Efficacy and Safety of a Novel Nicotinamide Modified-Release Formulation in the Treatment of Refractory Hyperphosphatemia in Patients Receiving Hemodialysis—A Randomized Clinical Trial

Ketteler, Markus; Wiȩcek, Andrzej; Rosenkranz, Alexander R.; Rekowski, Jan; Hellmann, Burkhard; Karus, Michael; Ammer, Richard

doi:10.1016/j.ekir.2020.12.012

Cited by 12 publications

(13 citation statements)

References 54 publications

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“…1,25‐dihydroxyvitamin D, which has been shown to upregulate intestinal NPT2b in preclinical models, 24,25,50 also increases phosphate absorption 11,51 and transporter‐mediated phosphate absorption 16 in ESRD patients, suggesting a role for NPT2b in human phosphate absorption. Nicotinamide therapy reduces hyperphosphatemia in patients on dialysis 52 . Preclinical studies indicate the effect of nicotinamides is through decreased NPT2b mediated transport, 20,53 providing additional evidence for an appreciable role of NPT2b in human phosphate absorption.…”

Section: Discussionmentioning

confidence: 98%

“…Nicotinamide therapy reduces hyperphosphatemia in patients on dialysis. 52 Preclinical studies indicate the effect of nicotinamides is through decreased NPT2b mediated transport, 20 , 53 providing additional evidence for an appreciable role of NPT2b in human phosphate absorption. Two NPT2b inhibitors that were reported to decrease phosphate absorption in preclinical models recently advanced to the clinic.…”

Section: Discussionmentioning

confidence: 99%

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Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models

Wang

et al. 2022

Pharmacology Res & Perspec

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An excess phosphate burden in renal disease has pathological consequences for bone, kidney, and heart. Therapies to decrease intestinal phosphate absorption have been used to address the problem, but with limited success. Here, we describe the in vivo effects of a novel potent inhibitor of the intestinal sodium‐dependent phosphate cotransporter NPT2b, LY3358966. Following treatment with LY3358966, phosphate uptake into plasma 15 min following an oral dose of radiolabeled phosphate was decreased 74% and 22% in mice and rats, respectively, indicating NPT2b plays a much more dominant role in mice than rats. Following the treatment with LY3358966 and radiolabeled phosphate, mouse feces were collected for 48 h to determine the ability of LY3358966 to inhibit phosphate absorption. Compared to vehicle‐treated animals, there was a significant increase in radiolabeled phosphate recovered in feces (8.6% of the dose, p < .0001). Similar studies performed in rats also increased phosphate recovered in feces (5.3% of the dose, p < .05). When used in combination with the phosphate binder sevelamer in rats, there was a further small, but not significant, increase in fecal phosphate. In conclusion, LY3358966 revealed a more prominent role for NPT2b on acute intestinal phosphate uptake into plasma in mice than rats. However, the modest effects on total intestinal phosphate absorption observed in mice and rats with LY3359866 when used alone or in combination with sevelamer highlights the challenge to identify new more effective therapeutic targets and/or drug combinations to treat the phosphate burden in patients with renal disease.

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Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models

Wang

et al. 2022

Pharmacology Res & Perspec

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“…However, the study that did not observe a decrease in serum phosphate levels, the COMBINE trial (NCT02258074), had a dropout rate of 25% in the NAM group due to pill burden and gastrointestinal symptoms [191]. In the NICOREN (NCT01011699) and NOPHOS trials, the majority of reported adverse events are also gastrointestinal upset, as well as thrombocytopenia, anemia and pruritus [193,194]. However, a meta-analysis of the efficacy and safety of NAM on phosphate metabolism in hemodialysis patients revealed that thrombocytopenia was the only significant adverse effect caused by NAM [195].…”

Section: Clinical Interventionsmentioning

confidence: 99%

NAD+ Metabolism and Interventions in Premature Renal Aging and Chronic Kidney Disease

