The tale of lenalidomide clinical superiority over thalidomide and regulatory and cost-effectiveness issues

Paumgartten, Francisco José Roma

doi:10.1590/1413-812320182410.28522017

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FREE THEMES • Ciênc. saúde coletiva 24 (10) • Oct 2019 • https://doi.org/10.1590/1413-812320182410.28522017 copy

The tale of lenalidomide clinical superiority over thalidomide and regulatory and cost-effectiveness issues

A narrativa de que a lenalidomida é clinicamente superior à talidomida, e questões regulatórias e de custo-efetividade

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

In April 2017, the National Sanitary Surveillance Agency (ANVISA-Brazil) approved lenalidomide (LEN) for multiple myeloma (MM) and myelodysplastic syndrome. ANVISA had rejected the first application in 2010, and denied a request for reconsideration in 2012. The reason for rejection was the lack of comparative effectiveness studies proving that LEN was more effective than thalidomide (THAL), a strictly controlled drug regulated by Federal law 10.651/2003 and dispensed to patients (at no costs) through public health system units and hospitals. ANVISA unexplained retreat on the LEN approval for marketing was an unquestionable triumph of the lobbying that ensued the denial, at the forefront of which were politicians, Congress members, patient organizations and medical societies. Two randomized (phase III) trials and three observational (case-control and population-based cohort) compared the effectiveness of THAL- versus LEN-based therapies in MM. Overall, these studies showed no difference in efficacy between LEN- and THAL-based therapies. LEN caused less neuropathy, and more severe hematologic adverse effects. It is much costlier than THAL, and substitution of THAL by LEN shall raise considerably public healthcare costs in Brazil.

Keywords
Multiple myeloma; Cost-effectiveness; Cancer; Healthcare costs

Authors / year	Study type	Study population	Compared therapies	Clinical outcome
Authors / year	Study type	Study population	Compared therapies	Efficacy endpoints	Side effects
Stewart et al., 2015 ¹⁸18 Stewart AK, Jacobus S, Fonseca R, Weiss M, Callander NS, Chanan-Khan AA, Rajkumar SV. Melphalan, prednisone, and thalidomide vs melphalan, prednisone, and lenalidomide (ECOG E1A06) in untreated multiple myeloma. Blood 2015; 126(11):1294-1301.	Phase III Randomized Controlled Trial (non-inferiority design)	Elderly patients with untreated MM	MPT-T versus MPR-R	No difference in RR, PFS, and OS	MPR-R: lower incidence of peripheral neuropathy.
Zweegman et al., 2016 ¹⁹19 Zweegman S, van der Holt B, Mellqvist UH, Salomo M, Bos GM, Levin MD, Visser-Wisselaar H, Hansson M, van der Velden AW, Deenik W, Gruber A, Coenen JL, Plesner T, Klein SK, Tanis BC, Szatkowski DL, Brouwer RE, Westerman M, Leys MR, Sinnige HA, Haukås E, van der Hem KG, Durian MF, Mattijssen EV, van de Donk NW, Stevens-Kroef MJ, Sonneveld P, Waage A. Melphalan, prednisone, and lenalidomide versus melphalan, prednisone, and thalidomide in untreated multiple myeloma. Blood 2016; 127(9):1109-1116.	Phase III Multicenter open-label RCT (study design similar to that of Stewart et al.'s trial)	Newly-diagnosed MM who were ineligible to stem cell transplant	MPT-T versus MPR-R	No difference in PFS (primary efficacy endpoint)	MPT-T: increased incidence of peripheral neuropathy MPR-R: increased incidence of hematologic toxicity requiring growth factor support.
Gay et al., 2010 ²⁰20 Gay F, Hayman SR, Lacy MQ, Buadi F, Gertz MA, Kumar S, Dispenzieri A, Mikhael JR, Bergsagel PL, Dingli D, Reeder CB, Lust JA, Russell SJ, Roy V, Zeldenrust SR, Witzig TE, Fonseca R, Kyle RA, Greipp PR, Stewart AK, Rajkumar SV. Lenalidomide plus dexamethasone versus thalidomide plus dexamethasone in newly diagnosed multiple myeloma: a comparative analysis of 411 patients. Blood 2010; 115(7):1343-1350.	Observational (case-control designed) retrospective study. Matched-pair analysis adjusted for age, sex, transplantation, DXM dose⁺ + Patients treated with thalidomide and DXM received different doses of DXM. Adverse events were graded according to the US National Cancer Institute Common Terminology Criteria. HR: hazard ratio. mo: months. RR: response rates PFS: Progression free survival; TTP: time to progression; OS: overall survival. .	Newly diagnosed MM patients (initial therapy)	Lenalidomide + DXM versus Thalidomide + DXM.	Lenalidomide + DMX: longer TTP (median 27.4 versus 17.2 mo), PFS (26.7 versus 17.1 mo); OS (not reached versus 57.2 mo).	Similar proportion of patients in the 2 groups experienced at least one grade 3 or 4 adverse event (thalidomide versus lenalidomide: 54.6% versus 57.5%)^#
Sashidharan et al. 2015 ²¹21 Sashidharan N, Shenoy S, Kishore MK, Thanusubramanian H. Comparison of Two Therapeutic Regimes, Lenalidomide with Dexamethasone and Thalidomide with Dexamethasone, in the Treatment of Multiple Myeloma at a Tertiary Care Hospital in India. J Clin Diagn Res 2015; 9(5):XC01-XC04.	Observational (analysis of medical record files) retrospective study.	Newly diagnosed MM patients who attended medical care in tertiary hospitals in India.	Thalidomide + DXM (n=17) versus lenalidomide+DXM (n=19)	Proportion of patients showing minimal and partial clinical response to treatment (serum immunoglobulin levels, bone marrow biopsy)	Proportion of adverse events did not differ. Yet not differing statistically, 04 (23.5%) patients treated with thalidomide presented neuropathy against 01 (5.3%) that received lenalidomide.
Luo et al., 2017 ²²22 Luo J, Gagne JJ, Landon J, Avorn J, Kesselheim AS. Comparative effectiveness and safety of thalidomide and lenalidomide in patients with multiple myeloma in the United States of America: A population-based cohort study. Eur J Cancer 2017; 70:22-33.	Observational (population-based cohort).	Patients with MM receiving thalidomide or lenalidomide in routine care in the US. (N= 1264)	Thalidomide-based versus lenalidomide-based therapies	No difference in rates of death (HR: 95% CI, 1.00: 0.71-1.41)	Lenalidomide-based therapies: lower risk of peripheral neuropathy (HR: 95%CI, 0.71: 0.56-0.92).

