Vivoryon Therapeutics N.V. Reports H1 2024 Progress Marked by
Compelling Kidney Function Data and Execution of Strategy to
Advance Varoglutamstat in Kidney Disease
Vivoryon Therapeutics N.V. Reports H1
2024 Progress Marked by Compelling Kidney Function Data and
Execution of Strategy to Advance Varoglutamstat in Kidney
Disease
- Primary focus is developing
varoglutamstat, a Phase 2 investigational medicine with potential
to improve kidney function in patients with kidney disease
- Statistically significant
benefit of varoglutamstat on prospectively defined key kidney
function endpoint (eGFR1) and
significant reduction of pro-inflammatory cytokine pE-CCL2 observed
in VIVIAD Phase 2b AD study
- Substantially higher treatment
benefit of varoglutamstat on eGFR observed in post-hoc diabetes
subgroup2 triggering plans to advance
varoglutamstat into Phase 2 study in
DKD3
- Gained further insight into AD
results through clear evidence of differences between kidney and AD
outcomes from PK/PD analysis and new target occupancy
information
- Management to host a conference
call today at 3:00pm CEST (9:00am EDT)
- Vivoryon to host a virtual Kidney Disease KOL (Key Opinion
Leaders) webcast on Monday, September 30 at 3:00 pm CEST (9:00 am
EDT) to elaborate on varoglutamstat’s potential in kidney disease
with an emphasis on DKD
Halle (Saale) / Munich, Germany,
September 12, 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 financial results for the six-month
period ended June 30, 2024, and provides a corporate update. The
report is available on the Company’s website
https://www.vivoryon.com/financial-information/.
“The VIVIAD Phase 2b study showed outstanding
results in improving kidney function and we made strong progress
during the first half of 2024 in forging a new development strategy
for varoglutamstat in diabetic kidney disease (DKD),” said Frank
Weber, MD, CEO of Vivoryon. “In parallel, we advanced
pharmacokinetic and biomarker analyses which demonstrate a strong
dose response of varoglutamstat on kidney function improvement.
Furthermore, as we continue the evolution of our understanding of
the Alzheimer’s disease (AD) VIVIAD results, we have generated the
first evidence that varoglutamstat activity is required in the
cells of the brain – not only in the cerebrospinal fluid - to stop
the pathological process of pE-Abeta production.” He concluded,
“The VIVIAD data demonstrate varoglutamstat has an excellent safety
and tolerability profile, provide strong support for our
understanding of the potential of QPCTL inhibitors in inflammatory
and fibrotic diseases and lay the foundation for our strategic
shift towards kidney disease based on the outstanding effect we
observed on eGFR.”
H1 2024 and Post-Period
Updates
Strategic shift towards a focus on
inflammatory and fibrotic diseases
A significant positive effect of varoglutamstat
on kidney function observed in the VIVIAD Phase 2b study in AD
underpins the strategic shift to inflammatory and fibrotic
diseases. In April 2024, Vivoryon announced this strategic shift
following the announcement in March 2024 that the VIVIAD Phase 2b
study did not achieve its primary and key secondary endpoints in
early AD.
The VIVIAD protocol prospectively specified
measurement of kidney function by estimated glomerular filtration
rate (eGFR), a primary endpoint in many development programs of
kidney disorders, and additional biomarkers, in order to further
investigate this potential activity.
Key priorities now include:
- Preparing for a
proposed Phase 2 clinical study for varoglutamstat in diabetic
kidney disease (subject to additional funding and/or
partnership);
- Concluding
VIVIAD Phase 2b clinical study program and in-depth analysis;
- Analyzing the
data of the VIVA-MIND Phase 2 clinical study with varoglutamstat in
the U.S. in early AD by year end 2024;
- Continuing to actively pursue
potential business development and financing opportunities.
Varoglutamstat Mechanism of
Action
- Post-translational modification
occurs both physiologically and in disease settings and it is a
crucial process to functionalize proteins. Many different
post-translational modifications are catalyzed by enzymes that have
become known drug targets, e.g. kinases, proteases, or
methylases.
