A Phase 1, Randomized, Double-Blinded, Placebo-Controlled, Single- and Multiple- Dose Escalation Study to Evaluate the Safety, Tolerability, and Pharmacokinetics of Oral VVZ-2471 in Healthy Male Volunteers

Start Date01 Nov 2022

Sponsor / Collaborator

Vivozon, Inc.

NCT04430088

/ Unknown statusPhase 3

A Phase 3, Multicenter, Randomized, Double-Blind, Parallel Group, Placebo-Controlled Study to Evaluate the Efficacy and Safety of VVZ-149 Injections for the Treatment of Postoperative Pain Following Bunionectomy

The purpose of this phase 3 study is to evaluate the efficacy and safety of an analgesic drug candidate, VVZ-149 Injections for treating post-operative pain following bunionectomy.

Start Date26 Jun 2020

Sponsor / Collaborator

Vivozon, Inc.

100 Clinical Results associated with Vivozon, Inc.

0 Patents (Medical) associated with Vivozon, Inc.

Literatures (Medical) associated with Vivozon, Inc.

01 Jun 2025·CNS DRUGS

Evaluation of Safety, Pharmacokinetic, and Pharmacodynamic Characteristics of a Novel Dual mGluR5/5-HT2AR Antagonist (VVZ-2471) in a Randomized, Double-Blind, First-in-Human Study

Article

Author: Lee, Sang Rim ; Cho, Sunyoung ; Kim, Jina ; Chung, Jae-Yong ; Song, Inkyung ; Yu, Kyung-Sang ; Lee, HyunJoon ; Bae, Sungyeun

BACKGROUND:

VVZ-2471 is a dual-target compound that simultaneously inhibits both metabotropic glutamate receptor subtype 5 and serotonin receptor subtype 2A. Preclinical studies have supported VVZ-2471 as a promising candidate for opioid use disorder. This study aimed to evaluate the safety and pharmacokinetic (PK)-pharmacodynamic (PD) characteristics of VVZ-2471 capsules in healthy Korean adults.

METHODS:

A phase I, double blind, placebo controlled, single ascending dose (SAD) and multiple ascending dose (MAD) study was conducted in healthy adult males. In the SAD study, participants received a single oral dose of VVZ-2471 ranging from 25 to 600 mg, including a satellite food-effect group receiving 200 mg. In the MAD study, participants received 200 mg once daily (QD), 200 mg twice daily, and 400 mg QD for 7 days. Plasma and urine samples were collected for the PK analyses. Safety analysis was based on adverse events, clinical laboratory tests, vital signs, physical examinations, 12-lead electrograms, oxygen saturation monitoring, and the Beck Depression Inventory-II test. The potential of VVZ-2471 for treating addiction was explored using a well-established questionnaire on smoking urges (QSU-Brief) consisting of ten items.

RESULTS:

A total of 49 and 24 healthy Korean adult males completed the SAD and MAD study, respectively. The overall demographic characteristics of participants who received VVZ-2471 or placebo in the SAD and MAD studies were generally comparable. Following a single oral dose of VVZ-2471 up to 600 mg, the area under the concentration-time curve (AUC) increased proportionally with the dose. After repeated administration, the accumulation ratio of VVZ-2471 ranged from 1.4 to 2.0. In the fed state, the maximum plasma concentration and AUC of VVZ-2471 decreased to 0.78-fold and 0.61-fold, respectively, compared with the fasting state. Urinary excretion was marginal. The most common adverse events were nausea and dizziness. Among 29 smokers, participants given VVZ-2471 at 200 mg or higher had reduced smoking urges compared with the placebo.

CONCLUSIONS:

VVZ-2471 was well tolerated up to a single oral dose of 600 mg and a daily oral dose of 400 mg for 7 days. While preliminary, a trend of reducing smoking urges was observed in the VVZ-2471 group.

REGISTRATION:

Clinical Research Information Service (CRiS), Republic of Korea (a primary registry in the World Health Organization (WHO) Registry Network) identifier no. KCT000889.

