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RECCE 327 Treatment

RECCE® 327 Treatment

Recce Pharmaceuticals Ltd.'s anti-infective pipeline includes patented, broad-spectrum, synthetic polymer RECCE® 327 (R327), an intravenous and topical therapy being developed for the treatment of severe and potentially life-threatening infections caused by both Gram-positive and Gram-negative bacteria, including their superbug forms, such as Urinary Tract Infections (UTIs), which are common infectious diseases caused by pathogens, such as Escherichia coli (E. coli) (62%). Recce's anti-infectives are wholly synthetic, based on a patented polymeric structure, and designed to overcome resistance. Recce's anti-infectives can potentially overcome the hypercellular mutation of bacteria and viruses, which is the challenge of all existing antibiotics. R327 affects the assembly of bacterial cell division complex components that require cellular energy to remain assembled, confirming its ability to disrupt cellular bioenergetics. This decreases the formation of the bacterial cell division complex into ring-like structures (Z-rings) in a concentration-dependent manner. RECCE® 327 is not a UTI preventive vaccine.

The U.S. Food and Drug Administration (FDA) has awarded RECCE® 327 Qualified Infectious Disease Product designation under the Generating Antibiotic Initiatives Now (GAIN) Act, labeling it for Fast Track Designation, plus ten years of market exclusivity post approval. On May 7, 2024, Recce announced that the China National Intellectual Property Administration Granted a new Patent Family 2 for Recce's anti-infectives, "Copolymer and Method for Treatment of Bacterial Infections" in China, expiry 2035.

According to the World Health Organization (WHO), RECCE® 327 was added to the WHO List of Antibacterial Products in Clinical Development on June 18, 2024. R327 is the only compound classified as an adenosine triphosphate (ATP) production disruptor. Disruption of ATP production in bacterial cells, when targeted as the primary mechanism of action, not secondary to other cell perturbation mechanisms, can confer activity against Gram-positive and Gram-negative pathogens.

On May 15, 2024, Recce reported that it had successfully dosed the first male and female participants in the nexCohortrt with RECCE® 327, 4,000mg intravenously, at a fast infusion rate of 20 minutes in its Phase I/II UTI/Urosepsis clinical trial. On June 28, 2024, Recce announced that the Phase I/II rapid infusion clinical trial demonstrated efficacy in bacterial growth in dosed participants injected with RECCE® 327 at the highest tested dose of 4,000mg. These results indicate that RECCE® 327 administered intravenously is safe and efficacious against E. coli.

On October 8, 2024, the company announced that RECCE® 327 topical gel (R327G) was safe and well tolerated in human subjects, with promising antibacterial responses observed in patients.

Recce Pharmaceuticals Ltd (ASX: RCE, FSE: R9Q) is developing a New Class of Synthetic Anti-Infectives designed to address the urgent global health problems of antibiotic-resistant superbugs and emerging viral pathogens. On June 18, 2024, the Company confirmed a further cash refund of AUD $2,624,860.47 for the Research and Development Tax Incentive rebate from the Australian Tax Office for the financial year ending 30 June 2023. On August 5, 2024, the Company's pro forma cash position was A$19.8 million.

RECCE® 327 Urinary Tract Infection (UTI) Treatment Dosage

RECCE® 327 may be administered for intravenous, topical, nasal, oral, and inhaled use. RECCE® 327's universal mechanism of action has a patented ability to continuously kill bacteria without a tendency for the emergence of resistance, even with repeated use, indicating a unique ability to combat antibiotic-resistant superbugs. The Company has explored multiple infusion times of R327: 15 minutes, 20 minutes, 30 minutes, and 45 minutes. The highest dose tested in the phase 1 study is 4,000mg. Administering antibiotics through rapid intravenous infusions has proven to be a safe and effective method that significantly impacts patient treatment, reduces wait times, and alleviates nursing workloads worldwide.

