1503. Engraftment of Investigational Microbiome Drug, SER-262, in Subjects Receiving Vancomycin Is Associated with Reduced Rates of Recurrence after Primary Clostridium Difficile Infection (CDI)

Ford, Christopher B.; Litcofsky, Kevin; McGovern, Barbara; Pardi, Darrell S.; Nathan, Richard; Hansen, Val; Brennan, Robert T.; Pullman, John; Bernardo, Patricia; Tomlinson, Amelia D.; Horgan, Kevin J.; Bryant, Jessica A.; Walsh, Emily; Rodriguez, Michelle; Rogalin, Henry B.; Wang, Elaine; Henn, Matt

doi:10.1093/ofid/ofz360.1367

Cited by 7 publications

(5 citation statements)

References 0 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…SER-262 is able to compete with C. difficile for up to 90% of its carbon sources, and 10 of 12 strains included in the synthetic community convert primary to secondary bile acids to inhibit the growth and reduce the toxicity of C. difficile. SER-262 was safe and well tolerated in patients in a phase I clinical trial (NCT02830542), but it did not meet its primary endpoint of reducing overall rates of CDI in patients following antibiotic treatment (Ford et al, 2019), although efficacy may differ depending on the specific antibiotic used.…”

Section: Cellular Immunotherapymentioning

confidence: 99%

“…Seres SER-262 is a rationally designed synthetic microbial community designed to include highly prevalent bacterial species isolated from healthy donors from the Human Microbiome Project (Turnbaugh et al, 2007) and successful iterations of SER-109 (J.R. Wortman et al, 2016, conference). SER-262 contains a proprietary blend of spores from 12 bacterial strains including several Firmicutes species from the Lachnospiraceae, Erysipelatrichaceae, Peptostreptococcaceae, and Clostridiaceae families (Ford et al, 2019). SER-262 is able to compete with C. difficile for up to 90% of its carbon sources, and 10 of 12 strains included in the synthetic community convert primary to secondary bile acids to inhibit the growth and reduce the toxicity of C. difficile.…”

Section: Cellular Immunotherapymentioning

confidence: 99%

See 1 more Smart Citation

Synthetic biology in the clinic: engineering vaccines, diagnostics, and therapeutics

Tan

Letendre

Collins

et al. 2021

Cell

View full text Add to dashboard Cite

Section: Cellular Immunotherapymentioning

confidence: 99%

Section: Cellular Immunotherapymentioning

confidence: 99%

Synthetic biology in the clinic: engineering vaccines, diagnostics, and therapeutics

Tan

Letendre

Collins

et al. 2021

Cell

View full text Add to dashboard Cite

“… ● Delivered as doubly encapsulated V-caps ® stored at 2 to 8°C until dispensing. Phase 2 trial complete, halted further development CP-101 94 , 119 Finch Therapeutics ● Oral Full-Spectrum MicrobiotaTM (broad consortium) ● Lyophilized capsule of, full-spectrum microbiota containing diverse microorganisms Further development halted Designed oral capsules VE-303; 103 , 104 Vendanta Biosciences ● A defined consortium of 8 commensal strains of clonally derived and distinct Clostridium species (5 strains from Clostridia cluster XIVa, 2 from cluster IV, and 1 from cluster XVII) ● Enteric capsules each containing 1×10 8 CFU of lyophilized bacteria from each species for a total 8×10 8 CFU of bacteria in 400mg combined with sucrose, histidine, yeast extract, cysteine, and other excipients Phase 2 trial complete NTCD-M3 (VP20621 ); 105 , 120 Shire pharmaceuticals ● Enteric capsules containing a non-toxigenic C. difficile strain M3 Phase 2 trial complete MET-2; 93 Microbial Ecosystem Therapeutics ● A proprietary consortium of 40 commensal bacterial species from strains which are then purified and combined as a lyophilized product into capsules for oral delivery Phase 1 trial complete ART24 (ADS024) 9 Adiso Therapeutics ● A single-strain of Bacillus velezensis lyophilized and administered via capsule Phase 1 DSM33864 DifProtec(TM) 117 Novozymes A/S ● A single strain probiotic dietary supplement capsule containing Bacillus velezensis Phase = N/A SER-262 121 Seres Therapeutics ● Cultivated Eubacterial Spore Suspension, Encapsulated Ecobiotic ® ● A rationally designed, multi-strain microbiome therapeutic produced synthetically by in vitro anaerobic fermentation to produce commensal bacteria in spore form Phase 1 complete Abbreviation : CFU, colony-forming unit...…”

