After three decades of rapid and impressive technical development in renal replacement therapy, dialysis patients were still faced with a high morbidity and mortality risk. Morbidity was reflected in frequent hospitalizations for solving vascular access dysfunction, infection-related problems, cardiovascular events and other dialysis-related pathologies, including ß₂-microglobulin amyloidosis. Mortality was high, averaging 17% per year worldwide with large inter-country variations (Japan 7%, Europe 15% and USA 25%). Causes of mortality were predominantly cardiovascular diseases (ischemic cardiac, stroke, arrhythmia, sudden death, etc.) in about 50% of patients, followed by infection, cachexia and various other causes. Several reports identified that, despite multiple adjustments for age, case-mix and comorbidity, the main source of morbidity and mortality in chronic kidney disease patients was the practice of conventional three times weekly, short sessions with low-flux hemodialyzers and acetate-buffered dialysate.

Several hypotheses were proposed to explain the shortfalls in renal replacement therapy. It is not our intention to review the details of the pathophysiological pathways elaborated to elucidate these findings. However, it is important to mention the putative causes and barriers of conventional hemodialysis in order understand the need for designing a more efficient and physiological renal replacement modality. Briefly, the term ‘dialysis-related pathology’ addresses five main pathophysiological features of the earlier dialysis therapy. First, the incomplete correction of uremic abnormalities by dialysis, this led to the chronic retention of particular toxic compounds [1] and was the focus of attention of the ‘uremic toxin group’. In fact, two theories were being followed at that time: the ‘small molecule hypothesis’ and the ‘middle molecule hypothesis’. The ‘small molecule hypothesis’ was supported by the US nephrology community that uniformly used the ‘dialysis dose’ concept based on urea Kt/V ratio [2-4]. The ‘middle molecule hypothesis’, on the other hand, was supported by the European nephrology community that postulated that chronic accumulation of larger molecular size toxins, which are poorly cleared by conventional hemodialysis, were implicated in the high mortality of dialysis patients [5]. The second pathophysiological feature was the ‘bioincompatibility’ of the hemodialysis system. The generation of bioactive byproducts from protein and cell activation systems led to repetitive inflammation and immune-mediated insults. In this context, two components of the hemodialysis system were identified as triggers for biologic reactions: the biochemical composition of the dialysis membrane (cellulosic versus synthetic polymers) and the microbial contamination of the dialysis fluid [6]. The third pathophysiological aspect of dialysis was the ‘hemodynamic instability’ of short treatment schedules, accounting for maltolerance in 30-40% of dialysis sessions. Hypotensive episodes induced by dialysis sessions were soon recognized as repetitive cardiac ischemic insults leading, potentially, to myocardial lesions. Apart from high ultrafiltration rate, another factor implicated was the sodium acetate buffering of the dialysate; this was finally proven to play a major role by its vasodilatory and negative inotropic roles in the maltolerance of dialysis sessions [7-9]. The fourth pathophysiological facet was the ‘unphysiology’ of intermittent therapy that maintained dialysis patients in a permanent unstable situation by creating a ‘peak-and-valley’ profile of the patient’s internal milieu [10]. Finally, the fifth characteristic was the inability to correct ‘metabolic abnormalities’ of chronic kidney patients, such as anemia, vitamin D deficiency, lipid disorders and mineral and bone disorders [11].