Published: 9 December 2021
Committees
Minutes for the 67th meeting of
the Medicines Classification Committee held in Wellington on 26 October
2021 at 9:30 am
Present:
Andi Shirtcliffe (Chair)
Dr Natasha White
Dr David (Buzz) Boothman-Burrell
Dr Marcia Walker
Kerri Miedema
Angela Renall
Jacinta Patel (Secretary)
In attendance (from Medsafe):
Courtenay Kularatne (Advisor, Product Regulation)
Sam Horsefield (Advisor, Regulatory Practice and Analysis)
Matthew Spencer (Manager, Product Regulation)
1 |
WelcomeThe Chair opened the meeting at 9.32am with a karakia and welcomed members and guests. |
2 |
Apologies |
3 |
Confirmation of the minutes of the 66th meeting held on 11 May 2021 |
4 |
Declaration of conflicts of interestThe Conflict of Interest forms were returned to the Secretary. The following conflicts of interest were declared:
All other members declared they had no additional interests which would pose a conflict with any of the items on the agenda. |
5 |
Matters arising |
5.1 |
Objections to recommendations made at the 66th meetingNo valid objections were received. |
5.2 |
Update on outstanding agenda items from the 66th meeting |
a. |
(6.1) Allopurinol for reviewAt the 66th meeting, the Committee deferred making a recommendation in order to engage with the Pharmacy Council process for medicines reclassification as outlined in the guidance. The Pharmacy Council have provided the following document. DiscussionThe Committee received a letter from the submitter requesting the decision for allopurinol to be deferred to a later date. RecommendationThe submission for allopurinol will be considered by the Committee at a future meeting. |
b. |
(7.2a) CardarineBackgroundAt the 66th meeting the Committee requested that Medsafe write an information paper for the Committee on cardarine and other SARM-like substances. DiscussionThe Committee thanked the Medsafe Investigation and Enforcement Team for providing an informative paper on cardarine and agreed with the suggestion for harmonisation with the Australian Schedule, in line with the long-standing Trans-Tasman scheduling harmonisation agreement. Cardarine has been classified as a Schedule 10 substance in Australia. The Committee acknowledges the scheduling system varies between countries and therefore agree that it is appropriate to schedule cardarine as a prescription medicine to harmonise. The Committee expressed interest in the potential for a class entry for SARM-like substances and has requested that Medsafe investigate and provide a paper exploring the potential to create a class entry. RecommendationThat cardarine should be added to the New Zealand Schedule as a prescription medicine. |
c. |
(8.2.1) SalbutamolBackgroundAt the 66th meeting the Committee considered the change in classification of salbutamol in Australia. The Committee noted that under the current legislation (Section 44 of the Medicines Act 1981) a pharmacist can provide an emergency supply of a medicine however, supply is restricted to New Zealand citizens and residents that have previously been prescribed the medicine. The Committee notes in practice, use of the emergency supply function by pharmacists, and their understanding of the relevant provisions of the Medicines Act may not be consistent. They therefore advise that there would be benefit in the Pharmacy Council communicating guidance of the interpretation of emergency supply. Additionally, the Committee note that the Australian reclassification does not align with current New Zealand asthma guidelines. DiscussionThe Committee noted that this item appeared as a part of the standing harmonisation item on the 66th meeting agenda. The members revisited their discussion from the 66th meeting and reaffirmed that the classification change does not align with current asthma guidelines. The Committee concluded that the provisions of the emergency supply clause in the Medicines Act 1981 provides the same pharmacist-level access of salbutamol without the risk of unintended consequences such as masking uncontrolled asthma. The Committee note that the emergency supply clause is intended for New Zealand citizens and residents that have previously had the medicine before therefore restricts access to patients that do not meet these criteria such as travellers and tourists. The Committee suggested an extension to the emergency supply provisions would better address these specific accessibility issues. The Committee would like to extend their thanks to the Pharmacy council for their commitment, following the 66th meeting, to include information around emergency supply of salbutamol in their newsletter. RecommendationThat there should be no change in classification to salbutamol. |
d. |
