Pemigatinib

Uitgebreide indicatie	Myeloid/Lymphoid Neoplasms ((8p11 var)
Therapeutische waarde	Nog geen inschatting mogelijk
Totale kosten	67.500,00
Registratiefase	Klinische studies

Product

Werkzame stof	Pemigatinib
Domein	Hematologie
Reden van opname	Indicatieuitbreiding
Hoofdindicatie	Myeloproliferatieve aandoeningen
Uitgebreide indicatie	Myeloid/Lymphoid Neoplasms ((8p11 var)
Merknaam	Pemazyre
Fabrikant	Incyte
Portfoliohouder	Incyte
Werkingsmechanisme	Tyrosine kinase remmer
Toedieningsweg	Oraal
Toedieningsvorm	Tablet
Bekostigingskader	Intramuraal (MSZ)
Aanvullende opmerkingen	FGFR-1 rearrangement positivity status must be known prior to initiation of Pemazyre therapy. Assessment for FGFR 1 rearrangement positivity in tumor specimen should be performed with an appropriate diagnostic test.

Registratie

Registratieroute	Centraal (EMA)
Type traject	Normaal traject
ATMP	Nee
Indieningsdatum	December 2023
Verwachte registratie	September 2024
Weesgeneesmiddel	Ja
Registratiefase	Klinische studies
Aanvullende opmerkingen	Registration will be based on results of the FIGHT-203 study: a single arm, open-label phase 2 study evaluating the efficacy and safety of pemigatinib monotherapy in patients with MLN with FGFR1 rearrangement.

Therapeutische waarde

Huidige behandelopties	MLN with FGFR1 rearrangement is a rare and progressive hematological malignancy. Incidence approx. <1 case per 100.000 persons/year. For patients with MLN with FGFR1 rearrangement in chronic phase, the National Comprehensive Cancer Network (NCCN) US-guidelines identify enrolment in clinical trials as the preferred treatment option. In the absence of a clinical trial, the current recommended approach is monotherapy with a tyrosine kinase inhibitor (TKI) with activity against FGFR1.The NCCN guidelines list pemigatinib, midostaurin, and ponatinib as TKIs with activity against FGFR1. However, none of these drugs (except pemigatinib in US) have been approved for the treatment of MLN with FGFR1 rearrangement.
Therapeutische waarde	Nog geen inschatting mogelijk Deze inschatting doet geen uitspraak over de mogelijke opname in het pakket.
Onderbouwing	Not assessed, no approved treatment for MLN with FGFR-1 rearrangement available. Latest results of the FIGHT-203 study (presented at 2022 ASH) showed in treatment naïve or previously treated patients with MLN with FGFR-1 rearrangements: Of 38 evaluable patients, 28 (73.7%) achieved a clinical complete response (CR; primary endpoint). The rate of complete cytogenetic responses (CCyR) was 70.0% (n=28/40). The rates of CRs and CCyRs in previously treated, efficacy-evaluable patients were 75.8% (n=25/33) and 71.4% (n=25/35), respectively. Of 21 patients with chronic phase (CP) disease, 18 (85.7%) exhibited both clinical CRs and CCyRs. Of 17 patients with blast phase (BP) disease, 9 presented with clinical CRs (52.9%), and 8 (47.1%) with CCyRs. The median exposure to pemigatinib treatment was 6.3 months (range: 0.5-50.2).
Behandelduur	Mediaan 6.3 maand/maanden
Toedieningsfrequentie	1 maal per dag
Dosis per toediening	13,5 mg
Bronnen	ASH 2022 presentation details: Lead Author: Srdan Verstovsek, poster P1732: FIGHT-203, an ongoing phase 2 study of pemigatinib in patients with myeloid/lymphoid neoplasms (MLNs) with fibroblast growth factor receptor 1 (FGFR1) rearrangement (MLNFGFR1): a focus on centrally reviewed clinical and cytogenetic responses in previously treated patients. ClinicalTrials.gov. FIGHT-203. Accessed Dec 2022. https://clinicaltrials.gov/ct2/show/NCT03011372.
Aanvullende opmerkingen	Latest results of the FIGHT-203 study (presented at 2022 ASH) showed in treatment naïve or previously treated patients with MLN with FGFR-1 rearrangements: Of 38 evaluable patients, 28 (73.7%) achieved a clinical complete response (CR; primary endpoint). The rate of complete cytogenetic responses (CCyR) was 70.0% (n=28/40). The rates of CRs and CCyRs in previously treated, efficacy-evaluable patients were 75.8% (n=25/33) and 71.4% (n=25/35), respectively. Of 21 patients with chronic phase (CP) disease, 18 (85.7%) exhibited both clinical CRs and CCyRs. Of 17 patients with blast phase (BP) disease, 9 presented with clinical CRs (52.9%), and 8 (47.1%) with CCyRs. The median exposure to pemigatinib treatment was 6.3 months (range: 0.5-50.2).

Verwacht patiëntvolume per jaar

Patiëntvolume	< 1 Marktaandeel wordt in de regel niet meegenomen tenzij anders vermeld.
Aanvullende opmerkingen	Very rare disease. No published estimates of incidence or prevalence Incidence estimated: <1 case per 100.000 persons/year.

Patiëntvolume

< 1

Marktaandeel wordt in de regel niet meegenomen tenzij anders vermeld.

Aanvullende opmerkingen

Very rare disease. No published estimates of incidence or prevalence Incidence estimated: <1 case per 100.000 persons/year.

Verwachte kosten per patiënt per jaar

Kosten	65.000,00 - 70.000,00
Aanvullende opmerkingen	Lijstprijs €7.732

Mogelijke totale kosten per jaar

Totale kosten	67.500,00 Dit bedrag geeft een indicatie van de totale kosten. Het is de uitkomst van het gemiddelde verwacht patiëntvolume maal de gemiddelde kosten per patiënt; beiden per jaar.

Totale kosten

67.500,00

Dit bedrag geeft een indicatie van de totale kosten. Het is de uitkomst van het gemiddelde verwacht patiëntvolume maal de gemiddelde kosten per patiënt; beiden per jaar.

Off-label gebruik

Er is op dit moment niets bekend over off-label gebruik.

Indicatieuitbreiding

Er is op dit moment niets bekend over indicatieuitbreidingen.

Overige informatie

Er is op dit moment geen overige informatie.