Vivoryon Therapeutics N.V. Presents Outstanding Phase 2b Results of Varoglutamstat on Kidney Function at ASN Kidney Week 2024
October 26 2024 - 3:30AM
UK Regulatory
Vivoryon Therapeutics N.V. Presents Outstanding Phase 2b Results of
Varoglutamstat on Kidney Function at ASN Kidney Week 2024
Vivoryon Therapeutics N.V. Presents
Outstanding Phase 2b Results of Varoglutamstat on Kidney Function
at ASN Kidney Week 2024
- Selected for late-breaking oral
presentation at ASN kidney week, the world’s premier nephrology
meeting
- Results presented show a
statistically significant and clinically meaningful improvement of
the prospectively defined kidney function parameter
eGFR1 by 3.4mL/min/year (p<0.0001)
in the varoglutamstat arm compared to placebo
- Results in the subgroup of
patients with diabetes2 showed an
8.2mL/min/year difference in favor of varoglutamstat
(p=0.02)
- The results were consistent in
several sensitivity analyses including using the CKD-EPI 2021
formula for both creatinine and cystatin-C
- Varoglutamstat demonstrated an
excellent safety and tolerability profile and there were no signs
of increased proteinuria
- A new Phase 2 study is in
planning to confirm the effect in patients with DKD3
stage 3b and 4
Halle (Saale) / Munich, Germany, October
26, 2024 – Vivoryon Therapeutics N.V. (Euronext Amsterdam:
VVY; NL00150002Q7) (Vivoryon), a clinical stage
company focused on the discovery and development of small molecule
medicines to modulate the activity and stability of pathologically
altered proteins, today announced highlights from a late-breaking
oral presentation held yesterday, October 25, 2024, at the American
Society of Nephrology (ASN) Kidney Week 2024 in San Diego,
California.
The presentation by the Company’s CEO, Frank
Weber, M.D. titled “Varoglutamstat Increases Glomerular Filtration
in Elderly Patients without Signs of Proteinuria and Potentially
Offers a New Approach to Treat Diabetic Kidney Disease (DKD)”
featured Phase 2 clinical study data substantiating the opportunity
to further develop varoglutamstat, Vivoryon’s Phase 2
investigational medicine with the potential to improve kidney
function, in people with kidney disease.
“We’re privileged to have been accepted to share
the exciting results of varoglutamstat on kidney function with so
many scientific and medical experts in the kidney field.
Varoglutamstat showed statistically significant and clinically
meaningful improvements of eGFR versus placebo and a sustained
improvement of eGFR above baseline, potentially indicating partial
recovery of the kidney. We are grateful for many fruitful
discussions and extremely encouraged by the positive reactions we
received from the community,” said Frank Weber, M.D., CEO of
Vivoryon. “The efficacy and safety data presented at ASN represent
a unique profile for an oral product for treating kidney disorders
and guide the future development of varoglutamstat. Our primary
focus is delivering a much-needed novel treatment option for
patients suffering from DKD. Beyond this, we see potential for
varoglutamstat across a broad range of kidney diseases including
rare diseases affecting kidney function, such as Fabry disease and
Alport syndrome.”
Presentation Highlights
Background:
- Varoglutamstat is a specific and
selective inhibitor of glutaminyl cyclases and confers a novel
mechanism of action that attenuates inflammation and fibrosis
through reduction of pyroglutamized versions of chemokines and
pro-fibrotic peptides, thereby positively impacting kidney
function.
- Assessment of progression of kidney
dysfunction as measured by the eGFR slope4 was included
prospectively in VIVIAD (NCT04498650), Vivoryon’s Phase 2b
multicenter, randomized, double-blind, placebo-controlled, parallel
group dose-finding study in 259 patients in Alzheimer’s
disease.
- The average age of participants in
VIVIAD was >68 years, dosing was twice-daily with either 300mg
or 600mg varoglutamstat, or placebo and treatment duration was
48-96 weeks; key kidney-related study features included a mean
baseline eGFR of ~80mL/min/1.73m2, eGFR, urine dipstick
and vital signs measured every 12 weeks; the diabetes subgroup
comprised ~12% of VIVIAD patients.
Compelling efficacy and safety data in elderly people at
risk for kidney disease:
- eGFR improved
significantly for varoglutamstat compared to placebo and above
baseline in both total population and diabetes subgroup, with the
latter revealing a substantially higher treatment
effect5 of >8.2mL/min/1.73m2/year (p=0.02;
varoglutamstat n=20 / placebo n=12) compared to the overall VIVIAD
study population (3.4mL/min/1.73m2/year (p<0.001;
varoglutamstat n=141 / placebo n=117)).
