for patients with EM (EVOLVE-1/2 and CONQUER EM) than for those with CM (REGAIN and CONQUER CM) (Table 5). The percentages of discontinuations due to AEs were not statistically significantly higher for galcanezumab versus placebo in the EVOLVE-1/2, REGAIN, and CONQUER trials.

Therefore, this analysis shows galcanezumab is an effective preventive treatment for both chronic and episodic migraine with an excellent safety profile, where the benefits outweigh the possible risks associated with the drug.

Supplementary Information

Below is the link to the electronic supplementary material.

Supplementary file1 (DOCX 53 kb)^{(53.9KB, docx)}

Acknowledgements

We thank the patients, their families, the study sites, and the study personnel who participated in these clinical trials.

Funding

This study and the journal’s Rapid Service and Open Access Fees were funded by Eli Lilly and Company, Indianapolis, IN, USA. The authors received no financial support for the research, authorship, and/or publication of this article.

Medical Writing, Editorial, and Other Assistance

Medical writing support was provided by Regina E. Burris, PhD, and editorial support was provided by Antonia Baldo, both of Syneos Health. Medical writing and editorial support were funded by Eli Lilly and Company, Indianapolis, IN, USA in accordance with Good Publication Practice (GPP3) guidelines (http://www.ismpp.org/gpp3).

Authorship

All named authors meet the International Committee of Medical Journal Editors (ICMJE) criteria for authorship for this article, take responsibility for the integrity of the work as a whole, and have given their approval for this version to be published.

Authors’ Contributions

Leslie Citrome: Study concept and design, analysis and interpretation of data, drafting of manuscript, critical revision of manuscript for important intellectual content. Margarita Sánchez del Rio: Analysis and interpretation of data, critical revision of manuscript for important intellectual content. Yan Dong: Study concept, analysis and interpretation of data, critical revision of manuscript for important intellectual content. Russell M. Nichols: Interpretation of data, critical revision of manuscript for important intellectual content. Antje Tockhorn-Heidenreich: Interpretation of data, critical revision of manuscript for important intellectual content. Shonda A. Foster: Interpretation of data, critical revision of manuscript for important intellectual content. Virginia L. Stauffer: Study concept and design, interpretation of data, critical revision of manuscript for important intellectual content.

Prior Presentation

Some of the data contained in this article were first presented at the 19th Congress of the International Headache Society, September 5–8, 2019, in Dublin, Ireland.

Disclosures

Leslie Citrome in the past 12 months has served as consultant: AbbVie, Acadia, Alkermes, Allergan, Angelini, Astellas, Avanir, Axsome, BioXcel, Boehringer Ingelheim, Cadent Therapeutics, Eisai, Impel, Intra-Cellular Therapies, Janssen, Karuna, Lundbeck, Lyndra, Medavante-ProPhase, Merck, Neurocrine, Noven, Otsuka, Ovid, Relmada, Sage, Sunovion, Teva, University of Arizona, and one-off ad hoc consulting for individuals/entities conducting marketing, commercial, or scientific scoping research; speaker: AbbVie, Acadia, Alkermes, Allergan, Angelini, Eisai, Intra-Cellular Therapies, Janssen, Lundbeck, Neurocrine, Noven, Otsuka, Sunovion, Takeda, Teva, and CME activities organized by medical education companies such as Medscape, NACCME, NEI, Vindico, and Universities and Professional Organizations/Societies; owns stocks (small number of shares of common stock): Bristol-Myers Squibb, Eli Lilly, J & J, Merck, Pfizer purchased > 10 years ago; and received royalties: Wiley (Editor-in-Chief, International Journal of Clinical Practice, through end 2019), UpToDate (reviewer), Springer Healthcare (book), Elsevier (Topic Editor, Psychiatry, Clinical Therapeutics). Margarita Sánchez del Rio has received fees from Allergan, Eli-Lilly, Novartis, and Teva as a speaker or for her participation in advisory boards. Yan Dong, Russell M. Nichols, Shonda A. Foster, and Virginia L. Stauffer are full-time employees of Eli Lilly and Company, Indianapolis, IN, USA, and minority holders of company stock. Antje Tockhorn-Heidenreich is a full-time employee of Eli Lilly and Company, Erl Wood Manor, Surrey, UK.