- Pyroglutamate (pE) formation, a
specific post-translational modification catalyzed by the
glutaminyl cyclase enzymes QPCT and QPCTL, has emerged as a central
element in different diseases including neurodegenerative,
inflammatory and fibrotic diseases as well as cancer.
- Varoglutamstat is a highly potent
oral small molecule inhibitor of human QPCT and QPCTL, designed to
prevent inflammatory and fibrotic processes by blocking
pyroglutamate formation on key disease drivers.
- QPCTL inhibition has demonstrated
robust evidence of efficacy in animal models of inflammatory and
fibrotic disorders such as glomerulonephritis and non-alcoholic
steatohepatitis (NASH).
Varoglutamstat – VIVIAD kidney function
results (total study population)
- Varoglutamstat
600mg BID increased eGFR over the treatment period up to 96 weeks
in patients with early AD, indicating a potential benefit of
varoglutamstat on kidney function. The treatment effect in the
overall VIVIAD study population was 3.4mL/min/1.73m2/year
(p<0.001; varoglutamstat n=141 / placebo n=117).
- Further
sensitivity and subgroup analysis has shown this effect is observed
across the range of eGFR levels at baseline in the study, and when
assessed using a set of diverse and validated methods for
calculating kidney function.
- Additionally, the Company has
explored the effect of varoglutamstat on levels of pyroglu-CCL2
(pE-CCL2), a pro-inflammatory cytokine. Persistent, low grade
inflammation is considered a hallmark feature of chronic kidney
disease (CKD). Results showed a significant and dose-dependent
reduction in pE-CCL2 in the serum of VIVIAD patients following
treatment with varoglutamstat. This demonstrates the effectiveness
of varoglutamstat in inhibiting systemic intracellular QPCTL and
strongly supports an anti-inflammatory effect.
Significant effects of varoglutamstat in
diabetes subgroup2
- Analysis of eGFR in a subgroup of
patients with diabetes2 in the VIVIAD Phase 2b study
reveals a substantially higher treatment effect4 of
>8mL/min/1.73m2/year (p=0.02; varoglutamstat n=20 / placebo
n=12) compared to the overall VIVIAD study population where the
treatment effect was 3.4mL/min/1.73m2/year (p<0.001;
varoglutamstat n=141 / placebo n=117).
- Promising additional effects were
observed in the diabetes subgroup in varoglutamstat treated
patients including a reduction in liver transaminases, mild weight
loss, and a reduction in diastolic blood pressure.
- Data revealed that the positive
effect on kidney function in the diabetes subgroup appears to be
independent of any change in glycemic control (HbA1C remained
steady over the period for the varoglutamstat group).
- A reduction of the plasma
concentration of the inflammatory and fibrosis inducing pE-CCL2
(p=0.004) was observed in the varoglutamstat arm, indicating a
strong anti-inflammatory effect.
- Varoglutamstat was well-tolerated
at the dose tested (up to 600mg twice daily) and there were no
meaningful differences in adverse events observed in renal and
metabolic system organ classes versus placebo or the total
population.
Proposed Clinical Development Plan in
Diabetic Kidney Disease
(DKD)3
- Despite advances in the standard of
care for DKD, there remains a significant unmet need for new
therapies to stabilize kidney function and prevent disease
progression.
- Vivoryon plans to start a Phase 2
study in DKD that is intended to include patients with disease
stages more advanced than those observed in the VIVIAD Phase 2
study, enabling an expansion of the overall target patient
population. The Company envisages a placebo-controlled study of up
to approximately 120 subjects with stage 3b/4 DKD. These subjects
would be randomized 1:1 to varoglutamstat 600mg twice daily or
placebo, on top of standard of care medications. Key endpoints are
planned to include eGFR slope analysis, measures of albuminuria
(UA(p)CR), inflammation and fibrosis-related biomarkers, as well as
safety.