- Results and effect size were
consistent using a set of diverse and validated methods for eGFR
assessment (2021 CKD-EPI cystatin C, 2021 CKD-EPI
creatinine-cystatin C 2021 CKD-EPI creatinine,
MDRD6).
- Urine dipstick analysis showed no
evidence of increased proteinuria in the treatment group compared
to placebo, with the majority of study participants having no
proteinuria through all time points measured in the study.
- Robust safety data confirmed
varoglutamstat’s excellent safety profile consistent across two
years study duration with no adverse kidney effects and no
meaningful differences observed in renal and metabolic systems
adverse events in both total population and diabetes subgroup.
Next steps:
- Placebo-controlled Phase 2 study in
stage 3b/4 DKD patients on top of SoC in planning to confirm the
results to date and investigate additional endpoints including
albuminuria/proteinuria, inflammation and fibrosis-related
biomarkers.
- Pre-clinical
investigation of additional rare/orphan kidney disorders (Alport
syndrome, Fabry disease).
1 Estimated glomerular
filtration rate (eGFR), a validated measure of kidney function, was
calculated as a slope analysis across two years taking all
available data into account.
2 Diabetes subgroup defined as patients
having at baseline either medical history of diabetes (type 1 or 2)
and/or comedication with drugs used in diabetes and/or untreated
with an HbA1c > 6.5%.
3 The timing and execution of the planned
Phase 2 study in diabetic kidney disease is subject to additional
funding / partnership. 4
Measuring the eGFR slope via random coefficients
(RC) analysis was the primary efficacy
endpoint in recent FDA approvals in CKD, as well as in many ongoing
Phase 3 studies. 5
Treatment effect – the between-group difference in eGFR slope
between varoglutamstat and placebo. 6
Estimated glomerular filtration rate based on creatinine and
calculated using modification of diet in renal disease (MDRD)
method.
###
Varoglutamstat in Kidney
Disease
Varoglutamstat (PQ912) is a proprietary, potent and selective
inhibitor of human glutaminyl cyclases QPCT and QPCTL with
therapeutic potential in indications including inflammatory and
fibrotic diseases, neurodegenerative diseases, cancer and others.
Initially advancing development aiming to treat Alzheimer’s disease
(AD), varoglutamstat has been investigated in a number of different
clinical studies, all of which have consistently demonstrated a
favorable safety and tolerability profile both in healthy
volunteers and patients with AD. Based on the known
anti-inflammatory activity of varoglutamstat, the protocol for the
Phase 2 VIVIAD study in AD, which was completed in the first half
of 2024, included the investigation of kidney function and
measurement of biomarkers of kidney inflammation and fibrosis to
explore the role of QPCT/L inhibition on kidney function. Although
patients in VIVIAD were selected for their AD status and not for
their kidney function level, many of them had reduced kidney
function due to age and/or comorbidities. Analysis showed a
statistically significant benefit of varoglutamstat on a
prospectively defined key kidney function endpoint (eGFR) and a
significant reduction of the pro-inflammatory cytokine pE-CCL2. A
substantially higher treatment benefit of varoglutamstat on eGFR
was observed in a post-hoc diabetes subgroup, triggering plans to
advance varoglutamstat into Phase 2 study in DKD, which is
currently in planning.
About Vivoryon Therapeutics
N.V.
Vivoryon is a clinical stage biotechnology company focused on
developing innovative small molecule-based medicines. Driven by its
passion for ground-breaking science and innovation, the Company
strives to change the lives of patients in need suffering from
severe diseases. The Company leverages its in-depth expertise in
understanding post-translational modifications to develop medicines
that modulate the activity and stability of proteins which are
altered in disease settings. The Company has established a pipeline
of orally available small molecule inhibitors for various
indications including Alzheimer’s disease, inflammatory and
fibrotic disorders, including of the kidney, and cancer.
www.vivoryon.com.
Vivoryon Forward Looking
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trends, the economy and other future conditions. The
forward-looking statements involve a number of known and unknown
risks and uncertainties. These risks and uncertainties and other
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effects of the plans and events described herein. The Company’s
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should be placed on such forward-looking statements. This press
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press release, including any forward-looking statements, speaks
only as of the date of this press release. The Company does not
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be disclosed by law.
For more information, please contact:
Investor Contact
Vivoryon Therapeutics N.V.
Dr. Manuela Bader, Director IR & Communication
Email: IR@vivoryon.com
Media Contact
Trophic Communications
Valeria Fisher or Verena Schossmann
Tel: +49 175 8041816 / +49 151 219 412 77
Email: vivoryon@trophic.eu
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