	Thalidomide	Lenalidomide
Brand name	Generic name	Revilimid ^®
Manufacturer	State owned (public) industry (FUNED-MG)	Pharmaceutical company (Celgene ^® Co)
Potential to cause birth defects (teratogenicity)	Proven to humans and non-human primates	Proven to non-human primates (likely human teratogen)
Regulation	Federal Law (10.651/2003) and additional rules issued by ANVISA	Regulation to be issued by ANVISA (Public Consultation No. 393/2017)
Sales	Prohibited	No restriction.
Costs	Low cost medicine	(very) High cost medicine
Promotion of Prescription & Advertisement	Prohibited (nonexistent)	Allowed if directed to prescribers (as any other prescription drug)⁺ + According to PC 393/2017 (Art,45), "any" advertisement of lenalidomide is forbidden. However, Art.45 (paragraph) makes an exemption for advertising lenalidomide-based medicines in publications intended to medical or scientific purposes. In practice, there is no restriction to propaganda, because this is the usual way by which pharmaceutical companies promote prescription of "prescription-only" drugs among physicians.
Use for off-label therapeutic indications	Strictly controlled by ANVISA	Uncontrolled by ANVISA
Drug distribution and dispensing	Exclusively to public health units and hospitals (controlled by health authorities)	Distribution and dispensing controlled by the company
Authorized prescribers / pharmacists	Registered by local health authority	Qualified and registered by the company.

ABRASCO - Associação Brasileira de Saúde Coletiva Av. Brasil, 4036 - sala 700 Manguinhos, 21040-361 Rio de Janeiro RJ - Brazil, Tel.: +55 21 3882-9153 / 3882-9151 - Rio de Janeiro - RJ - Brazil
E-mail: cienciasaudecoletiva@fiocruz.br

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[TFN1] MPT-T: Induction with "melphalan/prednisone/thalidomide" and maintenance with thalidomide. MPR-R: Induction with "melphalan/prednisone/lenalidomide (Revilimid ^® )" and maintenance with lenalidomide. DXM: dexamethasone.

[TFN2] ⁺
Patients treated with thalidomide and DXM received different doses of DXM. Adverse events were graded according to the US National Cancer Institute Common Terminology Criteria. HR: hazard ratio. mo: months. RR: response rates PFS: Progression free survival; TTP: time to progression; OS: overall survival.