Elexacaftor/Ivacaftor/Tezacaftor: First Approval
Sheridan M. Hoy1
© Springer Nature Switzerland AG 2019
Abstract
A fixed-dose combination tablet of the cystic fibrosis transmembrane conductance regulator (CFTR) corrector tezacaftor and the CFTR potentiator ivacaftor with the next-generation CFTR corrector elexacaftor (hereafter referred to as elexacaftor/ ivacaftor/tezacaftor) [Trikafta™] has been developed by Vertex Pharmaceuticals Inc. to treat patients with the most com- mon cystic fibrosis mutation (F508del). Its use has been associated with statistically significant and/or clinically meaning- ful improvements in lung function and respiratory-related quality of life compared with comparator regimens (placebo or ivacaftor/tezacaftor) in multinational phase II and III studies, and in October 2019 elexacaftor/ivacaftor/tezacaftor was approved by the US FDA for the treatment of cystic fibrosis in patients aged ≥ 12 years who have ≥ 1 F508del mutation in the CFTR gene. A regulatory assessment for elexacaftor/ivacaftor/tezacaftor as a treatment for cystic fibrosis is underway in the EU. This article summarizes the milestones in the development of elexacaftor/ivacaftor/tezacaftor leading to this first approval for the treatment of cystic fibrosis in patients aged ≥ 12 years who have ≥ 1 F508del mutation in the CFTR gene.
Enhanced material for this AdisInsight Report can be found at https://doi.org/10.6084/m9.figshare.10317176
1 Introduction
The transportation of chloride and bicarbonate across the apical membrane of digestive enzyme-, mucus-, saliva-, sweat- and tear-producing epithelial cells is regulated by the cystic fibrosis transmembrane conductance regulator (CFTR) protein [1]. Mutations in the gene encoding the CFTR protein result in abnormal chloride (and conse- quently fluid) and bicarbonate transportation, leading to dehydrated and acidified mucosal surfaces and, ultimately, the formation and build-up of a viscous and sticky mucus [1–4]. This mucus obstructs luminal compartments and ducts, resulting in chronic infections and organ (e.g. res- piratory tract, gastrointestinal tract) dysfunction [1–4]. Among patients with the autosomal recessive disorder cystic fibrosis, the most common CFTR gene mutation identified is F508del [2, 3].
Initial cystic fibrosis treatments focused on the com- plications of the disease (i.e. end organ effects); however,
the central role disrupted ion transportation plays in the
This profile has been extracted and modified from the AdisInsight database. AdisInsight tracks drug development worldwide through the entire development process, from discovery, through pre- clinical and clinical studies to market launch and beyond.
Sheridan M. Hoy [email protected]
1 Springer Nature, Private Bag 65901, Mairangi Bay, Auckland 0754, New Zealand
pathogenesis of cystic fibrosis has led to the development of pharmacological agents that modulate ion transportation by targeting the underlying defect (i.e. the mutant CFTR pro- tein) [1–4]. Two classes of CFTR modulators are currently available for the treatment of patients with cystic fibrosis: correctors increase defective CFTR protein processing and trafficking to the cell surface, while potentiators improve mutant CFTR protein activity at the cell surface [1].
