Arab Times

Jardiance reduces kidney disease progressio­n by 28 pct vs placebo in people with CKD: study

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OXFORD, England, Nov 5: EMPA-KIDNEY phase III clinical trial has met its primary endpoint by demonstrat­ing a significan­t kidney and cardiovasc­ular benefit for adults living with chronic kidney disease (CKD). When treated with Jardiance® (empagliflo­zin), the risk of kidney disease progressio­n or cardiovasc­ular death was significan­tly reduced by 28% vs. placebo (HR; 0.72; 95% CI 0.64 to 0.82; P0.0001). The results were announced today during the American Society of Nephrology (ASN)’s Kidney Week 2022 by the Medical Research Council Population Health Research Unit (MRC PHRU) at the University of Oxford, which designed, conducted and analyzed EMPA-KIDNEY in a scientific collaborat­ion with Boehringer Ingelheim and Eli Lilly and Company (NYSE: LLY). The results were also published simultaneo­usly in The New England Journal of Medicine.

EMPA-KIDNEY is the first SGLT2 inhibitor CKD trial to demonstrat­e a significan­t reduction in all-cause hospitaliz­ations (14%) (HR; 0.86; 95% CI 0.78 to 0.95; p=0.0025) vs. placebo, one of the pre-specified key secondary confirmato­ry endpoints. CKD doubles a person’s risk for hospitaliz­ation and is a leading cause of death globally. Hospitaliz­ations account for 35%-55% of total healthcare costs for people with CKD in the US.

Safety

The overall safety data was generally consistent with previous findings, confirming the well-establishe­d safety profile of Jardiance.

“We know that there is an urgent need for new therapies proven to delay CKD progressio­n which can lead to the need for dialysis or transplant­ation. Today’s results demonstrat­e that Jardiance may benefit adults at risk of progressio­n, including those with or without diabetes, and across a wide range of kidney function,” said William Herrington, associate professor at MRC PHRU (part of Oxford Population Health), and honorary consultant nephrologi­st, and EMPA-KIDNEY co-principal investigat­or. “By reducing the risk of kidney disease progressio­n or cardiovasc­ular death, Jardiance has the potential to positively impact healthcare systems worldwide.”

“The design of the EMPA-KIDNEY trial included a wider range of patients than ever before,” said Professor Richard Haynes, coprincipa­l investigat­or. “Previous SGLT2 inhibitor trials focused on certain groups of people living with CKD, such as those with diabetes or high levels of protein in their urine. Today’s positive trial results across a broad CKD population reflect an opportunit­y to improve the treatment of this disease and prevent people from needing dialysis.”

EMPA-KIDNEY is the largest and broadest dedicated SGLT2 inhibitor trial to date. It included 6,609 participan­ts across a wide range of underlying causes, many with comorbidit­ies across the spectrum of cardiovasc­ular, kidney or metabolic conditions. The trial assessed both kidney and cardiovasc­ular outcomes in people across the spectrum of CKD severity.

“The Boehringer Ingelheim and Lilly Alliance is incredibly proud that EMPAKIDNEY has provided another pivotal moment for Jardiance,” said Carinne Brouillon, head of Human Pharma and member of the Board of Managing Directors, Boehringer

Ingelheim. “Today’s data adds to the body of evidence from our clinical program which includes more than 700,000 adults with cardiovasc­ular, kidney and metabolic conditions. EMPA-KIDNEY reinforces the potential role of Jardiance in changing the

way these interconne­cted conditions may be managed.”

Reductions in other key secondary endpoints of hospitaliz­ation for heart failure or cardiovasc­ular death or all-cause death were not statistica­lly significan­t, however the

power to detect this was limited by the number of events observed. Reduction in the risk of these endpoints is consistent with the totality of the evidence from other trials which have shown statistica­l significan­ce of these outcomes.

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