- Vivoryon is evaluating business
development and financing opportunities, to further explore the
potential of varoglutamstat and QPCT/L inhibitors in kidney disease
in both large indications, such as DKD, and in certain rare
diseases that impact kidney function, such as Fabry disease and
Alport Syndrome.
Varoglutamstat – early Alzheimer’s
disease (AD)
- Vivoryon has continued its in-depth
analysis of the VIVIAD data. Findings to date continue to confirm
there is no consistent effect of varoglutamstat up to 600mg BID on
cognition and function, including in high exposure patients.
Results from pharmacokinetic, pharmacodynamic and biomarker data,
including an assay for measuring pE-Abeta forms, suggests that
intracellular QPCT may play a greater role in driving clinical
outcomes in AD. Data from VIVA-MIND, anticipated by the end of
2024, is expected to contribute to the overall dataset informing
varoglutamstat’s development strategy in AD.
Corporate Development
Updates
- In March 2024,
Kugan Sathiyanandarajah and Professor Dr. Morten Asser Karsdal
stepped down from Vivoryon’s Board of Directors. They had been
appointed as Non-Executive Directors in June 2023.
- In March 2024,
Anne Doering, CFA, assumed the role of Chief Financial Officer
(CFO) of Vivoryon, following her previous position as Chief
Strategy & Investor Relations Officer.
- Vivoryon held its 2024 Annual
General Meeting (AGM) on Friday, June 21, 2024, at 1:00 p.m. (CEST)
in Amsterdam, the Netherlands. The shareholders approved all items
on the agenda of the meeting. The full agenda and all relevant
documents are available on the Company’s website
(https://www.vivoryon.com/2024-annual-general-meeting/). Agenda
items of particular note include the reappointment of Dr. Michael
Schaeffer, Chief Business Officer, as executive director as well as
the amendment to the Company’s articles of association with regard
to, among other changes, the decrease of the nominal value of the
shares in the capital of the Company to EUR 0.01 from EUR 1.00,
which was implemented on September 5, 2024.
Financial Results for the First Half of
2024
Revenues were zero in the six
months ended June 30, 2024, as well as in the six months ended June
30, 2023.
Research and development
expenses increased by EUR 4.0 million to EUR 10.3 million
in the six months ended June 30, 2024, compared to EUR 6.3 million
in the six months ended June 30, 2023. This increase was largely
attributable to the increase in clinical development costs from the
VIVIAD and VIVA-MIND studies as well as early investments into
kidney related research.
General and administrative
expenses were EUR 3.5 million in the six months ended
June 30, 2024, compared to EUR 4.4 million in the six months
ended June 30, 2023. The decrease of EUR 0.9 million was
largely attributable to higher non-executive board compensation in
2023.
Net loss for
the six months ended June 30, 2024, was EUR 13.6 million,
compared to EUR 10.7 million for the six months ended June 30,
2023.
The Company held EUR 15.3 million in
cash and cash equivalents as of June 30, 2024,
compared to EUR 28.6 million, which includes cash and cash
equivalents and term deposits within financial assets, as of
December 31, 2023. Cash utilization for the first six months of
2024 reflects the intensive investment period in VIVIAD and
VIVA-MIND, both of which are expected to meaningfully ramp down in
the second half 2024 as both studies approach their conclusion.
Outlook & Financial
Guidance
As published on April 24, 2024, the Company
expects, on the basis of its most recent financial and business
plan, that its existing cash and cash equivalents will be
sufficient to fund its operating plans, excluding any additional
financings, into the second quarter of 2025.
This cash runway guidance reflects the shift in
focus of research and development resources towards inflammatory
and fibrotic disorders, such as of the kidney, and an overall
reduction in cash utilization including the ramp down of spending
on VIVIAD as it approaches its conclusion, the discontinuation of
VIVA-MIND, the discontinuation of VIVALONG preparation activities
given the developments of VIVIAD and VIVA-MIND, as well as the
streamlining of manufacturing costs and programs for API
development.
The viability of the Company beyond the second
quarter of 2025 is dependent on its ability to raise additional
funds to finance its operations which also depends on the success
of its research and development activities such as those focusing
on exploring opportunities in kidney disease.