Breakthrough Therapy designation in USA (May) Orphan Drug Status in USA (Aug)
NDA accepted and Priority Review granted in USA (Aug)
Approved in USA (Oct) MAA validated in EU (Oct)
2017 2018 2019 2020 2021 2022
NCT03227471
NCT03525548
Phase I/II trial Phase III trials
NCT03525444
NCT03691779
NCT03525574 NCT04105972
NCT04058353
NCT04043806
NCT04058366
Key milestones in the development of elexacaftor/ivacaftor/tezacaftor for cystic fibrosis. MAA Marketing Authorisation Application, NDA New Drug Application
Correctors and potentiators may be used in combination to further enhance CFTR protein activity [1]. However, while the combination of a corrector (lumacaftor or tezacaftor) with a potentiator (ivacaftor) has shown efficacy in patients with cystic fibrosis homozygous for F508del CFTR, neither combination sufficiently improves clinical outcomes in those with cystic fibrosis heterozygous for F508del CFTR and a minimal function mutation (i.e. a mutation associated with no protein production or no in vitro response to ivacaftor or ivacaftor/tezacaftor) [5]. A combination of the CFTR cor- rector tezacaftor and the CFTR potentiator ivacaftor with the next-generation CFTR corrector elexacaftor (hereafter referred to as elexacaftor/ivacaftor/tezacaftor) [Trikafta™] has received its first approval (in the USA in October 2019) for the treatment of cystic fibrosis in patients aged ≥ 12 years who have ≥ 1 F508del mutation in the CFTR gene [2, 6]. Developed by Vertex Pharmaceuticals Inc., it is the first tri- ple combination therapy available to treat patients with the most common cystic fibrosis mutation [2]. The recommended
2 Scientific Summary
2.1 Pharmacodynamics
Both elexacaftor and tezacaftor increase the amount of F508del CFTR protein reaching the cell surface by facili- tating its processing and trafficking [6]. As each drug binds to a different site on the protein, their concomitant adminis- tration results in an additive effect [6]. Ivacaftor potentiates CFTR protein activity at the cell surface by increasing its open probability (gating) and thus its transportation of chlo- ride [6, 8]. The combined effect of elexacaftor, ivacaftor and tezacaftor is an increase in the quality and function of the F508del CFTR protein at the cell surface, which results in increased activity (as measured by CFTR mediated chloride transport) [6].
dosage regimen is two elexacaftor/ivacaftor/tezacaftor tablets (each containing elexacaftor 100 mg, ivacaftor 75 mg and tezacaftor 50 mg) in the morning and one ivacaftor 150 mg tablet approximately 12 h later, administered orally with fat- containing food [e.g. butter, eggs, meat, nuts, peanut butter, whole milk dairy products (such as cheese and yogurt)] [6]. A regulatory assessment for elexacaftor/ivacaftor/tezacaftor
F3C
N
O
O O O
N S H
N N N N
as a treatment for cystic fibrosis is underway in the EU [7].
Chemical structure of elexacaftor
In bronchial epithelial cells derived from patients aged ≥ 18 years with cystic fibrosis heterozygous for F508del CFTR and a minimal function mutation (n = 4) or homozygous for F508del CFTR (n = 3) participat- ing in a multinational, phase II, proof-of-concept study (NCT03227471; Study 001) [see Sect. 2.3] [9], elex- acaftor increased the expression of mature CFTR protein, and elexacaftor plus tezacaftor, with or without ivacaftor, significantly (p < 0.05) increased mature CFTR protein levels and (subsequently) chloride transportation com- pared with vehicle or ivacaftor plus tezacaftor [9]. It is worth noting that the addition of ivacaftor to elexacaftor plus tezacaftor resulted in an approximately 1.4- to 3.1- fold greater increase in chloride transportation (values derived from a graph) than elexacaftor plus ivacaftor, elex- acaftor plus tezacaftor or tezacaftor plus ivacaftor. The improvements in CFTR protein function were reflected in reductions from baseline in sweat chloride concentra- tions at week 4 in this study [9]. In a 24-week, multi- national, phase III study (NCT03525444; Study 102)
[5] (see Sect. 2.3) in patients aged ≥ 12 years with cystic
fibrosis heterozygous for F508del CFTR and a minimal function mutation, elexacaftor/ivacaftor/tezacaftor sig- nificantly reduced sweat chloride concentrations from baseline at week 4 relative to placebo [least-squares mean (LSM) treatment difference in the LSM absolute change of − 41.2 mmol/L; p < 0.001], with the reduction sustained through to week 24 (LSM treatment difference in the LSM absolute change of − 41.7 mmol/L; p < 0.001). The tri- ple combination of elexacaftor, ivacaftor and tezacaftor also significantly reduced sweat chloride concentrations from baseline at week 4 relative to ivacaftor/tezacaftor (LSM treatment difference of − 45.1 mmol/L; p < 0.001) in patients aged ≥ 12 years with cystic fibrosis homozy- gous for F508del CFTR participating in a 4-week, mul- tinational, phase III study (NCT03525548; Study 103)
[10] (see Sect. 2.3). Of note, mean sweat chloride con- centrations at study end (week 24 [5] and 4 [10]) were
57.9 mmol/L [5] and 48.0 mmol/L [10] in elexacaftor/ ivacaftor/tezacaftor recipients, ≈ 92.5 mmol/L (value esti- mated from a graph) [10] in ivacaftor/tezacaftor recipients and 102.4 mmol/L in placebo recipients [5].