(8.2.2) MelatoninBackgroundAt the 66th meeting the Committee requested clarity on the rationale behind the scheduling change made in Australia. DiscussionThe Committee noted that this item appeared as a part of the standing harmonisation item on the 66th meeting agenda. The Committee commented that melatonin had been recently reviewed at the 61st meeting held on 2 November 2018 and that the changes to the Australian schedule were similar to the current scheduling of melatonin in New Zealand. The differences noted in the Australian classification were the reference to a monotherapy and duration of treatment. The Committee reviewed the Australian decision and was not satisfied that the evidence supports a further change to New Zealand’s current scheduling therefore does not recommend harmonising. RecommendationThat there should be no change in classification to melatonin. The Committee considered the current classification conditions to be satisfactory. |
e. |
(8.3.2.c) CalcifediolBackgroundAt the 66th meeting the Committee requested Medsafe provide more information regarding the use of this substance in nutritional supplements. DiscussionThe Committee noted that this item appeared as a part of the standing harmonisation item on the 66th meeting agenda. The Committee reviewed the interim and final decision made by the Australian delegate and agreed to harmonise. RecommendationThat calcifediol should be added to the New Zealand Schedule as a prescription medicine. |
f. |
(8.3.3.b) ArbutinBackgroundAt the 66th meeting the Committee noted that this substance is found in topical cosmetics for reduction of the appearance of spots and hyper-pigmentation. They requested the rationale behind the change made in Australia. DiscussionThe Committee noted that this item appeared as a part of the standing harmonisation item on the 66th meeting agenda. The Committee reviewed the interim and final decision made by the Australian delegate. The members commented that the mild to moderate irreversible toxicity was associated with oral doses of arbutin rather than topical treatments commonly found in cosmetics. The Committee agreed to harmonise. RecommendationThat arbutin should be added to the New Zealand Schedule as a prescription medicine in oral preparations except herbal preparations containing 500 mg or less beta-arbutin per recommended daily dose. |
5.3 |
Record of out of session held in October 2021The Chair noted the out of session that took place to address on the following agenda items that were not discussed at the 65th meeting:
The Committee agreed that the new chemical entities should be classified as prescription medicines and the warning and advisory statements for choline salicylate are added to the labelling statements database. RecommendationThat risdiplam and cemiplimab should be classified as prescription medicines. That the following warning and advisory statements are added to the labelling and statements database for products containing choline salicylate:
Secretary’s Note:The classification changes to risdiplam and cemiplimab were implemented by way of notice in the New Zealand gazette on 2 November 2021. |
6 |
Submissions for reclassification |
6.1 |
Ibuprofen 300mg in powder form –
proposed reclassification from prescription medicine to restricted
medicine
|
7 |
New medicines for classification |
a. |
RipretinibQinlock Tablet 50mg (TT50-10920) Qinlock is a kinase inhibitor indicated for the treatment of adult patients with advanced gastrointestinal stromal tumours (GIST) who have received prior treatment with 3 or more kinase inhibitors, including imatinib. RecommendationThat ripretinib should be added to the New Zealand schedule as prescription medicine. |
b. |
FaricimabVabysmo Solution for injection 120mg/mL (TT50-10940) Vabysmo is a bispecific angiopoietin-2 (Ang-2) and vascular endothelial growth factor (VEGF) inhibitor indicated for the treatment of:
RecommendationThat faricimab should be added to the New Zealand schedule as a prescription medicine. |
8 |
Harmonisation of the New Zealand and Australian schedules |
8.1 |
New chemical entities which are not yet classified in New ZealandThe Committee note that it is standard practice for new chemical entities to be classified as prescription medicines until they have been used widely in a country with an acceptable medicines evaluation process and a good adverse reaction reporting system. |
|
18 May 2021 |
a. |
DeutetrabenazineDeutetrabenazine is the deuterated form of tetrabenazine. The precise mechanism by which deutetrabenazine and tetrabenazine exert their effects in the treatment of tardive dyskinesia and chorea in patients with Huntington's disease is unknown but is believed to be related to the reversible depletion of monoamines (such as dopamine, serotonin, norepinephrine, and histamine) from nerve terminals. The major circulating metabolites (α-dihydrotetrabenazine (HTBZ) and β-HTBZ) of deutetrabenazine, are reversible inhibitors of vesicular monoamine transporter 2 (VMAT2), resulting in decreased uptake of monoamines into synaptic vesicles and depletion of monoamine stores. Deutetrabenzine is indicated for the treatment of chorea associated with Huntington's disease; tardive dyskinesia in adult. From 1 June 2021, deutetrabenzine is classified as a prescription medicine in Australia. RecommendationThat deutetrabenazine should be added to the New Zealand schedule as a prescription medicine. |
b. |