RECCE® 327 Urinary Tract Infection (UTI) Indication

Data in 2024 is expected to pave the way for a Phase II UTI/Urosepsis efficacy trial, potentially establishing R327 as a frontline treatment. UTI is one of the most common infectious diseases in the pediatric population. In high-income countries, UTIs affect up to 2.8% of children annually, with recurrence rates ranging from 8% to 30% [2,3]. It is estimated that 11.3% of females and 3.6% of males develop at least one episode of UTI within the first 16 years of life.

RECCE® 327 Acinetobacter Baumannii Indication

On July 8, 2024, results from a study on the efficacy of RECCE® 327 (R327) against the multidrug-resistant World Health Organization (WHO) priority pathogen Acinetobacter baumannii (A. baumannii) demonstrated R327’s bactericidal activity compared to placebo and ciprofloxacin in just one-hour post-treatment and at 24 hours post-treatment in primary human epidermal keratinocytes (skin cells) infected with A. baumannii.

RECCE® 327 Mechanism of Action

Most antibiotics inhibit a single target, such as bacterial gyrase enzymes, cell wall biosynthetic enzymes, or enzymes required for DNA replication during bacterial cell division. They operate on a ‘lock and key’ mechanism and only bind to a few active sites on the bacterial target. However, if a mutation is introduced into the target site, the antibiotic will cease to be effective. Recce’s anti-infectives are wholly synthetic, based on a patented polymeric structure, and have been designed to overcome resistance.

RECCE 327 UTI Treatment Side Effects

No significant side effects have been reported. In April 2024, Recce Pharmaceuticals reported that an Independent Safety Committee had approved an increase of R327 to 4,000mg (I.V.) over a fast infusion of 30 minutes. In June 2024, the Company reported no serious side effects in a Phase 1/2 study.

RECCE 327 UTI Treatment Availability

RECCE® 327 is not market-approved for human use. As of April 2024, the Company was producing 5,000 GMP doses of R327 per week.

RECCE 327 UTI Treatment News

August 5, 2024—Recce Pharmaceuticals Limited announces the successful close of its Share Purchase Plan, which was announced on July 2, 2024.

June 28, 2024 - Dr. Marc Sharp, Chief Scientific Officer at Linnaeus Bioscience, leading independent experts in bacterial Mechanism of Action analysis, added: "The ability of R327 to achieve biologically relevant concentrations and exhibit antibacterial activity in urine samples is highly encouraging."

June 18, 2024 - Recce Pharmaceuticals CEO James Graham said, "We are pleased that R327 has been included in the list of antibacterial products to tackle the urgent global health threat posed by antibiotic resistance. There is a demand for new antibiotic therapies, and this report further showcases R327's potential as a novel treatment for a broad range of life-threatening and resistant bacteria."

May 15, 2024 - The first participants were successfully dosed at 4,000mg IV over 20 minutes, at 4,000mg in a phase 1/2 study.

April 17, 2024 - Recce Pharmaceuticals Ltd. announced the successful batch completion under Good Manufacturing Practices for RECCE® 327 (R327), with the patented manufacturing process now producing 5,000 GMP doses of R327 per week.

September 26, 2023 - Recce Pharmaceuticals Ltd. announced it completed the cohort dosing of healthy male and female subjects in its Phase I/II clinical trial, evaluating its lead anti-infective candidate, RECCE® 327, at faster infusion rates.

RECCE® 327 UTI Treatment Clinical Trials

UTI clinical trials are active as of May 2024. A phase 1 clinical trial (ACTRN12623000448640) consists of up to 4 cohorts with 4 participants at each dose level. Each participant will begin with a single dose of RECCE®327 intravenously over Period A (longer infusion duration), followed by 48 hours of safety surveillance and PK data collection. The second dose of RECCE®327 infusion over Period B (shorter infusion duration) had the same dose level and concentration and a minimum time elapsed of 48 hours from the start of the first to the second dose. For the subsequent, a non-Data Safety Monitoring Board committee will review the safety and PK data (the latter, if available). It may suggest adjusting the dose level, infusion rate, and/ or concentration of the RECCE®327 before proceeding to the nexCohortrt. The non-DSMB committee may determine not to proceed with additional cohorts as well. Four non-DSMB committee meetings will be planned one week after Period B for the last participant in eacCohortrt.

