Cilazapril with hydrochlorothiazide is a fixed-dose combination medicine (cilazapril 5mg + hydrochlorothiazide 12.5
mg) for the treatment of patients with hypertension when dual antihypertensive treatment is indicated.1 Apotex,
the supplier of Apo-Cilazapril/Hydrochlorothiazide, has announced that it will no longer be able to supply this medicine
in New Zealand.2 Apo-Cilazapril/Hydrochlorothiazide is the only registered brand of cilazapril with hydrochlorothiazide
in New Zealand, therefore this decision will mean that:
- From 1 March, 2020: cilazapril with hydrochlorothiazide will no longer be available funded for patients
that have never been prescribed this medicine before
- Prescribers should ensure no new patients are started on this medicine from 1 March, 2020
- Prescribers will need to endorse* any prescriptions for patients who were taking this medicine prior
to 1 March, 2020 and should begin transitioning them to alternative treatments
- From July, 2020: current cilazapril with hydrochlorothiazide stocks are anticipated to run out
- Patients still receiving this combination product after 1 March, 2020 will need to have switched to an alternative
regimen by July, 2020
* Pharmacists may annotate a prescription of cilazapril with hydrochlorothiazide as endorsed if a record exists of prior
dispensing, if required.
Patients with hypertension currently taking cilazapril with hydrochlorothiazide will need to transition to an alternative
antihypertensive regimen; the decision on the replacement regimen should be individualised. Most patients are likely to
prefer to continue using another fixed-dose combination because they have established a familiar dosing routine, and it
is likely to have a comparable clinical effect. However, other options include transitioning to two separate antihypertensives,
or in rare cases, de-escalating treatment to use of a single antihypertensive.
Transitioning to another fixed-dose combination
As of February 2020, there are two fully funded fixed-dose combination antihypertensives available in New Zealand which
are suitable alternatives to cilazapril with hydrochlorothiazide (Table 1).1 Both also include hydrochlorothiazide*,
combined with either an ACE inhibitor (quinapril) or an angiotensin II receptor blocker (ARB; losartan). When transitioning
a patient from one fixed-dose combination to another, it is recommended that their blood pressure is checked one month
after switching, and then at least once every three to six months after blood pressure targets have been achieved, depending
on the patients characteristics and level of cardiovascular disease (CVD) risk.3
*See: “Consider the potential increased risk of non-melanoma skin cancers when
prescribing hydrochlorothiazide-containing medicines”
Table 1. Fully funded fixed-dose ACE inhibitor-/ARB-thiazide diuretic combinations for the treatment of hypertension 1
| Fixed-dose combination medicine |
Approximate equivalent strength* |
Dosing regimen |
Quinapril with hydrochlorothiazide
(brand name: Accuretic) |
20 mg† quinapril with 12.5 mg hydrochlorothiazide |
Initially one 10/12.5 mg tablet, once daily, increased to one 20/ 12.5 mg tablet, once daily, if necessary |
Losartan with hydrochlorothiazide
(brand name: Arrow-Losartan & Hydrochlorothiazide) |
50 mg losartan with 12.5 mg hydrochlorothiazide |
Initially one 50/12.5 mg tablet, once daily, increased to 2 tablets (i.e. 100/25 mg), once daily, if necessary |
* Compared with 5 mg cilazapril/12.5 mg hydrochlorothiazide
† Quinapril with hydrochlorothiazide is also available in a 10 mg (quinapril) with 12.5 mg (hydrochlorothiazide) preparation
Transitioning to two separate antihypertensive medicines
Although prescribing fixed-dose antihypertensive combinations is a valuable strategy to promote medicine adherence,
some patients may be satisfied with transitioning to two separate medicines as it allows for a specific choice and customised
dosing of the antihypertensives used.
ACE inhibitors/ARBs, calcium channel blockers and thiazide (and thiazide-like) diuretics are all first line antihypertensives with a comparable
blood pressure lowering effect.3 The choice of antihypertensive depends on patient characteristics, co-morbidities,
age, tolerance, concomitant medicine use and patient preference. Beta-blockers should only be prescribed as an add-on
for resistant hypertension despite use of the three first line medicines, or if there is a specific indication, e.g. atrial
fibrillation.3
For further information on antihypertensive medicine options, visit the NZ formulary (NZF) at:
https://nzf.org.nz/nzf_1168
Cilazapril will still be available, but an alternative ACE inhibitor should be considered
The decision to stop supplying cilazapril with hydro-chlorothiazide does not apply to cilazapril tablets alone, and
supplies of cilazapril have been secured until 2022. However, New Zealand is one of the few countries where cilazapril
is used frequently.4 Given that there is only one manufacturer of the active ingredient in cilazapril, any
supply issues in the future would significantly impact patients prescribed this medicine. Therefore, if treatment with
two separate antihypertensives is preferred, prescribers should consider using an alternative subsidised ACE inhibitor
if appropriate, e.g. enalapril, lisinopril, perindopril, quinapril.