No clinically relevant QT/corrected QT interval prolonga- tion was observed in healthy volunteers receiving suprath- erapeutic doses (i.e. ≤ 2/≤ 3/≤ 3-fold the maximum dose) of elexacaftor/ivacaftor/tezacaftor [6].
2.2 Pharmacokinetics
The pharmacokinetics of elexacaftor, ivacaftor and tezacaftor are similar between healthy volunteers and patients with cystic fibrosis [6]. Moreover, according to a population pharmacokinetic analysis, elexacaftor, ivacaftor
and tezacaftor exposures at steady state were similar between patients aged ≥ 18 years and those aged 12 to < 18 years receiving oral elexacaftor/ivacaftor/tezacaftor (elexacaftor 200 mg once daily, ivacaftor 150 mg twice daily and tezacaftor 100 mg once daily) [6].
In patients aged ≥ 12 years with cystic fibrosis, the absolute bioavailability of elexacaftor is 80%; values for tezacaftor and ivacaftor have not been determined [6]. The maximum concentrations of elexacaftor, iva- caftor and tezacaftor were reached in a median of 6, 4 and 3 h, respectively, and food increased the exposure of elexacaftor and ivacaftor 1.9- to 2.5-fold and 2.5- to 4-fold, respectively (see Sect. 1). Elexacaftor, ivacaftor and tezacaftor reached steady state within 14, 3.5 and 8 days, respectively, and had accumulation ratios of 2.3,
2.4 and 1.6, respectively. At least 99% of elexacaftor, ivacaftor and tezacaftor is protein bound [primarily to albumin (elexacaftor, ivacaftor and tezacaftor), alpha 1-acid glycoprotein (ivacaftor) and human gamma-glob- ulin (ivacaftor)]. The metabolism of elexacaftor, ivacaftor and tezacaftor occurs predominately via cytochrome P450 (CYP)3A4/5, with the metabolites of elexacaftor and tezacaftor demonstrating a similar potency to that of the parent drug. The mean terminal half-lives of elex- acaftor, ivacaftor and tezacaftor were approximately 24.7,
13.1 and 60.3 h, respectively. Elexacaftor, ivacaftor and tezacaftor are each primarily (87.3%, 87.8% and 72%, respectively) eliminated via the faeces, with elexacaftor eliminated mainly as metabolites [6].
As elexacaftor, ivacaftor and tezacaftor are all metabolised by CYP3A, their exposure may be increased or decreased if they are coadministered with drugs that are inhibitors or inducers, respectively, of CYP3A [6]. Thus, coadministering elexacaftor/ivacaftor/tezacaftor with strong CYP3A induc- ers (e.g. rifampicin) is not recommended and the dose of elexacaftor/ivacaftor/tezacaftor should be reduced when it is used concomitantly with moderate (e.g. fluconazole) or strong (e.g. ketoconazole) CYP3A4 inhibitors. Also, food or drink containing grapefruit should be avoided by patients receiving elexacaftor/ivacaftor/tezacaftor [6].