Announced on June 28, 2024, the Phase 1/2 trial met all primary endpoints, demonstrating the compound's tolerability and strong antibacterial efficacy. The study successfully concludes having determined an optimal dosing regimen for R327 (20-minute infusion optimal) intravenously, showing rapid onset and sustained impact on Escherichia coli via an ATP mechanism in the urine of dosed participants with the safety of participants maintained. Building on these promising results, Recce Pharmaceuticals plans to commence a Phase 2 trial in the second half of 2024, involving 30 patients, to validate these findings further and explore additional therapeutic indications for  327. The Company is also investigating the potential of R327 in treating a broader range of bacterial infections beyond UTIs and urosepsis, such as acute bacterial skin and skin structure infections.

0 min read
Manufacturer: 
Recce Pharmaceuticals Ltd.
Reviewer: 
Robert Carlson, MD
Vaccine: 
RECCE 327 Treatment
Availability: 
N/A
Generic: 
R327
Drug Class: 
Synthetic Anti-Infectives
Clinical Trial Phase I: 
ACTRN12623000448640
Condition: 
Urinary Tract Infection
Last Reviewed: 
Wednesday, October 9, 2024 - 04:10
Brand: 
RECCE® 327
Status: 
Candidate
Manufacturer Country ID: 
AU
FDA First In Class: 
Yes
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An innovative, second-generation vaccine for dengue prevention recently received prequalification from the World Health Organization (WHO).

Developed by Takeda GmbH, QDENGA® (TAK-003) (Dengue Tetravalent Vaccine [Live, Attenuated]) is an approved two-dose vaccine containing weakened versions of the four dengue serotypes that cause disease in people.

As of May 2024, QDENGA was launched in 21 countries and is available in 17 European countries but not the United States.

“The prequalification of TAK-003 is an important step in the expansion of global access to dengue vaccines, as it is now eligible for procurement by UN agencies, including UNICEF and PAHO,” said Dr. Rogerio Gaspar, WHO Director for Regulation and Prequalification, in a press release on May 15, 2024.

The WHO prequalification list also includes the Dengvaxia (CYD-TDV) vaccine developed by Sanofi Pasteur. 

According to the WHO, the most significant number of dengue outbreaks reported was in 2023 with the WHO Region of the Americas reporting about 4.5 million cases and 2,300 deaths. 

Vaccine Treats: 
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Image Caption: 
WHO 2024
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Location Tags: 
Geneva
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A vaccine candidate for control of the cytomegalovirus (“CMV”) in patients undergoing liver transplantation dosed its initial patient in a multi-center, placebo-controlled, randomized Phase 2 clinical study.

Initially developed by the City of Hope, Triplex was exclusively licensed to Helocyte.

Triplex is a universal (non-HLA-restricted) recombinant Modified Vaccinia Ankara viral vector vaccine engineered to induce a robust and durable virus-specific T cell response to three immuno-dominant proteins [UL83 (pp65), UL123 (IE1), UL122 (IE2)] linked to CMV complications in the post-transplant setting.

The trial is funded by a grant from the U.S.S NIH’s National Institute of Allergy and Infectious Diseases to the University of Washington Seattle. This grant has provided $9 million to date, with an estimated additional $12 million over the next four years in support of the Phase 2 clinical trial.

Ajit Limaye, M.D., Professor of Medicine and Director of the Solid Organ Transplant Infectious Disease Program at the University of Washington and Principal Investigator of the “CMV vaccine in Orthotopic Liver Transplant” trial, said in a press release on May 14, 2024, “There remains a significant unmet medical need to develop new therapies that can reduce the frequency and severity of CMV events in the organ transplant setting, where CMV continues to present life-threatening complications that directly impact patient outcomes and survival.”

According to the U.S. CDC, CMV is a common virus for people of all ages.

