End-stage Renal Disease Clinical Trial
Official title:
Modulation of Gut Microbiota in End-stage Renal Disease: A Pilot Study
In end-stage renal disease (ESRD) cardiovascular and infectious complications are common. The gut microbiome might play an important pathophysiological role. ESRD is hypothesized to be associated with profound alterations of gut microbiome and gut permeability. The investigators aim to test whether a multispecies probiotic mixture is able to revert the microbiome changes and decrease gut permeability. Furthermore the investigators aim to test whether this improvement in microbiome composition and gut permeability is also associated with improvements in endotoxemia, uremia and cardiovascular risk factors.
Chronic kidney disease (CKD) has a prevalence of 10% in the general population and up to 20%
in high-risk groups, such as patients with diabetes. Despite the widespread availability of
renal replacement therapy in the western world, mortality of patients with end-stage renal
disease (ESRD) is still high. The life expectancy of patients with renal replacement therapy
in Austria is reduced by more than 50%.
Patients on renal replacement therapy exhibit an increased cardiovascular mortality (10-30
fold higher than in the general population) associated with accelerated vascular
calcification. The KIDNEY DISEASE IMPROVING GLOBAL OUTCOMES (KDIGO)-work group introduced the
term CKD-Mineral and Bone Disorder (CKD-MBD) which describes a clinical syndrome encompassing
mineral, bone, and calcific cardio-vascular abnormalities that develop as a complication of
CKD. This syndrome emerges as a result of a declining kidney function and is characterized by
changes of circulating levels of parathyroid hormone (PTH), 25-hydroxyvitamin D
(25(OH)D),1,25-dihydroxyvitamin D (1,25(OH)2D), other vitamin D metabolites and fibroblast
growth factor-23 (FGF-23). The ability of the failing kidneys to excrete phosphate is
diminished and hyperphosphatemia occurs. High phosphate levels together with calcium as well
as low concentrations of fetuin A, the main calcification inhibitor under physiological
conditions, lead to increased vascular and extravascular calcification and renal bone
disease. Another important calcification inhibitor is the vitamin K2-dependent matrix
Gla-protein (MGP). Dialysis patients exhibit a low vitamin K intake and suffer substantially
from vitamin K deficiency. Insufficient vitamin K intake leads to the production of
non-carboxylated, inactive MGP and deficiency of carboxylated MGP may contribute
substantially to the development and progression of arterial calcification. Bacterial
infection and sepsis, although decreasing over the last decades, also account for up to 20%
of deaths in ESRD-patients and are the second most common cause of mortality and
hospitalization. Mortality due to sepsis is 100 - 300 times higher in dialysis patients as
compared to the general population. The mechanisms of the increased susceptibility to
infection are unclear but recent studies suggest that in patients with ESRD, innate immune
response is defective. One reason for defective innate immunity might lie in an increased
risk for endotoxemia. Hemodialysis (HD)-induced regional splanchnic ischemia leads to
increased gut permeability and consecutive endotoxin translocation. This possibly results in
alterations in gut microbiome composition.
Recently profound alterations of the composition of the gut microbiome in ESRD have been
shown. In ESRD subjects, more Firmicutes, Actinobacteria and Proteobacteria and fewer
Sutterellaceae, Bacteroidaceae, and Lactobacillaceae were observed relative to controls. The
frequent use of antibiotics, phosphate binders and an often polypragmatic drug consumption
has a considerable impact on the microbiome of ESRD-patients.
These alterations of gut microbiota can impact on several mechanisms in ESRD. Gut bacteria
produce vitamin K and the microbiome composition might therefore play a pivotal role in
providing enough vitamin K for a sufficient carboxylation of MGP, a potent inhibitor of
arterial calcification. Treatment with vitamin K antagonists, for example, has been
associated with a 10 fold increased risk for the development of calcification and
calciphylaxis, a life threatening calcifying arteriolopathy in CKD-patients. Furthermore the
gut is a potential source of endotoxin in patients with ESRD, due to translocation of
bacterial products across the gastrointestinal barrier. In ESRD the presence of endotoxin is
an independent predictor for mortality. Ultrafiltration during hemodialysis treatment leads
to critical ischemia in the splanchnic vascular bed, thus adversely affecting the integrity
of the gut barrier. Disruption of gut barrier function in ESRD allows translocation of
endotoxin and bacterial metabolites to the systemic circulation, which contributes to
inflammation and uremia and prompts progression of the disease. Furthermore, subclinical
inflammation in ESRD-patients has been shown to promote progression of cardiovascular disease
as well. The gut microbiome also impacts on glucose metabolism and plays a critical role in
obesity and the development of insulin resistance and type 2 diabetes. Protein fermentation
by gut microbiota generates toxic metabolites and many of the known uremic toxins are of
intestinal origin, including p-cresol and indoxyl sulfate. Modulation of the microbiome can
contribute to the reduction/elimination of uremic toxins.
Improving the poor prognosis of ESRD patients is an ongoing challenge. An increased awareness
of the limitations in conventional dialysis techniques has renewed interest in alternative
therapeutics in recent years. An unmet clinical need for adjuvant therapeutic strategies
persists in patients whether renal transplantation is intended or not. Supplementation of
probiotics and thereby targeting the intestine, an important source of endotoxin and uremic
toxins, might be a promising approach to partly overcome the high morbidity and mortality in
ESRD patients. Probiotics are living beneficial microorganisms, able to gastroduodenal
passage and maintain viability throughout the gut. Feasibility of gut microbiome modulation
in ESRD was shown in animal and human settings. However, so far, it is unknown to what extend
probiotics are able to re-establish gut microbiome homeostasis in ESRD. Furthermore the
effects of a probiotic intervention on cardiovascular risk factors, inflammation, gut barrier
and uremia have not been studied in detail yet.
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