01 Feb 2025·JOURNAL OF CLINICAL ANESTHESIA

Reduction of postoperative pain and opioid consumption by VVZ-149, first-in-class analgesic molecule: A confirmatory phase 3 trial of laparoscopic colectomy

Article

Author: Cho, Sunyoung ; Bahk, Jae-Hyon ; Park, Mi-Hye ; Lee, Ho-Jin ; Kim, Jina ; Oh, Ah-Young ; Sim, Ji-Yeon ; Kim, Duk Kyung ; Park, Insun ; Moon, Young-Jin ; Nedeljkovic, Srdjan S ; Song, Inkyung ; Lee, Sang Rim ; Yoon, Seung Zhoo

STUDY OBJECTIVE:

VVZ-149 is a small molecule that inhibits the glycine transporter type 2 and the serotonin receptor 5-hydroxytryptamine 2 A. In this Phase 3 study, we investigated the efficacy and safety of VVZ-149 as a single-use injectable analgesic for treating moderate to severe postoperative pain after laparoscopic colectomy.

DESIGN:

Randomized, parallel group, double-blind, Phase 3 clinical trial (Trial no. NCT05764525).

SETTING:

5 tertiary referral centers in South Korea.

PATIENTS:

284 patients undergoing laparoscopic colectomy.

INTERVENTIONS:

A continuous 10-h intravenous infusion of VVZ-149 (n = 141) or placebo (n = 143) administered after emergence from anesthesia.

MEASUREMENTS:

Pain intensity was assessed using a numeric rating scale (NRS) from the start of infusion for 48 h. The primary efficacy measure was the Sum of Pain Intensity Difference (SPID) for the first 12 h after the start of drug infusion. Other efficacy measures included SPID at other time points, opioid consumption via on-demand patient-controlled analgesia (PCA) and rescue medication, and proportion of patients who did not require rescue opioids for 48 h post-dose.

MAIN RESULTS:

Pain relief as measured by SPID was significantly improved by 35 % in the VVZ-149 group compared to the placebo group at 6 h (p = 0.0193) and 12 h (p = 0.0047) after the start of infusion. Significantly lower pain intensity scores were observed between 4-10 h in the VVZ-149 group compared to the placebo group (p = 0.0007), reaching mild pain (mean NRS <4) at 8 h. VVZ-149 alleviated pain during the first 12 h post-dose with 30.8 % less opioid consumption and 60.2 % fewer PCA requests when compared with placebo. A higher proportion of patients receiving VVZ-149 were rescue opioid-free during 2-6 h (p = 0.0026) and 6-12 h (p = 0.0024) compared with the placebo group. VVZ-149 administration in post-colectomy patients was generally safe and well tolerated.

CONCLUSIONS:

When compared to placebo, VVZ-149 infusion demonstrated a significant reduction of pain within the first 12 h after surgery with a substantial decrease in opioid use. VVZ-149 rapidly lowers the pain intensity starting at as early as 4 h post-dose, allowing subjects to experience mild pain levels from 8 h through 48 h. Therefore, the analgesic effect of VVZ-149 was shown to effectively relieve pain and reduce opioid use for treating moderate to severe pain in the early postoperative care setting.

REGISTRATION NUMBER:

Trial Number NCT05764525.

08 Sep 2021·Pain medicine (Malden, Mass.)Q3 · MEDICINE

Role of VVZ-149, a Novel Analgesic Molecule, in the Affective Component of Pain: Results from an Exploratory Proof-of-Concept Study of Postoperative Pain following Laparoscopic and Robotic-Laparoscopic Gastrectomy

Q3 · MEDICINE

Article

Author: Kim, Jina ; Cho, Sunyoung ; Bai, Sun Joon ; Song, Inkyung ; Nedeljkovic, Srdjan S ; Lee, Sang Rim ; Lee, Chaewon

Abstract:

Objective:

VVZ-149 is a small molecule that both inhibits the glycine transporter type 2 and the serotonin receptor 5 hydroxytryptamine 2 A. In a randomized, parallel-group, and double-blind trial (NCT02844725), we investigated the analgesic efficacy and safety of VVZ-149 Injections, which is under clinical development as a single-use injectable product for treating moderate to severe postoperative pain.

