Below is the product datasheet. This has been provided by the manufacturer and should always be provided with the medication. Introduction 
Company name: MSD Animal Health
Address: Walton Manor
Walton
Milton Keynes
MK7 7AJ
Telephone: 01908 685685 (Customer Support Centre)
Fax: 01908 685555
Email: vet-support.uk@merck.com
Website: www.msd-animal-health.co.uk
Presentation
Vasotop 0.625 mg tablets: orange oblong flavoured tablets half scored on
both sides. Each tablet contains 0.625 mg ramipril and 1.0 mg brown
ferric oxide (E 172).
Vasotop 1.25 mg tablets: beige oblong flavoured tablets half scored on both sides. Each tablet contains 1.25 mg ramipril.
Vasotop 2.5 mg tablets: yellow oblong flavoured tablets half scored on
both sides. Each tablet contains 2.5 mg ramipril and 0.5 mg yellow
ferric oxide (E 172).
Vasotop 5 mg tablets: light pink oblong flavoured tablets half scored on
both sides. Each tablet contains 5 mg ramipril and 0.25 mg red ferric
oxide (E 172).
Uses
For the treatment of congestive heart failure (NYHA decompensation
grades II-IV) in dogs. Vasotop can be used in combination with diuretics
and the cardiac glycosides, digoxin or methyl-digoxin.
Administration of ramipril in patients with congestive heart failure
improves cardiovascular function, the related clinical signs and the
prognosis. Ramipril has also been shown to reduce the mortality rate
among patients with persistent or transient heart failure following an
acute myocardial infarction (man, dog).
Dosage and administration
The therapeutic dose in the dog is 0.125 mg ramipril per kg bw per day.
Depending on the severity of pulmonary congestion the dose may be
increased after 2 weeks to 0.25 mg ramipril per kg bw per day. Treatment
is once daily by mouth.
Dosage Schedule:
| Bodyweight
| Vasotop Standard dose
| (kg)
| 0.625
| 1.25
| 2.5
| 5
| ≤ 2.5
| ½
|
|
|
| 2.6 - 5
| 1
|
|
|
| 6-10
|
| 1
|
|
| 11-20
|
|
| 1
|
| 21-40
|
|
|
| 1
| 41-50
|
| 1
|
| 1
| 51-60
|
|
| 1
| 1
|
The table provides a suggested tablet regime only. To ensure accurate
dosing, each individual should be carefully weighed before calculating
the standard or double dose to be administered.
The product may also be used in combination with the diuretic furosemide
and/or the cardiac glycosides digoxin or methyl-digoxin.
See Dosage schedule.
Contra-indications, warnings, etc
Not to be used in clinical cases of vascular stenosis (e.g. aortic stenosis) or obstructive hypertrophic cardiomyopathy.
Substances that deplete blood volume, such as diuretics, or which
vasodilate, such as angiotensin converting enzyme (ACE) inhibitors, may
contribute to lowering systemic blood pressure. This may result in
pre-renal uraemia (azotaemia). Renal function should be monitored both
before and seven days after commencement of treatment with ACE
inhibitors. This also applies when the dosage of an ACE inhibitor or of a
concurrently administered diuretic is increased. It is advisable to
periodically monitor renal function throughout treatment.
No studies have been carried to assess the use of the drug in pregnancy
or lactation in bitches. ACE inhibitors have been found to be
teratogenic in the second and third trimesters in other species. An
angiotensin converting enzyme is known to be critical to the development
of the neonatal kidney, this product should not be used in pregnancy or
lactation.
At the start of treatment with ACE inhibitors or after a dosage
increase, reduced blood pressure can occur in rare cases, which may
manifest itself by fatigue, lethargy or ataxia. In such cases treatment
should be discontinued until the patients condition has returned to
normal and then resumed with 50% of the original dose. As high doses of
diuretics can also lead to a fall in blood pressure, the concurrent
administration of diuretics in the early phase of treatment with ACE
inhibitors should be avoided in these patients.