In the U.S., nearly one in three children is already infected with CMV by age five. About 1 out of 200 babies are born with congenital CMV.

And over half of adults have been infected with CMV by age 40.

Once CMV is in a person’s body, it stays there for life and can reactivate. According to the CDC, most people with CMV infection have no symptoms and aren’t aware that they have been infected.

Helocyte is a clinical-stage company developing novel immunotherapies to prevent and treat cancer and infectious diseases, including CMV and HIV.

Vaccine Treats: 
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Image Caption: 
by Sasin Tipchai
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Although several countries have adopted a single-dose human papillomavirus (HPV) vaccination strategy, many other countries, such as the United States, continue to include multiple doses in their vaccination programs.

As of May 2024, six vaccines are authorized globally to protect males and females against cancers caused by HPV.

According to an article published by the Lancet Infectious Diseases on May 8, 2024, there are ethical reasons to transition to a single-dose strategy.

These scientists discuss how a single-dose HPV vaccination strategy advances equity in three dimensions: vaccine equity, health equity, and gender equity.

Adopting a single-dose strategy eases pressure on vaccine supply, lowers program costs, and is easier to distribute.

This change facilitates vaccine procurement and implementation programs (contributing to vaccine equity) and reaching hard-to-reach people or populations (contributing to health equity).

A lower number of cases of HPV-related diseases that stem from greater vaccine distribution reduces the burden on women, who are at a higher risk of HPV-related disease or who act as caregivers, which prevents them from accessing opportunities that contribute to their empowerment (contributing to gender equity).

Thus, these scientists wrote that pursuing the single-dose HPV vaccination program strategy is ethically desirable.

In April 2022, WHO's Strategic Advisory Group of Experts on Immunization concluded that a single-dose HPV vaccine delivers virus protection comparable to 2-dose schedules.

In the U.S., the Centers for Disease Control and Prevention (CDC) HPV vaccination has been recommended for women since 2006 and for men since 2011. Current CDC HPV vaccination schedules were updated in 2023.

Vaccine Treats: 
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Image Caption: 
by Pete Linforth
Live Blog Update Author: 
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Location Tags: 
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Vaccine: 
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The world's first and only licensed chikungunya vaccine today presented further positive pivotal Phase 3 data in adolescents.

On May 13, 2024, Valneva SE announced following the initial analysis up to Day 29 post-vaccination, the most recent analysis of study VLA1553-321 evaluated the safety and immunogenicity six months after vaccination with a single dose of the chikungunya virus (CHIKV) vaccine IXCHIQ®.

The Day 180 results confirm the initial positive immunogenicity and safety data Valneva reported previously and are intended to support filing for potential label extension for use in adolescents aged 12 to 17 years.

The data are also expected to support the licensure of IXCHIQ® in Brazil, which would be the first potential approval for use in endemic populations.

The U.S. FDA approved IXCHIQ in November 2023, and the Centers for Disease Control and Prevention (CDC) recently adopted the Advisory Committee on Immunization Practices' recommendations on the use of the vaccine in the U.S.

Juan Carlos Jaramillo, M.D., Chief Medical Officer of Valneva, said in a press release, "We are highly encouraged by these data, as they reinforce the strong immunity and safety observed in adults and the elderly, upon which FDA approval was granted."

"Given the substantial risk that chikungunya presents to individuals residing in or traveling to endemic regions, it's imperative to ensure the vaccine is available to all age groups. This broader accessibility can help provide protection and mitigate the burden of this debilitating illness."

Three marketing applications are under review by the European Medicines Agency, Health Canada, and the Brazilian Health Regulatory Agency, with potential approvals in 2024. 

The CDC recently issued an updated Level 2 Travel Health Advisory confirming chikungunya vaccination is recommended for adults traveling to a destination with a current CHIKV outbreak.

Vaccine Treats: 
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Image: 
Image Caption: 
US CDC Chikungunya virus case map May 2024
Live Blog Update Author: 
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Location Tags: 
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Vaccine: 
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