New phase 1B data support further investigation into Adiso Therapeutic's prospective treatment.
This article was originally published by HCPLive®. It has been lightly edited.
A promising live biotherapeutic agent in development for the prevention of recurrent Clostridiodes difficile infection (rCDI) now has early-stage data supporting its safety, tolerability, and potential efficacy in patients recovering from CDI.
In new phase 1B data presented at the American College of Gastroenterology (ACG) 2023 Annual Scientific Meeting in Vancouver, British Columbia, Canada, an international team of investigators reported that ADS024, an investigative, orally administered single-strain live biotherapeutic product (Bacillus velezensis) from Adiso Therapeutics was associated with CDI toxin level reduction over 4 weeks while maintaining favorable safety and tolerability vs placebo in patients at risk of rCDI.
Investigators led by Jessica R. Allegretti, MD, MPH, of Brigham and Women's Hospital and Harvard Medical School, conducted the phase 1B, randomized, controlled, double-blind, multicenter trial to evaluate the safety and efficacy of ASD024. Similar to previously investigated live biotherapeutics, the understood potential of the agent in the prevention of rCDI is aspirational.
“Recurrence of CDI is due to the failure of antibiotics to eradicate spores that can germinate post-treatment,” Allegretti and colleagues wrote. “[ADS024] kills CDI and degrades its toxins.”
Investigators enrolled patients cured of a recent CDI following a standard-care course of antibiotics into the trial. Two cohorts of patients were randomized 3:1 to either 5 x 109 CFU/daily oral ADS024 or placebo. Cohort A (n = 8) received care for 7 days; cohort B (n = 28) received care for 28 days. All patients were followed for 6 months after their final dose.
The team sought a primary end point of safety and tolerability associated with ADS024, as well as key secondary end points of evaluation of recurrence, time to recurrence (TTR), change in CDI toxin levels from baseline, presence of ADS024 in the system, and microbiome analyses.
Among the 36 trial participants, 17 had experienced rCDI. Another 31 (86.1%) completed the phase 1b trial. The median age was 58 years, and 69% of patients were female. Median duration of treatment exposure was 28 (range, 2–28) days.
Among the 27 patients to receive ADS024 in either cohort, 17 (63) experienced 1 or more treatment emergent adverse events (TEAEs). Fifty-two percent of patients reported a mild to moderate TEAE. The most common events were diarrhea (n = 8), flatulence (n = 7) and abdominal pain (n = 6). Among the 4 (15%) patients to report a serious TEAE, 2 reported CDI; the other 2 reported a wound infection and abdominal pain.
Regarding tolerability, Allegretti and colleagues reported that 4 (15%) treated patients experienced rCDI, with a median TTR of 10 (range, 2-14) days vs just 1 patient on placebo (TTR, 108 days). They noted a temporal association between increased CDI counts and toxin levels, and recurrence. However, counts and toxin levels declined overall from baseline to end of dosing with ADS024 vs placebo.
Alhough ADS024 was detected in 7 (29.2%) of the patients receiving ADS024, it did not persist after the end of the dosing period.
“No significant changes in alpha-diversity between treatment arms were detected,” the investigators noted. “Significant differences in beta-diversity occurred over time and between treatment arms.”
The team concluded that ADS024 was linked to declining CDI count and toxin levels from baseline to week 4 vs an increase with placebo, and patients at risk of rCDI reported low variance and alpha- and beta-diversity with the investigative drug.
“ADS024 appears safe and well tolerated and CDI recurrence frequency was similar between arms in this small study,” they wrote. “These findings warrant further investigation of ADS024.”
Reference
Allegretti JR, Gupta R, Aguilar H, Pullman J, et al. P0173 - ADS024, a Bacillus velezensis strain, for prevention of recurrence of Clostridioides difficile infection: results from a randomized, placebo-controlled, double-blind, phase 1b study. Paper presented at: ACG 2023 Annual Scientific Meeting; Vancouver, British Columbia, Canada.; October 20-25, 2023.
Insurance Insights: Dr Jason Shafrin Estimates DMD Insurance Value
July 18th 2024On this episode of Managed Care Cast, we're talking with the author of a study published in the July 2024 issue of The American Journal of Managed Care® that estimates the insurance value of novel Duchenne muscular dystrophy (DMD) treatment.
Listen
New AI Tool Identifies Undiagnosed PNH in Health Records
October 30th 2024The machine learning model shows promise in detecting paroxysmal nocturnal hemoglobinuria (PNH) by assessing electronic health records (EHR) data, potentially transforming the diagnostic landscape for rare diseases.
Read More
Zanubrutinib More Effective Than Ibrutinib in Treating Patients With Relapsed/Refractory CLL, SLL
October 30th 2024The long-term response rate for zanubrutinib was better than ibrutinib in patients with relapsed/refractory chronic lymphocytic leukemia (CLL) and small lymphocytic lymphoma (SLL).
Read More