Eslicarbazepine AcetateThe precise mechanisms of action of eslicarbazepine acetate are unknown. However, in vitro electrophysiological studies indicate that both eslicarbazepine acetate and its metabolites stabilise the inactivated state of voltage gated sodium channels, precluding their return to the activated state and thereby preventing repetitive neuronal firing. Eslicarbazepine acetate is indicated in the treatment of partial-onset seizures, with or without secondary generalisation, in adults with newly diagnosed epilepsy; adjunctive therapy in adults, adolescents and children aged above 6 years, with partial- onset seizures with or without secondary generalisation. From 1 June 2021, eslicarbazepine acetate is classified as a prescription medicine in Australia. RecommendationThat eslicarbazepine should be added to the New Zealand schedule as a prescription medicine. |
c. |
LemborexantLemborexant is a competitive antagonist of both orexin receptors, orexin receptors type 1 (OX1R) and orexin receptors type 2 (OX2R), with a higher affinity for OX2R. It belongs to the pharmacologic class of orexin receptor antagonists. The orexin neuropeptide signalling system is a central promoter of wakefulness. Blocking the binding of wake promoting neuropeptides orexin A and orexin B to receptors OX1R and OX2R is thought to suppress wake drive. Antagonism or orexin receptors may also underlie potential adverse effects such as signs of narcolepsy/cataplexy. Lemborexant administered to mice at oral doses greater than 10mg/kg resulted in behaviour characteristic of cataplexy when presented with chocolate. Chocolate is a stimulus that has been demonstrated to increase cataplexy occurrences in narcoleptic mice. Lemborexant is indicated for the treatment of insomnia, characterised by difficulties with sleep onset and/or sleep maintenance in accordance with latest DSM criteria. From 1 June 2021, lemborexant is classified as a prescription medicine in Australia. RecommendationThat lemborexant should be added to the New Zealand schedule as a prescription medicine. |
d. |
LuspaterceptLuspatercept-aamt is a recombinant fusion protein that induces erythroid maturation by binding several endogenous TGF-beta superfamily ligands, diminishing Smad2/3 signaling. In beta-thalassemia and myelodysplastic syndromes, by decreasing abnormally elevated Smad2/3 signaling, hematology parameters associated with ineffective erythropoiesis are improved in mice. Luspatercept has Orphan drug designation for the treatment of myelofibrosis. From 1 June 2021, luspatercept is classified as a prescription medicine in Australia. RecommendationThat luspatercept should be added to the New Zealand schedule as a prescription medicine. |
e. |
TrabectedinTrabectedin binds to the minor groove of deoxyribonucleic acid (DNA), bending the helix to the major groove. This binding to DNA triggers a cascade of events affecting several transcription factors, DNA binding proteins, and DNA repair pathways, resulting in perturbation of the cell cycle. Trabectedin is indicated for the treatment of patients with unresectable or metastatic liposarcoma or leiomyosarcoma who received a prior anthracycline-containing regimen. From 1 June 2021, trabectedin is classified as a prescription medicine in Australia. RecommendationThat trabectedin should be added to the New Zealand schedule as a prescription medicine. |
8.2 |
Decisions by the Secretary to the Department of Health and Aging in Australia (or the Secretary’s Delegate) |
8.2.1 |
Decisions by the Delegate – 19 July 2021 |
|
BilastineThe Schedule 4 (prescription) entry was amended to except when included in Schedule 3. A new entry was created in Schedule 3 (restricted) for bilastine in divided oral preparations containing 20mg or less in adults and adolescents 12 years of age and older. The date of implementation was 1 June 2021. RecommendationThat the New Zealand classification of bilastine should remain unchanged. |
8.2.2 |
Final decision 21 December 2021 |
|
NicotineThe Schedule 4 (prescription) entry was amended to include nicotine in liquid preparations when in Schedule 4. The date of implementation was 1 October 2021. DiscussionThe Committee reviewed the decision made by the Australian delegate and reflected on the different nicotine use in New Zealand. The Committee acknowledges that there are a number of differences between Australia and New Zealand and it has requested further information to consider this classification change in New Zealand. The Committee requests that Medsafe consults with the Vaping Regulatory Authority and provide advice on policy objectives relating to vaping, how nicotine in vaping products is regulated under the Medicines Act 1981, and any potential consequences of a reclassification of liquid nicotine for discussion at the next meeting. RecommendationThat nicotine should be noted for a change in classification and be placed on the 68th meeting agenda to allow for consultation with the Vaping Regulatory Authority. |
9 |
Agenda items for the next meeting
|
10 |
General business |
|
No general business was discussed. |
11 |
Date of next meeting |
A date in April 2022 will be confirmed. |
There being no further business, the Chair thanked members and guests for their attendance and closed the meeting at 11.55am.
This document was prepared and written by Jacinta Patel the Medicines Classification Committee Secretary