Conference Call and Webcast
Vivoryon will host a conference call and webcast today, September
12, 2024, at 3:00 pm CEST (9:00 am EDT). A Q&A session will
follow the presentation of the first half 2024 results.
A live webcast and slides will be made available at:
https://www.vivoryon.com/news-and-events/presentations-webcasts/
To join the conference call via phone, participants may
pre-register and will receive dedicated dial-in details to easily
and quickly access the call via the following website:
https://register.vevent.com/register/BIb82f5f65fffe4d5faaade135258da32a
It is suggested participants dial into the conference call 15
minutes prior to the scheduled start time to avoid any delays in
attendance.
Approximately one day after the call, a slide-synchronized audio
replay of the conference will be available on:
https://www.vivoryon.com/news-and-events/presentations-webcasts/
Virtual Kidney Disease Key Opinion Leaders Event on
September 30, 2024
Vivoryon will host a virtual Kidney Disease KOL
(Key Opinion Leaders) conference call and webcast on Monday,
September 30, 2024, featuring expert presentations by seasoned KOLs
followed by a Q&A session on the standard of care and existing
medical need, market development and commercial potential in kidney
disorders, as well as evidence generation and statistical
principles in kidney disease drug development, with special
emphasis on diabetic kidney disease.
Featured speakers:
- Tobias B. Huber,
MD - Chair of the Center of Internal Medicine and Director
of the III. Department of Medicine - University Medical Center
Hamburg-Eppendorf (UKE), Germany. Acting as Medical Advisor for
clinical study design. Research collaboration with Vivoryon
focusing on pre-clinical and mechanistic activities relating to
varoglutamstat and the role of QPCT/L on kidney function.
- Florian Jehle -
CEO of Vifor-FMC Renal Pharma. Acting as Industry Expert Advisor to
Vivoryon in the kidney field including strategic business and
commercial advice.
- Kevin Carroll, PhD
- CEO, KJC Statistics. Acting as statistical analysis expert,
providing and calculating statistical read-outs and advising on
clinical study statistical aspects.
Conference call details
Date: September 30, 2024
Time: 3:00 pm CEST / 9:00 am EDT
A live webcast and slides will be made available at:
https://www.vivoryon.com/news-and-events/presentations-webcasts/
Please register to join the conference call via the following
website:
https://edge.media-server.com/mmc/p/b8g57xvh/
###
Vivoryon Therapeutics N.V. Financial
Statements
Unaudited Statement of Operations and Comprehensive Loss
for the Six Months Ended June 30, 2024 and 2023
|
|
For the six months
ended June 30, |
|
in kEUR, except for share data |
2024
(unaudited) |
2023
(unaudited) |
|
|
|
|
|
Research and development expenses |
(10,308) |
(6,259) |
|
General and administrative expenses |
(3,501) |
(4,433) |
|
Operating loss |
(13,809) |
(10,692) |
|
Finance income |
303 |
258 |
|
Finance expenses |
(53) |
(327) |
|
Finance result |
250 |
(69) |
|
Result before income taxes |
(13,559) |
(10,761) |
|
Income taxes |
— |
45 |
|
Net loss for the period |
(13,559) |
(10,716) |
|
Items not to be reclassified subsequently to profit or
loss |
|
|
|
Remeasurement of the net defined benefit pension liability |
39 |
(9) |
|
Total other comprehensive profit / (loss) |
39 |
(9) |
|
Comprehensive loss |
(13,520) |
(10,725) |
|
Loss per share in EUR (basic and diluted) |
(0.52) |
(0.44) |
|
|
|
|
The accompanying notes are an integral part of
these condensed interim financial statements.
Vivoryon Therapeutics N.V.