Chanvillard

Tammaro

Sorrentino

2022

Cells

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Premature aging causes morphological and functional changes in the kidney, leading to chronic kidney disease (CKD). CKD is a global public health issue with far-reaching consequences, including cardio-vascular complications, increased frailty, shortened lifespan and a heightened risk of kidney failure. Dialysis or transplantation are lifesaving therapies, but they can also be debilitating. Currently, no cure is available for CKD, despite ongoing efforts to identify clinical biomarkers of premature renal aging and molecular pathways of disease progression. Kidney proximal tubular epithelial cells (PTECs) have high energy demand, and disruption of their energy homeostasis has been linked to the progression of kidney disease. Consequently, metabolic reprogramming of PTECs is gaining interest as a therapeutic tool. Preclinical and clinical evidence is emerging that NAD+ homeostasis, crucial for PTECs’ oxidative metabolism, is impaired in CKD, and administration of dietary NAD+ precursors could have a prophylactic role against age-related kidney disease. This review describes the biology of NAD+ in the kidney, including its precursors and cellular roles, and discusses the importance of NAD+ homeostasis for renal health. Furthermore, we provide a comprehensive summary of preclinical and clinical studies aimed at increasing NAD+ levels in premature renal aging and CKD.

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“…The dose-limiting adverse effect of niacin is skin flushing, caused by an increase in the vasodilator prostacyclin. Additional adverse effects of niacin and NAM include pruritus, skin rash, gastrointestinal disturbances and thrombocytopaenia [ 18 , 19 ]. Liver cell damage has been observed at intakes of niacin as little as 750 mg/day [ 20 ].…”

Section: Clinical Use Of Vitamin B3mentioning

confidence: 99%

“…Vitamin B3 vitamers have been tested in clinical trials for the treatment of hyperphosphataemia in CKD ( Figure 3B and Table 1 ). In CKD, niacin [ 26 ] or NAM [ 18 , 19 , 30 ], either alone or in combination with other phosphate binders, reduced serum phosphate levels in most trials through inhibition of the expression of the intestinal phosphate transporter NaPi2b by poorly characterized mechanisms. The main metabolite of NAM, N-methyl-2-pyridone-5-carboxamide, may accumulate in haemodialysis patients [ 19 ].…”

Section: Vitamin B3 In Ckdmentioning

confidence: 99%

Nicotinamide and acute kidney injury

Fontecha‐Barriuso

Lopez-Díaz

Carriazo

et al. 2021

Clinical Kidney Journal

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In a recent issue of ckj, Piedrafita et al reported that urine tryptophan and kynurenine are reduced in cardiac bypass surgery patients that develop acute kidney injury (AKI), suggesting reduced activity of the kynurenine pathway of nicotinamide adenine dinucleotide (NAD+) synthesis from tryptophan. However, nicotinamide (NAM) supplementation aiming at repleting NAD+ did not replete kidney NAD+ and did not improve glomerular filtration or reduce histological injury in ischemic-reperfusion kidney injury in mice. The lack of improvement of kidney injury is partially at odds with prior reports that did not study kidney NAD+, glomerular filtration or histology in NAM-treated wild-type mice with AKI. We now present an overview of research on therapy with vitamin B3 vitamers and derivate molecules [niacin, NAM, nicotinamide riboside (NR), NRH and nicotinamide mononucleotide (NMN)] in kidney injury, including an overview of ongoing clinical trials, and discuss the potential explanations for diverging reports on the impact of these therapeutic approaches on preclinical acute and chronic kidney disease.

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Efficacy and Safety of a Novel Nicotinamide Modified-Release Formulation in the Treatment of Refractory Hyperphosphatemia in Patients Receiving Hemodialysis—A Randomized Clinical Trial

Cited by 12 publications

References 54 publications

Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models

Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models

NAD+ Metabolism and Interventions in Premature Renal Aging and Chronic Kidney Disease

Nicotinamide and acute kidney injury

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