Section: Lbps and Fmt: Similarities Differences And The Intricacies O...mentioning

confidence: 99%

Microbiota-Based Live Biotherapeutic Products for Clostridioides Difficile Infection- The Devil is in the Details

Monday,

Tillotson,

Chopra

2024

IDR

View full text Add to dashboard Cite

Clostridioides difficile infection (CDI) remains a significant contributor to healthcare costs and morbidity due to high rates of recurrence. Currently, available antibiotic treatment strategies further disrupt the fecal microbiome and do not address the alterations in commensal flora (dysbiosis) that set the stage for CDI. Advances in microbiome-based research have resulted in the development of new agents, classified as live biotherapeutic products (LBPs), for preventing recurrent CDI (rCDI) by restoring eubiosis. Prior to the LBPs, fecal microbiota transplantation (FMT) was available for this purpose; however, lack of large-scale availability and safety concerns have remained barriers to its widespread use. The LBPs are an exciting development, but questions remain. Some are derived directly from human stool while other developmental products contain a defined microbial consortium manufactured ex vivo, and they may be composed of either living bacteria or their spores, making it difficult to compare members of this heterogenous drug class to one another. None have been studied head-to head or against FMT in preventing rCDI. As a class, they have considerable variability in their biologic composition, biopharmaceutic science, route of administration, stages of development, and clinical trial data. This review will start by explaining the role of dysbiosis in CDI, then give the details of the biopharmaceutical components for the LBPs which are approved or in development including how they differ from FMT and from one another. We then discuss the clinical trials of the LBPs currently approved for rCDI and end with the future clinical directions of LBPs beyond C. difficile .

show abstract

“…Understandably creation of a 'synthetic' FMT is a desired goal in terms of reproducibility, safety, regulation and scalability, as well as commercial opportunity. Results of 'manufactured' FMT to date have shown promise, 134,135 and further trials are ongoing [ClinicalTrials.gov identifiers: NCT03244644, NCT03788434 and NCT04208958 to list a few], but there remains a way to go before we are likely to see these entering widespread practice.…”

Section: Delivery Route Dosage and Preparation Techniquesmentioning

confidence: 99%

The role of faecal microbiota transplantation: looking beyondClostridioides difficileinfection

Goldenberg

2021

Therapeutic Advances in Infection

View full text Add to dashboard Cite

Faecal microbiota transplantation (FMT) is the transfer of screened and minimally processed faecal material from a ‘healthy’ donor to ‘diseased’ recipient. It has an established role, and is recommended as a therapeutic strategy, in the management of recurrent Clostridioides difficile infection (CDI). Recognition that gut dysbiosis is associated with, and may contribute to, numerous disease states has led to interest in exploiting FMT to ‘correct’ this microbial imbalance. Conditions for which it is proposed to be beneficial include inflammatory bowel disease, irritable bowel syndrome, liver disease and hepatic encephalopathy, neuropsychiatric conditions such as depression and anxiety, systemic inflammatory states like sepsis, and even coronavirus disease 2019. To understand what role, if any, FMT may play in the management of these conditions, it is important to consider the potential risks and benefits of the therapy. Regardless, there are several barriers to its more widespread adoption, which include incompletely understood mechanism of action (especially outside of CDI), inability to standardise treatment, disagreement on its active ingredients and how it should be regulated, and lack of long-term outcome and safety data. Whilst the transfer of faecal material from one individual to another to treat ailments or improve health has a history dating back thousands of years, there are fewer than 10 randomised controlled trials supporting its use. Moving forward, it will be imperative to gather as much data from FMT donors and recipients over as long a timeframe as possible, and for trials to be conducted with rigorous methodology, including appropriate control groups, in order to best understand the utility of FMT for indications beyond CDI. This review discusses the history of FMT, its appreciable mechanisms of action with reference to CDI, indications for FMT with an emerging evidence base above and beyond CDI, and future perspectives on the field.

show abstract

1503. Engraftment of Investigational Microbiome Drug, SER-262, in Subjects Receiving Vancomycin Is Associated with Reduced Rates of Recurrence after Primary Clostridium Difficile Infection (CDI)

Cited by 7 publications

References 0 publications

Synthetic biology in the clinic: engineering vaccines, diagnostics, and therapeutics

Synthetic biology in the clinic: engineering vaccines, diagnostics, and therapeutics

Microbiota-Based Live Biotherapeutic Products for Clostridioides Difficile Infection- The Devil is in the Details

The role of faecal microbiota transplantation: looking beyondClostridioides difficileinfection

Contact Info

Product

Resources

About