SPP100 (RASILEZ): POOLED DATA ANALYSIS CONFIRMS EFFICACY AND SAFETY IN OVER 7000
HYPERTENSIVE PATIENTS TREATED WITH FIRST-IN-CLASS RENIN INHIBITOR
Monotherapy and co-administration therapy data presented at World Congress of Cardiology
Basel/Switzerland and Bridgewater NJ/USA, 4 September 2006
Speedel (SWX: SPPN) welcomes the pooled analysis of positive Phase II/III data on SPP100 ( Rasilez1)
in the treatment of hypertension both as monotherapy and in co-administration with other antihypertensives.
This first pooled analysis was presented today by Novartis, at the World Congress of
Cardiology (WCC) in Barcelona. Pooled data were available from 7 randomised, double-blind multicentre
studies on 7060 patients with mild-to-moderate hypertension treated with SPP100 over 6-52 weeks.
Dr. Jessica Mann, Speedel Medical Director, said : "This is the first pooled analysis in which the efficacy
and safety of SPP100 in over 7000 patients have been assessed, reconfirming that SPP100 provides
highly effective and consistent blood pressure lowering with placebo-like tolerability in a broad range of
patients with mild-to-moderate hypertension. The data shows how SPP100 is an effective antihypertensive
independent of age, race and gender.”
SPP100 is the first-in-class once daily orally active renin inhibitor that Speedel successfully developed
through Phase I and II clinical trials before Novartis exercised its license-back option in 2002. The U.S.
Food and Drug Administration (FDA) in April 2006 accepted for review Novartis’ new drug application
(NDA) for SPP100 as a treatment for hypertension both as monotherapy and in co-administration.
Antihypertensive efficacy and safety of the oral renin inhibitor SPP100 in patients with
hypertension: a pooled analysis 2
• SPP100 provides dose-dependant blood pressure (BP) reductions at doses of up to 300mg
• Antihypertensive effects of SPP100 are consistent across the placebo-controlled studies
• SPP100 75mg-600mg provides effective and comparable BP reductions in elderly and young patients
and in both sexes
• Addition of SPP100 to other classes of antihypertensive therapy consistently provides additional BP
reductions
• SPP100 150mg and 300mg exhibit placebo-like tolerability and safety
Additionally at the WCC in Barcelona today, investigators presented four posters of data from Phase III clinical
trials of SPP100 in monotherapy and in co-adminstration therapy with a diuretic ( HCTZ), a calcium channel
blocker (amlodipine), and an ACE inhibitor (ramipril).The conclusions of the investigators are highlighted below:
SPP100 a novel renin inhibitor is well tolerated and has sustained BP-lowering effects alone or in
combination with HCTZ during long-term (52 weeks) treatment of hypertension3
• SPP100 as monotherapy and in combination with HCTZ is effective and well tolerated in the long-term
treatment of hypertension (12 months)
• SPP100 provided sustained 24hr BP control
• Patients in the study taking SPP100 avoided rebound high blood pressure, a potentially dangerous
condition
• Even after treatment withdrawal, patients treated with SPP100 continued to show benefits of reduced
blood pressure for several weeks
SPP100 a novel renin inhibitor, provides long term suppression of the renin system, when used alone or
in combination with hydrochlorothiazide, in the treatment of hypertension 4
• SPP100 lowered plasma renin activity (PRA) by a similar extent whether given as monotherapy or in
combination with HCTZ
• Long term treatment alone or in combination with HCTZ produced sustained suppression of the renin
system as shown by PRA reductions
• In patients switched to placebo during the withdrawal period, BP rose only gradually towards baseline,
indicating that rebound hypertension does not occur on withdrawal of SPP100
SPP100 as add on to amlodipine, provides significant additional blood pressure lowering without
increased oedema with doubling the amlodipine dose5
• The addition of SPP100 150mg to amlodipine 5mg provided statistically significant reductions in blood
pressure compared to amlodipine 5mg alone
• There was a higher incidence of oedema (water retention) using amlodipine 10mg monotherapy than
using combination therapy with SPP100 or amlodipine 5mg alone
SPP100, a novel renin inhibitor for treatment of hypertension, enhances renin system suppression by
reducing plasma renin activity alone or in combination with ramipril in patients with diabetes 6
• SPP100 300mg provided significantly superior reductions in MSSBP7 compared with ramipril 10mg
Combination treatment provided a clinically relevant additional BP reduction over that achieved using
monotherapy with ramipril
• The ability of SPP100 to suppress PRA when administered in combination with an ACE inhibitor may be
clinically important, as increased generation of angiotensin I by renin is associated with ‘escape’ from
the effects of ACE inhibitor monotherapy in patients with diabetes
• The combination of SPP100 and ramipril was well tolerated, and appeared to reduce the incidence of
ACE inhibitor-induced cough
Speedel believes that SPP100 has a five-year lead over the next generation of renin inhibitors being developed
in the industry. Speedel’s own family of renin inhibitors includes SPP635 currently in Phase I with results due in
the second half of 2006, followed by the SPP1100 series currently in toxicology testing with a compound due for
entry into man at the end of 2006, and the SPP800 series currently in late-stage pre-clinical profiling.