2.3 Therapeutic Trials
The triple combination therapy of elexacaftor, ivacaftor and tezacaftor showed promise as a treatment for cystic fibro- sis in patients aged ≥ 18 years heterozygous for F508del CFTR and a minimal function mutation, or homozygous for F508del CFTR participating in a 4-week, randomized, double-blind, double-dummy, multinational, phase II, dose- ranging, proof-of-concept study (NCT03227471; Study 001) [9]. Patients with the F508del/minimal function CFTR gen- otype received oral elexacaftor/ivacaftor/tezacaftor (elex- acaftor 50, 100 or 200 mg once daily in combination with
Alternative names Elexacaftor/ivacaftor/tezacaftor—Vertex Pharmaceuticals; ELX/TEZ/IVA; ivacaftor/tezacaftor/VX 445; tezacaftor/VX-445/ivacaftor; TRIKAFTA; VX 445/ivacaftor/tezacaftor; VX-445/TEZ/IVA; VX-445/VX-661/ VX-770
Class Amides; aminophenols; antifibrotics; benzodioxoles; cyclopropanes; fluorinated hydrocarbons; fluorobenzenes; indoles; pyrazoles; pyridines; pyrrolidines; quinolones; small molecules; sulfonamides
Mechanism of action Cystic fibrosis transmembrane conductance regulator stimulants Route of administration Oral
Pharmacodynamics Elexacaftor and tezacaftor: facilitate the processing and trafficking of the F508del CFTR protein, thereby increas- ing the amount of it reaching the cell surface; additive effect when administered concomitantly
Ivacaftor: increases the open probability (gating) activity of the CFTR protein, thereby increasing its transporta- tion of chloride
Pharmacokinetics (elex-
acaftor, ivacaftor and tezacaftor)
Median time to maximum plasma concentration of 6, 4 and 3 h, respectively, with steady state reached within 14,
3.5 and 8 days, respectively
Estimated terminal half-life of 24.7, 13.1 and 60.3 h, respectively
Most frequent adverse events Headache, diarrhoea, upper respiratory tract infection ATC codes
WHO ATC code R07A-X31 (ivacaftor/tezacaftor) EphMRA ATC code R7 (other respiratory system products)
Chemical name N-(2,4-Di-tert-butyl-5-hydroxyphenyl)-1,4-dihydro-4-oxoquinoline-3-carboxamide / 1-(2,2-difluoro-1,3-ben- zodioxol-5-yl)-N-[1-[(2R)-2,3-dihydroxypropyl]-6-fluoro-2-(1-hydroxy-2-methylpropan-2-yl)indol-5-yl] cyclopropane-1-carboxamide / N-(1,3-dimethylpyrazol-4-yl)sulfonyl-6-[3-(3,3,3-trifluoro-2,2-dimethylpropoxy) pyrazol-1-yl]-2-[(4S)-2,2,4-trimethylpyrrolidin-1-yl]pyridine-3-carboxamide
ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily; n = 10, 22 and 21, respectively) or placebo (n = 12) for 4 weeks. Those with the F508del/F508del CFTR geno- type underwent a 4-week run-in period with oral ivacaftor/ tezacaftor and then received either oral elexacaftor/ivacaftor/ tezacaftor (elexacaftor 200 mg once daily, ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily; n = 21) or oral ivacaftor/tezacaftor (ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily; n = 7) for 4 weeks [9].
Elexacaftor/ivacaftor/tezacaftor, but not the comparator regimens, significantly (p < 0.001) improved the LSM abso- lute change at week 4 in the percentage predicted forced expiratory volume in 1 s (ppFEV1; primary endpoint) rela- tive to baseline in both patients with the F508del/minimal function CFTR genotype (7.9–13.8 for all of the elexacaftor/ ivacaftor/tezacaftor groups and 0.0 for placebo) [mean baseline values of 56.4–60.0 and 59.0] and those with the F508del/F508del CFTR genotype (11.0 for elexacaftor/ ivacaftor/tezacaftor and 0.4 for ivacaftor/tezacaftor) [mean baseline values of 60.0 and 62.8] [9]. A treatment effect was seen as early as week 2 for this endpoint, and maintained to week 4 in all of the elexacaftor/ivacaftor/tezacaftor groups. Moreover, elexacaftor/ivacaftor/tezacaftor was associated with a clinically meaningful (i.e. a change of ≥ 4 points) improvement from baseline at week 4 in respiratory-related quality of life (QOL) [as measured by the Cystic Fibrosis Questionnaire-Revised (CFQ-R) respiratory domain score] in both patients with the F508del/minimal function CFTR genotype (LSM absolute change of 15.4–25.7 for all of the
elexacaftor/ivacaftor/tezacaftor groups and 4.2 for placebo) [mean baseline values of 61.1–65.9 and 57.4] and those with the F508del/F508del CFTR genotype (LSM absolute change of 20.7 for elexacaftor/ivacaftor/tezacaftor and 5.2 for iva- caftor/tezacaftor) [mean baseline values of 73.0 and 71.2]. Of note, improvements in efficacy outcomes among the 21 patients with the F508del/minimal function CFTR geno- type who received a deuterated form of ivacaftor (adminis- tered once daily) rather than ivacaftor itself (administered twice daily) as part of their treatment regimen were similar to those seen in the other treatment groups [9].