For further information on the prescribing and dosing of ACE inhibitors, see: “Prescribing
ACE inhibitors: time to reconsider old habits”
Consider prescribing an ACE inhibitor with a dihydropyridine calcium channel blocker for patients with a high CVD-risk.
In general, any combination of first-line antihypertensive medicines is likely to be suitable for patients with uncomplicated
hypertension (i.e. without co-morbidities). However, results from the ACCOMPLISH trial suggest that the combination of
an ACE inhibitor/ARB with a dihydropyridine calcium channel blocker, e.g. amlodipine or felodipine, is superior for reducing
cardiovascular events in patients with a high CVD risk, compared with an ACE inhibitor/ARB-thiazide diuretic combination.5
Transitioning to a single antihypertensive medicine
Although the majority of patients will require continued use of two antihypertensives, this necessary transition may
be an appropriate time to trial switching to a single first-line antihypertensive in some patients, e.g. long-term users
of fixed-dose combinations that have applied major lifestyle changes and are consistently achieving blood pressure targets.
Continued use of an ACE inhibitor is a suitable option for many patients, and if this decision is made then an alternative
to cilazapril should be considered (as previously described). Patients should have their blood pressure and renal function
checked one to three months following the switch to a single antihypertensive to evaluate whether they should continue
at their current dose, require a dose adjustment, or need to transition back to use of two antihypertensives.3
Consider the potential increased risk of non-melanoma skin cancers when prescribing hydrochlorothiazide-containing medicines
Two Danish case-control studies have reported that hydrochlorothiazide increases the risk of non-melanoma skin cancer,
specifically squamous cell carcinoma (SCC), SCC of the lip and basal cell carcinoma (BCC).6, 7 Although the
mechanism is unknown, this association may be due to the photosensitising effect of hydrochlorothiazide. In contrast,
a series of Taiwanese case-control studies did not demonstrate an association between hydrochlorothiazide use and the
risk of lip cancer, non-lip non-melanoma skin cancer and melanoma.8 These conflicting findings may be explained
by differences in the study populations, i.e. different skin tones and therefore different susceptibility to skin cancer,
the dose of hydrochlorothiazide used and cultural practices relating to sun exposure.
While further studies are needed to investigate the association between hydrochlorothiazide and the risk of non-melanoma
skin cancers, it is recommended that this potential risk is discussed when deciding on an antihypertensive regimen.9 If
a hydrochlorothiazide-containing medicine is selected, patients should be made aware of, and consistently adhere to, SunSmart
practices and perform regular self-checks of their skin for any suspicious looking lesions.9 For patients
who have experienced previous non-melanoma skin cancer, the risks and benefits of hydrochlorothiazide treatment should
be thoroughly discussed, taking into consideration other treatment options.9
There is currently insufficient evidence to determine if the increased risk of non-melanoma skin cancer is a thiazide class effect.
If an alternative thiazide (or thiazide-like) diuretic is preferred, then indapamide, chlortalidone or bendroflumethiazide are potential options.
Indapamide and chlortalidone have the strongest evidence of effectiveness, and the 2019 NICE guidelines state that indapamide is preferred
if a decision is made to switch diuretics.10 For patients where chlortalidone is selected, closer monitoring of serum electrolytes may be
warranted as a US observational study reported an increased risk of electrolyte disturbances with chlortalidone compared with hydrochlorothiazide.11
However, further investigation is required as the dose of hydrochlorothiazide used in this study was 25 mg (twice the amount contained in
currently available fixed-dose combinations in New Zealand) and the cohort was restricted to patients aged less than 70 years.11
For further information, see “Hydrochlorothiazide: risk of non-melanoma skin cancer” at:
https://www.medsafe.govt.nz/safety/Alerts/Hydrochlorothiazide.asp