Methods:

Sixty patients undergoing laparoscopic and robotic-laparoscopic gastrectomy were randomly assigned to receive a 10-hour intravenous infusion of VVZ-149 Injections or placebo, initiated approximately 1 hour before completion of surgical suturing. Major outcomes included pain intensity and opioid consumption via patient-controlled analgesia and rescue analgesia provided “as needed.” The treatment efficacy of VVZ-149 was further examined in a subpopulation requiring early rescue medication, previously associated with the presence of high levels of preoperative negative affect in a prior Phase 2 study (NCT02489526).

Results:

Pain intensity was lower in the VVZ-149 (n = 30) than the placebo group (n = 29), reaching statistical significance at 4 hours post-emergence (P < .05), with a 29.5% reduction in opioid consumption for 24 hours and fewer demands for patient-controlled analgesia. In the rescued subgroup, VVZ-149 further reduced pain intensity (P < .05) with 32.6% less opioid consumption for 24 hours compared to placebo patients.

Conclusions:

VVZ-149 demonstrated effective analgesia with reduced postoperative pain and opioid requirements. Consistent with the results from the previous Phase 2 study, patients with early rescue requirement had greater benefit from VVZ-149, supporting the hypothesis that VVZ-149 may alleviate the affective component of pain and mitigate excessive use of opioids postoperatively.

News (Medical) associated with Vivozon, Inc.

08 Nov 2021

·endpts.com

Korean regulators shut down Samsung Pharma manufacturing after finding additives, false records

South Korea’s health regulator has suspended Samsung Pharmaceutical’s manufacturing operations until mid-February after the agency learned that a production manager was tasked with responsibilities of two different plants. The revelation violated a law requiring each plant to be managed by one person. Monday’s halt comes just months after an inspection revealed a number of violations at one Samsung Pharma plant, including the use of additives without permission and false manufacturing records, the Korea Biomedical Review reported . Six drugs, including five of Samsung Pharma’s, have been suspended from being manufactured. Geramin, Moarex, Combicin, and an Aprogen Pharmaceutical drug Healthnamine have all been halted. The company is in no way affiliated with the South Korean electronics giant Samsung, or its subsidiary Samsung Biologics, a representative for the company said. In a statement on its website, Samsung Pharma attributed the error to negligence, and carelessness in checking in on the manager’s work, and insisted that it was not a problem with the quality of products shipped. “Nevertheless, (we are) deeply reflecting on the inconvenience caused by not thoroughly complying with the standards that we, as pharmaceutical manufacturers, should abide by,” the statement said. The three-month suspension is the first step in a series of potential punishments for companies who violate the law that prevents the double-dipping of employees. The next is a six-month manufacturing suspension, and the third strike will see the agency revoke a businesses license, Korea Biomedical Review reported. The suspension will start today and end on Feb. 14. Additional sanctions include the halt of manufacturing injections for five weeks and a four-month suspension of the five drugs under scrutiny. In a public statement, the company announced that the suspension would cost the company 5.7 billion won, or roughly $4.8 million. In June , a temporary suspension was ordered after violations surfaced, and the six drugs were forced to be recalled. Samsung Pharma illegally used additives arbitrarily and created false documents to cover up the violations. Regulators have also punished companies such as Vivozon and Binex for similar violations. The news brought down the company’s stock in the South Korean market when it first broke in June. But shares faltered very little after Monday’s news broke, still closing higher than the previous day. In the statement, Samsung Pharma said that it would revisit its founding philosophy and focus on its original duties as a pharmaceutical company. “We will do our best to become a Samsung Pharma that can be trusted by shareholders, customers, medical staff and patients again by removing the complacency of the past,” it said.

100 Deals associated with Vivozon, Inc.

100 Translational Medicine associated with Vivozon, Inc.

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Drug(Targets)	Indications	Global Highest Phase

VVZ-2471	Chronic Pain More	Phase 1
VVZ-N2	Chronic Pain More	Preclinical
VVZ-3416	Parkinson Disease More	Preclinical
VVZ-N5	Thrombosis More	Discovery
VVZ-N3	psychological symptoms behavior compulsive behavior addiction More	Discontinued

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