Patients in Study 001 had stable disease and a ppFEV1 at screening of 40–90 [9]. CFQ-R scores range from 0–100, with higher scores indicating higher QOL. Among patients with the F508del/minimal function CFTR genotype, those who received active treatment had as much as an 8.5-point lower baseline CFQ-R score than those who received pla- cebo. Other baseline characteristics (e.g. age, ppFEV1, sex) were well balanced across genotype and treatment groups [9]. The addition of elexacaftor to ivacaftor plus tezacaftor was associated with significant improvements relative to the comparator regimens in all of the primary and key second- ary endpoints for two randomized, double-blind, multina- tional, phase III studies (NCT03525444 (Study 102) [5] and NCT03525548 (Study 103) [10]) in patients aged ≥ 12 years with cystic fibrosis heterozygous for F508del CFTR and a minimal function mutation [5], or homozygous for F508del CFTR [10]. Results for the sweat chloride concentration end-
point are discussed in Sect. 2.1.
In Study 102 [5], patients received oral elexacaftor/iva- caftor/tezacaftor (elexacaftor 200 mg once daily, ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily) [n = 200] or placebo (n = 203) for 24 weeks; mean adher- ence was 98% in both treatment groups. In an interim analysis (defined as when ≥ 140 patients had completed week 4 and ≥ 100 patients had completed week 12), the LSM absolute change from baseline at week 4 in ppFEV1 (primary endpoint) was significantly greater with elexacaftor/ivacaftor/ tezacaftor than placebo [13.6 vs − 0.2; LSM between-group difference of 13.8 (95% CI 12.1–15.4); p < 0.001] (mean baseline values of 61.6 and 61.3). A treatment effect was seen as early as week 2 for this endpoint, and sustained to week 24 (final analysis) [13.9 vs −0.4; LSM between-group difference of 14.3 (95% CI 12.7–15.8); p < 0.001]. Significant (p < 0.05)
between-group differences favouring elexacaftor/ivacaftor/ tezacaftor over placebo in the LSM absolute change from baseline at week 4 in ppFEV1 were observed in all prespeci- fied subgroups [including age at screening (≥ 12 to < 18 years or ≥ 18 years); baseline ppFEV1 (< 70 or ≥ 70); previous use of bronchodilators, dornase alfa, hypertonic saline, inhaled antibiotics or inhaled corticosteroids (yes vs no); Pseu- domonas aeruginosa status within 2 years prior to screening (positive vs negative); and sex]. Consistent LSM differences between elexacaftor/ivacaftor/tezacaftor and placebo in this endpoint (11.3, 14.5 and 15.2, respectively) were also seen in the subgroups of patients in whom the minimal-function mutation caused an absence of CFTR protein production (n = 141 and 150), those with missense or in-frame deletion mutations (n = 44 and 38) and those with a baseline ppFEV1 of < 40 (n = 17 and 16), according to ad hoc analyses [5].
Triple combination therapy with elexacaftor, ivacaftor and tezacaftor also reduced pulmonary exacerbations and improved respiratory-related QOL and body mass index (BMI) in Study 102 [5]. The annualised rate of pulmonary exacerbations was 63% lower with elexacaftor/ivacaftor/ tezacaftor compared with placebo at week 24 [41 vs 113; rate ratio of 0.37 (95% CI 0.25–0.55); p < 0.001], with similar benefits seen in the annualised rates of pulmonary exacerba- tions leading to hospitalization [rate ratio of 0.29 (95% CI 0.14–0.61)] and pulmonary exacerbations requiring treat- ment with intravenous antibiotics [rate ratio of 0.22 (95% CI 0.11–0.43)]. Elexacaftor/ivacaftor/tezacaftor improved respir- atory-related QOL by a statistically significant and clinically meaningful extent from baseline (mean values of 68.3 and 70.0) at week 4 [LSM absolute change in the CFQ-R res- piratory domain score of 18.1 vs − 1.9; LSM between-group difference of 20.1 (95% CI 16.9–23.2); p < 0.001] relative to placebo, with these improvements sustained at week 24 [LSM absolute change of 17.5 vs − 2.7; LSM between-group dif- ference of 20.2 (95% CI 17.5–23.0); p < 0.001]. Moreover, BMI was significantly improved from baseline (mean values of 21.5 and 21.3 kg/m2) at week 24 (LSM absolute change of
1.13 vs 0.09; LSM between-group difference of 1.04 (95% CI 0.85–1.23); p < 0.001] compared with placebo [5].