Unaudited Condensed Statements of Financial Position as of
June 30, 2024 and December 31, 2023 (audited)
|
in kEUR |
June 30,
2024
(unaudited) |
December 31,
2023
(audited) |
|
ASSETS |
|
|
|
Non-current assets |
|
|
|
Property, plant and equipment |
31 |
40 |
|
Intangible assets |
904 |
941 |
|
Right-of-use assets |
9 |
36 |
|
Total non-current assets |
944 |
1,017 |
|
Current assets |
|
|
|
Financial assets |
74 |
10,165 |
|
Other current assets and prepayments |
701 |
1,085 |
|
Cash and cash equivalents |
15,272 |
18,562 |
|
Total current assets |
16,047 |
29,812 |
|
TOTAL ASSETS |
16,991 |
30,829 |
|
|
|
|
|
Equity |
|
|
|
Share capital |
26,067 |
26,067 |
|
Share premium |
135,671 |
135,671 |
|
Other capital reserves |
14,817 |
13,599 |
|
Accumulated other comprehensive loss |
(217) |
(256) |
|
Accumulated deficit |
(162,358) |
(148,799) |
|
Total equity |
13,980 |
26,282 |
|
Non-current liabilities |
|
|
|
Pension liability |
1,287 |
1,353 |
|
Provisions long-term |
12 |
12 |
|
Total non-current liabilities |
1,299 |
1,365 |
|
Current liabilities |
|
|
|
Trade payables |
1,465 |
2,894 |
|
Lease liabilities |
10 |
38 |
|
Other liabilities |
237 |
250 |
|
Total current liabilities |
1,712 |
3,182 |
|
Total Liabilities |
3,011 |
4,547 |
|
TOTAL EQUITY AND LIABILITIES |
16,991 |
30,829 |
|
|
|
|
The accompanying notes are an integral part of
these condensed interim financial statements.
Vivoryon Therapeutics N.V.
Unaudited Condensed Statements of Changes in Shareholders’
Equity for the six months ended June 30, 2024 and 2023
| in
kEUR |
Share
capital |
Share
premium |
Other
capital reserves |
Accumulated
other
comprehensive
loss |
Accumulated
deficit |
Total
equity |
|
|
|
|
|
|
|
|
| January 1,
2024 |
26,067 |
135,671 |
13,599 |
(256) |
(148,799) |
26,282 |
| Net loss for the
period |
— |
— |
— |
— |
(13,559) |
(13,559) |
| Remeasurement of
the net defined benefit pension liability |
— |
— |
— |
39 |
— |
39 |
|
Comprehensive loss |
— |
— |
— |
39 |
(13,559) |
(13,520) |
| Proceeds from the
issuance of common shares |
— |
— |
— |
— |
— |
— |
| Transaction costs
of equity transactions |
— |
— |
— |
— |
— |
— |
| Share-based
payments |
— |
— |
1,218 |
— |
— |
1,218 |
| Exercise of share
options |
— |
— |
— |
— |
— |
— |
| June 30,
2024 |
26,067 |
135,671 |
14,817 |
(217) |
(162,358) |
13,980 |
| |
|
|
|
|
|
|
| January 1,
2023 |
24,105 |
113,382 |
9,656 |
(180) |
(120,457) |
26,506 |
| Net loss for the
period |
— |
— |
— |
— |
(10,716) |
(10,716) |
| Remeasurement of
the net defined benefit pension liability |
— |
— |
— |
(9) |
— |
(9) |
|
Comprehensive loss |
— |
— |
— |
(9) |
(10,716) |
(10,725) |
| Proceeds from the
issuance of common shares |
1,786 |
23,214 |
— |
— |
— |
25,000 |
| Transactions costs
of equity transactions |
— |
(2,095) |
— |
— |
— |
(2,095) |
| Exercise of share
options |
— |
— |
2,305 |
— |
— |
2,305 |
| Share-based
payments |
71 |
472 |
— |
— |
— |
542 |
| June 30,
2023 |
25,962 |
134,973 |
11,961 |
(189) |
(131,173) |
41,534 |
| |
|
|
|
|
|
|
The accompanying notes are an integral part of
these condensed interim financial statements.
Vivoryon Therapeutics N.V.