About SPP100 (aliskiren, Rasilez8)
SPP100 (aliskiren, Rasliez) is the first-in-class oral renin inhibitor. The development of SPP100 is the result of over 20
years of research on renin. Renin is the key enzyme at the top of the Renin Angiotensin System (RAS), one of the key
regulators of blood pressure. The RAS is a cascade, starting with renin, leading to angiotensin I and finally to angiotensin II.
Angiotensin-converting enzyme inhibitors (ACE-Is) and angiotensin II receptor antagonists (ARBs) have been developed to
block this system "down stream" and have shown clinical efficacy in patients with hypertension and other cardiovascular
diseases.
By inhibiting renin at the top of the RAS, SPP100 decreases the system’s activity, as measured by Plasma Renin Activity.
PRA is believed to be very important in end-organ protection (e.g. heart and kidney). PRA is an independent and direct
surrogate marker for several cardio-renal diseases, such as myocardial infarction and chronic renal disease. It is only a
renin inhibitor that lowers PRA efficiently whereas most current leading anti-hypertensive drug classes such as ACE-Is and
ARBs increase PRA levels.
Speedel in-licensed SPP100 from Novartis in 1999, and successfully completed 18 clinical trials through Phase I and II in about 500 patients and healthy volunteers. Based on the results generated during this programme, Novartis exercised a
license-back option in 2002, and in March 2004 Novartis started trials with SPP100 in Phase III as monotherapy for
hypertension and in Phase IIb as combination therapy. Phase III trials are ongoing in the US, EU, and Japan, with first
regulatory submission in the US already filed in Q1 2006 and planned in the EU during 2006.
Speedel believes that it is the first company to establish successfully a clinical proof of concept in Phase II and to have developed and filed for patent protection a commercially viable manufacturing process for a renin inhibitor, an area of
industry research for over 20 years. In a Phase II study of 200 patients conducted by Speedel, it was demonstrated that
SPP100 achieves dose-dependent blood pressure reduction. The study also showed that 150mg and 300mg SPP100 once
daily were comparable to Losartan 100mg, which is double the starting dose of this ARB (Stanton, Jensen, Nussberger,
O’Brien, Hypertension.2003; 42: 1137-1143).
About Hypertension
Hypertension is a common disorder in which blood pressure is abnormally high, placing undue stress on the heart, blood
vessels and other organs such as the kidney and the brain. Blood pressure is determined in two phases as the heart
contracts and relaxes. Systolic blood pressure represents the force that blood exerts on the walls of arteries as the heart
contracts to pump out blood. Diastolic blood pressure represents the force as the heart relaxes to allow the blood to flow into the heart.
Due to its wide prevalence and impact on cardiovascular health, hypertension is a major cause of disease and death in
Europe and North America. More than one in three Europeans and North Americans over the age of 35 suffers from
hypertension – but for the vast majority of patients who undergo hypertension treatment, the causes of high blood pressure are unknown. More than 40 % of patients undergoing treatment with current therapies do not reach targeted blood pressure levels, and so there is a considerable unmet medical need.
The latest potential therapeutic agents for hypertension are renin inhibitors. Renin is an enzyme produced in the kidneys in
response to reduced renal perfusion. Through a cascade of biological events, renin acts to bring about sodium retention, an increase in blood pressure, and restoration of renal perfusion, which shuts off the signal for renin release. For hypertensive individuals, renin inhibitors are currently being investigated as a therapy that may provide benefits over current therapies to reduce blood pressure, decrease salt retention and may protect end organs such as the kidney, heart and brain.
About Speedel
Speedel is a public biopharmaceutical company that seeks to create value for patients, partners and investors by developing
innovative therapies for cardiovascular and metabolic diseases. Speedel is a world leader in renin inhibition, a promising new
approach with significant potential for treating cardiovascular diseases. Our lead compound SPP100 (Rasilez9), the first-in-class renin inhibitor, is partnered with Novartis for Phase III development and commercialisation in hypertension. Our pipeline covers three different modes of action, and in addition to SPP100, includes SPP301 in Phase III, SPP200 in Phase II, SPP635 in Phase I, and several pre-clinical projects.
Speedel develops novel product candidates through focused innovation and smart drug development from lead identification to the end of Phase II. We either partner with big pharma for Phase III and commercialisation in primary-care indications, or we may ourselves complete Phase III development in specialist indications. Candidate compounds for development and the company’s intellectual property come from our late-stage research unit Speedel Experimenta and from in-licensing.
Our team of approximately 70 employees, including over 30 experienced pharmaceutical scientists, is located at our headquarters and laboratories in Basel, Switzerland and at offices in New Jersey, USA and Tokyo, Japan. In March 2006 the company raised gross proceeds of CHF83.95 million (approximately EUR 53m or USD 64m) through the sale of 500,000 treasury shares. As a private company,we have previously raised gross proceeds of CHF 239 million (approximately EUR 154 million or USD 183 million) from private placements of equity securities and two convertible loans and we have had total revenues, principally from milestone payments, of CHF
57.7 million (approximately EUR 37 million or USD 44 million. The company’s shares were listed on the SWX Swiss Exchange under the symbol SPPN on 08 September 2005.
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