In Study 103, patients underwent a 4-week open-label run-in period with oral ivacaftor/tezacaftor (ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily) and then received either oral elexacaftor/ivacaftor/tezacaftor (elexacaftor 200 mg once daily, ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily) [n = 55] or oral ivacaftor/ tezacaftor (ivacaftor 150 mg every 12 h and tezacaftor 100 mg once daily) [n = 52] for 4 weeks [10]. Adding elex- acaftor to ivacaftor/tezacaftor resulted in superior lung function, with a LSM absolute change from baseline (mean values of 60.2 and 61.6) in ppFEV1 at week 4 of 10.4 versus
0.4 with ivacaftor/tezacaftor [LSM between-group differ- ence of 10.0 (95% CI 7.4–12.6); p < 0.0001]. A treatment effect was seen as early as week 2 for this endpoint, and improvements were consistent across all of the subgroups assessed [including age at screening (≥ 12 to < 18 years or ≥ 18 years); baseline ppFEV1 (< 70 or ≥ 70); previous use of bronchodilators, dornase alfa, hypertonic saline, inhaled antibiotics or inhaled corticosteroids (yes vs no); P. aer- uginosa status within 2 years prior to screening (positive vs negative); and sex]. Elexacaftor/ivacaftor/tezacaftor was also associated with statistically significant and clinically meaningful improvements from baseline (mean values of
72.6 and 70.6) in respiratory-related QOL at week 4 [LSM absolute change in the CFQ-R respiratory domain score of 16.0 vs − 1.4 with ivacaftor/tezacaftor; LSM between- group difference of 17.4 (95% CI 11.8–23.0); p < 0.001]. According to a post-hoc analysis, at week 4, elexacaftor/ ivacaftor/tezacaftor had improved BMI by 0.6 kg/m2 (LSM change from baseline; nominal p < 0.0001) and bodyweight (an important predictor of survival in patients with cystic fibrosis) by 1.6 kg (LSM change from baseline; nominal p < 0.0001) compared with ivacaftor/tezacaftor [10].
Patients in Studies 102 and 103 had stable disease and a ppFEV1 at screening of 40-90, and continued receiv- ing standard of care therapies (e.g. bronchodilators, dor- nase alfa, hypertonic saline, inhaled antibiotics) [5, 6, 10]. Those infected with organisms associated with a more rapid decline in pulmonary status (e.g. Burkholderia cenocepa- cia, B. dolosa, Mycobacterium abscessus) were among those excluded [5, 6, 10]. Following completion of the studies, all of the patients entered a (currently ongoing) 96-week open- label extension study (NCT03525574; Study 105) [5, 6, 10].
2.4 Adverse Events
Following the addition of elexacaftor to ivacaftor and tezacaftor, an acceptable adverse event (AE) profile was observed in patients aged ≥ 12 years with cystic fibrosis participating in Studies 001 [9], 102 [5] and 103 [10]. Most
ELX/TEZ/VX-561, PL, IVA/TEZ
ELX/IVA/TEZ, PL III Completed Multinational NCT03525444 (Study 102) Vertex Pharmaceuticals Inc. ELX/IVA/TEZ, IVA/TEZ III Completed Multinational NCT03525548 (Study 103) Vertex Pharmaceuticals Inc. ELX/IVA/TEZ III Active, not recruiting Multinational NCT03525574 (Study 105) Vertex Pharmaceuticals Inc. ELX/IVA/TEZ, IVA III Recruiting USA NCT04043806 (Study 113) Vertex Pharmaceuticals Inc.
ELX/IVA/TEZ, IVA, IVA/
TEZ
III Recruiting USA NCT04058353 (Study 104) Vertex Pharmaceuticals Inc.