Unaudited Condensed Statements of Cash Flows for the six
months ended June 30, 2024 and 2023
|
|
For the six months ended
June 30, |
|
in kEUR |
2024
(unaudited) |
2023
(unaudited) |
|
|
|
|
|
Operating activities |
|
|
|
Net loss for the period |
(13,559) |
(10,716) |
|
Adjustments for: |
|
|
|
Finance result |
(250) |
69 |
|
Depreciation and amortization |
73 |
79 |
|
Share based payments |
1,218 |
2,305 |
|
Foreign currency gain (loss) from other items than cash |
(25) |
(59) |
|
Deferred income tax |
— |
(45) |
|
Other non-cash adjustments |
19 |
(33) |
|
Changing in: |
|
|
|
Financial assets |
(4) |
(8,938) |
|
Other current assets and prepayments |
383 |
(2,036) |
|
Pension liabilities |
(66) |
(13) |
|
Trade payables |
(1,429) |
(1,252) |
|
Other liabilities |
(13) |
306 |
|
Interest received |
353 |
51 |
|
Interest paid |
— |
(1) |
|
Cash flows used in operating activities |
(13,300) |
(20,283) |
|
Investing activities |
|
|
|
Purchase of plant and equipment |
— |
(9) |
|
Proceeds from sale of financial assets |
10,000 |
— |
|
Cash flows used in investing activities |
10,000 |
(9) |
|
Financing activities |
|
|
|
Proceeds from the issuance of common shares |
— |
25,000 |
|
Capital raising costs |
— |
(2,095) |
|
Proceeds from exercise of share options |
— |
542 |
|
Payment of lease liabilities |
(28) |
(47) |
|
Cash flows provided by financing activities |
(28) |
23,400 |
|
Net increase in cash and cash equivalents |
(3,328) |
3,109 |
|
Cash and cash equivalents at the beginning of period |
18,562 |
26,555 |
|
Effect of exchange rate fluctuation on cash held |
38 |
(82) |
|
Cash and cash equivalents at end of period |
15,272 |
29,582 |
|
|
|
|
The accompanying notes are an integral part of these condensed
interim financial statements.
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
Statements
This press release includes forward-looking statements,
including, without limitation, those regarding the business
strategy, management plans and objectives for future operations of
Vivoryon Therapeutics N.V. (the “Company”), estimates and
projections with respect to the market for the Company’s products
and forecasts and statements as to when the Company’s products may
be available. Words such as “anticipate,” “believe,” “estimate,”
“expect,” “forecast,” “intend,” “may,” “plan,” “project,”
“predict,” “should” and “will” and similar expressions as they
relate to the Company are intended to identify such forward-looking
statements. These forward-looking statements are not guarantees of
future performance; rather they are based on the Management’s
current expectations and assumptions about future events and
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
factors could materially adversely affect the outcome and financial
effects of the plans and events described herein. The Company’s
results of operations, cash needs, financial condition, liquidity,
prospects, future transactions, strategies or events may differ
materially from those expressed or implied in such forward-looking
statements and from expectations. As a result, no undue reliance
should be placed on such forward-looking statements. This press
release does not contain risk factors. Certain risk factors that
may affect the Company’s future financial results are discussed in
the published annual financial statements of the Company. This
press release, including any forward-looking statements, speaks
only as of the date of this press release. The Company does not
assume any obligation to update any information or forward-looking
statements contained herein, save for any information required to
be disclosed by law.
For more information, please contact:
Investor Contact
Vivoryon Therapeutics N.V.
Dr. Manuela Bader, Director IR & Communication
Tel: +49 (0)345 555 99 30
Email: IR@vivoryon.com
Media Contact
Trophic Communications
Valeria Fisher
Tel: +49 175 8041816
Email: vivoryon@trophic.eu
1Estimated 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.
2Diabetes 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%.
3The timing and execution of the planned Phase 2 study
is subject to additional funding / partnership.
4Treatment effect – the between-group difference in eGFR
slope between varoglutamstat and placebo.
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