If signs of hypotension occur, treatment with Vasotop should be
suspended until fluid and electrolyte status is corrected. Treatment
with Vasotop should then be continued at 50% of the original dose. In
patients at risk of hypotension, it is advisable to introduce Vasotop
gradually over one week (starting with half the therapeutic dose).
Diurectics and a low sodium diet both potentiate the effect of ACE
inhibitors by activating the renin-angiotensin-aldosterone system. High
doses of diuretics and a low-sodium diet should therefore be avoided
during treatment with ACE inhibitors to prevent hypotension (with
clinical signs such as apathy, ataxia, rarely syncope or acute renal
failure). In patients treated concurrently with Vasotop and frusemide,
the dose of diuretic can be reduced to achieve the same diuretic effect
as with frusemide alone.
Do not administer potassium-sparing diuretics.
The concomitant administration of ACE inhibitors with non-steroidal
anti-inflammatory drugs (NSAIDS) leads to poor autoregulation of the
glomerular blood pressure and can therefore trigger acute renal failure.
Operator warnings:
Pregnant women should take special care to avoid accidental exposure,
because ACE inhibitors have been found to affect the unborn child during
pregnancy in humans. Wash hands after use. In case of accidental
ingestion by children seek medical advice immediately and show the label
to the doctor.
Withdrawal period
Not applicable.
For animal treatment only. Keep out of reach and sight of children.
Pharmaceutical precautions
Do not store above 30°C. Store in a dry place. Keep container in outer carton.
After each opening, replace the cap tightly.
Do not remove the desiccant capsule.
Use before the expiry date printed on the pack.
Dispose of used packaging in the household refuse. Unused product should be returned to the veterinary surgeon.
Legal category
POM-V
Packaging Quantities
All tablet strengths:
1 x 28 tablets in HD polyethylene container per box.
3 x 28 tablets in HD polyethylene container per box.
6 x 28 tablets in HD polyethylene container per box.
Not all pack sizes may be marketed.
Further information
Ramipril is rapidly and completely absorbed in the gastrointestinal
tract after oral administration. Ramipril is a pro-drug and is
metabolised in the liver to its active metabolite, ramiprilat. This
conversion may be reduced in dogs with impaired liver function.
Ramiprilat inhibits angiotensin-converting enzyme (ACE). This enzyme
catalyses the conversion of angiotensin I to angiotensin II in blood
plasma and in vascular endothelial tissues and degrades bradykinin. As
angiotensin II acts as a strong vasoconstrictor and bradykinin as a
vasodilator, the net effect of ramipril administration is systemic
vasodilation. Angiotensin II also causes the release of aldosterone
secretion. This in turn leads to an increase in the serum potassium
concentration.
Inhibition of tissue ACE in the heart results in locally reduced levels
of angiotensin II and in potentiation of Bradykinin effects. Angiotensin
II induces cell proliferation in smooth muscle, while bradykinin leads
to increase in local prostacyclin (PGI2) and
nitric oxide (NO), both inhibiting smooth muscle proliferation. The
effects of local ACE inhibition act synergistically in reducing
myotropic factors and result in distinct reduction of cardiac and
vascular smooth muscle cell proliferation. In this way ramipril prevents
or reduces, with lasting effect, myogenous hypertrophy in patients with
congestive heart failure (CHF) and results in reduction of peripheral
vascular resistance.
The plasma ACE activity was measured as the principal criterion of the pharmacodynamic effect.
After oral administration of Ramipril a significant inhibition of this
activity occurs quickly and gradually increases again during the dosage
interval, reaching of 50% of the initial value by 24 hours post
administration.
Marketing authorisation number(s) Vasotop 0.625 mg tablets
Vasotop 1.25 tablets
| Vm 01708/4500
Vm 01708/4403
| Vasotop 2.5 tablets
| Vm 01708/4404
| Vasotop 5 tablets
| Vm 01708/4400
|
| 