ELX/IVA/TEZ III Recruiting Multinational NCT03691779 (Study 106) Vertex Pharmaceuticals Inc. ELX/IVA/TEZ, IVA III Not yet recruiting NR NCT04058366 (Study 110) Vertex Pharmaceuticals Inc.
ELX/IVA/TEZ, IVA, IVA/
TEZ
III Not yet recruiting NR NCT04105972 (Study 109) Vertex Pharmaceuticals Inc.
ELX/IVA/TEZ NR Recruiting USA NCT04056702 Cystic Fibrosis Foundation
ELX/IVA/TEZ NR Not yet recruiting USA NCT04038047 (PROM-
ISE)
Cystic Fibrosis Foundation
ELX/IVA/TEZ, IVA Expanded access Available NR NCT04058210 (Study 901) Vertex Pharmaceuticals Inc.
ELX elexacaftor, IVA ivacaftor, NR not reported, PL placebo, TEZ tezacaftor, VX-561 deuterated IVA
AEs in these studies were mild or moderate in severity; no deaths were reported [5, 9, 10].
In Study 001 [9], ≥ 1 AE occurred in 92% of 74 patients in the combined elexacaftor/ivacaftor/tezacaftor group, 71% of 7 patients in the ivacaftor/tezacaftor group and 100% of 12 patients in the placebo group. The most frequently reported (occurring in ≥ 10% of patients in the combined elexacaftor/ivacaftor/tezacaftor group and with a numeri- cally higher incidence in this group than the ivacaftor/ tezacaftor or placebo groups) AEs in the respective groups were cough (occurring in 31%, 14% and 8% of patients), increased sputum (27%, 0% and 25%), infective pulmonary
exacerbations of cystic fibrosis (20%, 14% and 33%), haem-
optysis (14%, 0% and 17%) and pyrexia (12%, 14% and 8%). There was no evidence of acute bronchoconstriction. Severe AEs occurred in 20% of patients in the combined elexacaftor/ivacaftor/tezacaftor group, 4% of patients in the ivacaftor/tezacaftor group and 8% of patients in the placebo group; serious AEs occurred in three, one and one patient(s). AEs resulting in an interruption or discontinuation of the study medication occurred in 4% and 4% of patients in the combined elexacaftor/ivacaftor/tezacaftor group, 14% and 14% of those in the ivacaftor/tezacaftor group and 0% and 0% of those in the placebo group. In the combined elex- acaftor/ivacaftor/tezacaftor group, constipation (n = 1), elevated bilirubin levels (n = 1), and elevated aspartate ami- notransferase, alanine aminotransferase and creatine kinase levels and myopathy (n = 1) led to an interruption in the study medication, while chest pain (n = 1), elevated bilirubin levels (n = 1) and rash (n = 1) led to discontinuation of the study medication. Of note, the safety profile of elexacaftor/
deuterated ivacaftor/tezacaftor appears to be similar to that of elexacaftor/ivacaftor/tezacaftor [9].
In Study 102 [5], AEs were reported in most (93% and 96%) elexacaftor/ivacaftor/tezacaftor and placebo recipients (n = 202 and 201); ≥ 10% of patients experienced AEs that were consistent with common manifestations and compli- cations of cystic fibrosis and the majority of AEs resolved during the study. The AEs that occurred most frequently (incidence of ≥ 10% of patients in either treatment group) and in numerically more elexacaftor/ivacaftor/tezacaftor than placebo recipients were headache (in 17% vs 15% of patients), diarrhoea (13% vs 7%) and upper respiratory tract infection (12% vs 11%). Of note, rash was reported in 11% of patients receiving elexacaftor/ivacaftor/tezacaftor and 7% of those receiving placebo. However, regardless of the regi- men received, it occurred in more female than male patients and in more female patients taking than not taking hormonal contraceptives. Infective pulmonary exacerbations of cystic fibrosis occurred in approximately twofold less elexacaftor/ ivacaftor/tezacaftor recipients than placebo recipients (22% and 47%), while the incidence of increased sputum appeared similar between the groups (20% and 19%). Severe AEs were reported in 19% and 7% of patients in the respective groups; one patient receiving elexacaftor/ivacaftor/tezacaftor expe- rienced a life-threatening AE. Serious AEs occurred in 14% of elexacaftor/ivacaftor/tezacaftor recipients and 21% of placebo recipients; two elexacaftor/ivacaftor/tezacaftor recipients (and none of the placebo recipients) discontinued the study medication because of an AE [portal hypertension (in a patient with pre-existing cirrhosis) and rash]. Of note, elevated aminotransferase levels were reported as AEs in
11% of elexacaftor/ivacaftor/tezacaftor recipients and 4% of placebo recipients; most (91%) of those observed in patients receiving elexacaftor/ivacaftor/tezacaftor were mild or mod- erate in severity and not treatment limiting [5].