Compliance with Ethics Guidelines

The protocols for each study were reviewed and approved by the appropriate institutional or ethical review board for each site. All studies described were conducted according to Good Clinical Practice and the Declaration of Helsinki guidelines. Patients provided written informed consent before undergoing study procedures. Adverse outcomes such as serious AEs were reported to the sponsor, IRB and appropriate regulatory authority.

Data Availability

Eli Lilly and Company provides access to all individual participant data collected during the trial, after anonymization, with the exception of pharmacokinetic or genetic data. Data are available to request 6 months after the indication studied has been approved in the US and EU and after primary publication acceptance, whichever is later. No expiration date of data requests is currently set once data are made available. Access is provided after a proposal has been approved by an independent review committee identified for this purpose and after receipt of a signed data sharing agreement. Data and documents, including the study protocol, statistical analysis plan, clinical study report, blank or annotated case report forms, will be provided in a secure data sharing environment. For details on submitting a request, see the instructions provided at www.vivli.org.

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

Supplementary file1 (DOCX 53 kb)^{(53.9KB, docx)}

Data Availability Statement

[CR1] 1.Villalón CM, Olesen J. The role of CGRP in the pathophysiology of migraine and efficacy of CGRP receptor antagonists as acute antimigraine drugs. Pharmacol Ther. 2009;124:309–323. doi: 10.1016/j.pharmthera.2009.09.003. [DOI] [PubMed] [Google Scholar]

[CR2] 2.American Headache Society The American Headache Society position statement on integrating new migraine treatments into clinical practice. Headache. 2019;59:1–18. doi: 10.1111/head.13456. [DOI] [PubMed] [Google Scholar]

[CR3] 3.Sacco S, Bendtsen L, Ashina M, et al. European headache federation guideline on the use of monoclonal antibodies acting on the calcitonin gene related peptide or its receptor for migraine prevention. J Headache Pain. 2019;20:6. doi: 10.1186/s10194-018-0955-y. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR4] 4.Dodick DW, Goadsby PJ, Spierings ELH, Scherer JC, Sweeney SP, Grayzel DS. Safety and efficacy of LY2951742, a monoclonal antibody to calcitonin gene-related peptide, for the prevention of migraine: a phase 2, randomised, double-blind, placebo-controlled study. Lancet Neurol. 2014;13:885–892. doi: 10.1016/S1474-4422(14)70128-0. [DOI] [PubMed] [Google Scholar]

[CR5] 5.Skljarevski V, Oakes TM, Zhang Q, et al. Effect of different doses of galcanezumab vs placebo for episodic migraine prevention: a randomized clinical trial. JAMA Neurol. 2018;75:187–193. doi: 10.1001/jamaneurol.2017.3859. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR6] 6.Dodick DW, Ashina M, Brandes JL, et al. ARISE: A Phase 3 randomized trial of erenumab for episodic migraine. Cephalalgia. 2018;38:1026–1037. doi: 10.1177/0333102418759786. [DOI] [PubMed] [Google Scholar]

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PERMALINK

Benefit–Risk Assessment of Galcanezumab Versus Placebo for the Treatment of Episodic and Chronic Migraine Using the Metrics of Number Needed to Treat and Number Needed to Harm

Leslie Citrome

Margarita Sánchez del Rio

Yan Dong

Russell M Nichols

Antje Tockhorn-Heidenreich

Shonda A Foster

Virginia L Stauffer

Abstract

Introduction

Methods

Results

Conclusion

Trial Registration Numbers

Supplementary Information

Key Summary Points

Introduction

Methods

Data Sources

Table 1.

Outcome Measures

Statistical Analysis

Results

Patient Demographics and Disease Characteristics

Table 2.

Primary Analysis

Table 3.

Secondary Analysis

Table 4.

Table 5.

Effect Sizes Among Patients with Failure of ≥ 2 Prior Preventive Treatments due to Reasons of Efficacy and/or Tolerability

3-Month Data from all 4 Trials Stratified by Migraine Type (EM vs CM)

Pooled 6-Month Data for EVOLVE-1 and EVOLVE-2

Discussion

Limitations

Conclusions

Supplementary Information

Acknowledgements

Funding

Medical Writing, Editorial, and Other Assistance

Authorship

Authors’ Contributions

Prior Presentation

Disclosures

Compliance with Ethics Guidelines

Data Availability

References

Associated Data

Supplementary Materials

Data Availability Statement

ACTIONS

PERMALINK

RESOURCES

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