Ridinilazole


Ridinilazole is a non-absorbable small molecule antibiotic for oral administration to treat Clostridioides difficile infection. The Centers for Disease Control and Prevention estimates 500,000 cases of CDI per year and on average 29,000 deaths per year attributed to CDI in the United States. The CDC estimates a similar number of cases in the European Union each year.
its mechanism of action "remains to be fully determined." However, Summit Therapeutics believes that ridinilazole may be able to selectively target C. difficile without causing collateral damage to natural gut flora and thus is able to reduce CDI recurrence rate. In preclinical studies, ridinilazole showed a potent bactericidal effect against all strains of C. difficile tested.
Ridinilazole was designated as a Qualified Infectious Disease Product and was granted Fast Track status by the U.S. FDA. This status is reserved for drugs designed to treat diseases where there is currently a gap in the treatment, or a complete lack thereof. This Fast Track status adds five more years of exclusivity for ridinazole.
Speaking about Ridinilazole, Robert Duggan states, “Targeted antibiotics have the potential to improve the way infectious diseases are treated by targeting the infectious bacteria and minimising the damage of the healthy and protective microbiome. In C. difficile infection, the selective targeting of the infectious bacteria has significant potential to reduce recurrence and improve patient outcomes.”

Commercialization

Ridinilazole is manufactured by Summit Therapeutics. Summit Therapeutics plans to partner with another pharmaceutical company to begin Phase 3 trials. They predict for both the US and EU launch to occur in 2021 with peak sales of £930 million. Summit will receive a flat 20% royalty rate. Models predict that royalties will rise from £25.6 million in FY2022 to £75.2 in FY2027. Ridinilazole has been de-risked with positive Phase 2 data.
Summit Therapeutics estimates that the price will be $1,200 for one course of therapy in the US and approximately 20% less in the EU. This is in contrast to Merck's Dificid which was priced at $2,800 per course of therapy. Dificid did not sell well because it cost nearly four times as much as the generic vancomycin alternatives.
According to H.C. Wainwright, ridinilazole is currently undervalued since ridinilazole allows the patients gut microflora to be preserved which helps prevents deadly recurrent infections and allows for the use of ridinilazole as a first line therapy, in contrast with antibiotics already on the market.

Intellectual Property

Patents

Ridinilazole is not available for composition of matter patent protection worldwide. However, ridinilazole still has several other patents in several key domestic and international markets, including the three biggest markets:
Although ridinilazole has been patented, Summit Therapeutics has not yet signed a partnership to continue with Phase III clinical trials. Therefore, the patent life may need to be extended.

Competitors

There are several other competitors with new drug candidates targeting C. difficile. The most promising of these other drugs is Merck's Zinplava which was recently approved. Market analysts don't know how the approval of bezlotoxumab will affect the valuation of ridinilazole. Bezlotoxumab is not an antibiotic, but it is used to in conjunction with antibiotics to increase their effectiveness in treating CDI. Other pharmaceutical companies working on drugs to treat CDI include Synthetic Biologics, Sanofi, and Shire.

Regulatory Information

Phase I & II Clinical Trials

Ridinilazole was approved for Phase III clinical trials after a successful Phase II study showed that ridinilazole was tolerated at all doses and has a highly selective profile. Ridinilazole showed a sustained clinical response. The study was a double-blind, randomized, active-controlled, multi-center trial with 100 patients comparing ridinilazole to vancomycin. Adults in the trial had a clinical diagnosis of CDI with no more than 24 hours of antimicrobial treatment and no more than 3 cases of CDI in the previous 12 months. One-half of the study participants received a 200 mg of ridinilazole twice a day; the other half received 125 mg of vancomycin four times a day.
In a Phase II proof-of-concept trial in CDI patients, ridinilazole showed statistical superiority in SCR rates compared to the standard of care, vancomycin. In this trial, SCR was defined as clinical cure at end of treatment and no recurrence of CDI within 30 days of the end of therapy. SCR rates were 66.7% for ridinilazole compared to 42.4% for vancomycin. Rates of clinical cure at the end of treatment was 77.8%. There was also a reduction in recurrent CDI: 34.8% with ridinilazole. Ridinilazole might be more useful for at-risk groups. This includes patients aged 75 or greater, patients with severe cases of CDI, and patients with prior episodes.
There was no increase in adverse effects associated with ridinilazole. Ridinilazole decreased gastrointestinal adverse effects. Only 40% of patients reported adverse GI effects, compared to 56% of cases with vancomycin. These results show that ridinilazole might be useful in the aforementioned at-risk groups and as a first line treatment. Lowering the rate of recurrent CDI via use of ridinilazole could save the U.S. healthcare system $30,000 per patient due to a decreased number of hospitalizations.
, there is currently an ongoing Phase II clinical trial underway in the US comparing ridinilazole with fidaxomicin in the treatment of CDI.

Phase III Clinical Trials

The partner with Summit Therapeutics must conduct 2 randomized, double-blind trials comparing ridinilazole to vancomycin or fidaxomicin. These trials will take two to three years, thereby predicting a 2021 commercial launch.