In Study 103 [10], 58% of 55 elexacaftor/ivacaftor/ tezacaftor recipients and 63% of 52 ivacaftor/tezacaftor recipients experienced AEs, with 2% and 0% experiencing grade 3 or 4 AEs. Most AEs resolved during the study, with no patient in either group discontinuing treatment because of an AE. Moreover, the safety profile of elexacaftor/iva- caftor/tezacaftor in this study was consistent among the sub- groups. The most commonly occurring AEs (in ≥ 4 patients in either group and with a numerically higher incidence in the elexacaftor/ivacaftor/tezacaftor group than the ivacaftor/ tezacaftor group) were cough (15% vs 8%), nasopharyngi- tis (7% vs 4%), oropharyngeal pain (7% vs 0%) and upper respiratory tract infection (7% vs 4%). It is worth noting that rash was reported in two elexacaftor/ivacaftor/tezacaftor recipients and two ivacaftor/tezacaftor recipients (all of whom were female), with hormonal contraceptives taken by one patient in each treatment group who had rash. Moreover, infective pulmonary exacerbations of cystic fibrosis occurred in only 2% of patients in the elexacaftor/ivacaftor/tezacaftor group, but in 12% of those in the ivacaftor/tezacaftor group. Severe AEs occurred in none of the patients receiving elex- acaftor/ivacaftor/tezacaftor, but one of the patients receiving ivacaftor/tezacaftor, while serious AEs occurred in two elex- acaftor/ivacaftor/tezacaftor recipients (pulmonary exacerba- tion and rash) and one ivacaftor/tezacaftor recipient (pulmo- nary exacerbation). Treatment-related AEs occurred in 22% and 17% of patients in the respective groups, and serious treatment-related AEs in 2% and 0%. Elevated aminotrans- ferase levels were reported as AEs (which were assessed as mild in severity and not serious) in 4% of elexacaftor/ ivacaftor/tezacaftor recipients and 2% of ivacaftor/tezacaftor recipients [10].
2.5 Ongoing Clinical Trials
There are several ongoing studies of elexacaftor/iva- caftor/tezacaftor in patients with cystic fibrosis. Two ran- domized, double-blind, phase III studies are recruiting (NCT04058353) or not yet recruiting (NCT04105972) patients aged ≥ 12 years, while one noncomparative phase III study (NCT03691779) is recruiting patients aged 6–11 years. Three long-term, open-label, phase III studies are cur- rently active, but not recruiting (NCT03525574), recruiting (NCT04043806) or not recruiting (NCT04058366) patients aged ≥ 12 years. Elexacaftor/ivacaftor/tezacaftor is also being investigated in two further studies [NCT04056702 and NCT04038047 (PROMISE)], both of which have been initiated by the Cystic Fibrosis Foundation.
3 Current Status
Elexacaftor/ivacaftor/tezacaftor received its first approval on 21 October 2019 for the treatment of cystic fibrosis in patients aged ≥ 12 years who have ≥ 1 F508del mutation in the CFTR gene in the USA.
Compliance with Ethical Standards
Funding The preparation of this review was not supported by any external funding.
Conflict of interest During the peer review process the manufacturer of the agent under review was offered an opportunity to comment on the article. Changes resulting from any comments received were made by the author on the basis of scientific completeness and accu- racy. Sheridan Hoy is a salaried employee of Adis International Ltd/ Springer Nature, is responsible for the article content and declares no relevant conflicts of interest.
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