Nutritional management in patients with chronic kidney disease

Sun Moon Kim; Ji Yong Jung

doi:10.3904/kjim.2020.408

Kim and Jung: Nutritional management in patients with chronic kidney disease

Review

Korean J Intern Med 2020;35(6):1279-1290.

Published online: September 23, 2020

DOI: https://doi.org/10.3904/kjim.2020.408

Nutritional management in patients with chronic kidney disease

Sun Moon Kim¹, Ji Yong Jung^2,³

¹Division of Nephrology, Department of Internal Medicine, Chungbuk National University Hospital, Cheongju, Korea

²Division of Nephrology, Department of Internal Medicine, Gachon University Gil Medical Center, Incheon, Korea

³Department of Internal Medicine, Gachon University College of Medicine, Incheon, Korea

Correspondence to Ji Yong Jung, M.D. Division of Nephrology, Department of Internal Medicine, Gachon University Gil Medical Center, 21 Namdong-daero 774beon-gil, Namdong-gu, Incheon 21565, Korea Tel: +82-32-458-2621 Fax: +82-32-460-3431 E-mail: jyjung@gachon.ac.kr

This paper was contributed by The Korean Society of Nephrology.

Received August 10, 2020 Accepted September 9, 2020

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/) which permits unrestricted noncommercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

The global prevalence of chronic kidney disease (CKD) is increasing with the aging of populations worldwide. As kidney function declines, the accumulation of metabolic waste products and excessive electrolytes can significantly impair the health of patients with CKD. As nutritional management of patients with CKD is thought to control uremic symptoms and provide beneficial effects on the progression of kidney dysfunction, the diet of patients with CKD should be an important consideration in their care. Many guidelines recommend limiting protein intake in these patients, as high-protein diets aggravate kidney dysfunction. Excess sodium may be associated with CKD progression and all-cause mortality and, therefore, limiting salt intake is generally recommended. Low potassium is associated with muscle weakness and hypertension, whereas high potassium is associated with cardiac arrhythmia. Therefore, recent guidelines recommend adjusting dietary potassium intake on an individual basis to maintain serum potassium levels within the normal range. Appropriate dietary calcium intake is recommended to maintain calcium balance in patients with CKD G3, G4. Given the many dietary considerations for patients with CKD, effective nutritional management is challenging. Individualized strategies are needed to ensure the best outcome for patients with CKD.

Keywords: Diet, protein-restricted; Nutrients; Progression of chronic kidney disease; Individualization

INTRODUCTION

Chronic kidney disease (CKD) occurs due to structural or functional kidney impairment for more than 3 months, and is divided into five stages according to the decline in glomerular filtration rate (GFR) from early CKD to kidney failure (KF). In Korea, the prevalence rates of CKD and KF have been increasing in recent decades with the increase in the older population and the prevalence of diabetes [1,2]. Chronic inflammation in patients with CKD can induce protein catabolism through increased insulin resistance, and protein catabolism can significantly impair an individual’s nutritional status [3,4]. Patients with CKD may experience hyperkalemia, hyperphosphatemia, anorexia, as well as muscle and fat wasting. Protein-energy wasting (PEW) was first described in 2007 by the International Society of Renal Nutrition and Metabolism as a state of nutritional and metabolic derangements characterized by the loss of systemic body protein and energy stores in patients with non-dialysis CKD and KF [5]. The prevalence of PEW in patients with early to moderate CKD was reported to be 20% to 25%, increasing as kidney dysfunction progresses up to 75% in KF [6]. Malnutrition, decreased physical activity, uremia-induced hypercatabolism, acidosis, and persistent inflammation can all contribute to PEW [7,8], which is associated with increased risks of hospitalization and mortality [9]. Dietary supplementation with adequate protein and energy may reduce PEW. While nutritional therapy for progressive kidney dysfunction remains controversial, previous studies have shown that it can help control uremia, electrolyte and acid-base imbalances, water and salt retention, and mineral and bone disorders (MBD) [3]. Dietary modifications can reduce the accumulation of waste products, which may relieve uremic symptoms and delay the initiation of maintenance dialysis treatment in patients with non-dialysis CKD. Therefore, nutritional management should be considered during all stages of CKD, and all physicians caring for patients with CKD should be aware of the dietary and nutritional requirements of these patients [10]. This review is focused on several aspects of nutritional management in patients with CKD.

PROTEIN

Protein intake is one of the most widely discussed issues in the nutritional management of CKD. A high-protein diet, defined as intake of > 1.2 g protein per kilogram of body weight per day (g/kg/day), has been shown to cause significant deterioration in kidney function [11]. High protein intake increases kidney blood flow and elevates intraglomerular pressure, which leads to higher GFR and more efficient excretion of protein-derived nitrogen products. The hyperfiltration induced by high protein intake has been described in several experimental models and clinical studies [12-16]. High-protein diet-induced glomerular hyperfiltration may have deleterious consequences on the kidney and other organs in the long term [11]. Several studies have shown that long-term exposure to a high-protein diet may cause kidney damage and progressive kidney dysfunction [17,18]. The Nurses’ Health Study evaluated the effects of protein intake on estimated GFR based on serum creatinine (eGFR_cr) decline in 1,624 women over 11 years [17]. The results showed that high protein intake was associated with an eGFR_cr decline among individuals with decreased kidney function (defined as eGFR_cr of 55 to 80 mL/min/1.73 m²) but not in those with normal kidney function. Recently, Jhee et al. [18] reported that a high-protein diet induced glomerular hyperfiltration and a rapid decline of kidney function in the general population. A high-protein diet increased the risk of kidney hyperfiltration and a rapid decline of kidney function in the general population. While the effects of a high-protein diet in individuals with normal kidney function are controversial, high protein intake should be avoided in patients with CKD or risk of CKD [16,17].

Dietary protein intake has increased to above the recommended level in the general population in Korea over the past 20 years [19,20]. According to the Korea National Health and Nutrition Examination Survey (KNHANES) data in 2017 [19], the mean dietary protein intake was 153% of the recommended intake in men and 128% in women among the general population in Korea. The major food sources of protein at that time were cereals (12.7% of total dietary protein intake), pork (11.3%), and chicken (8.3%) [19]. A multicenter, observational, prospective study demonstrated that the mean dietary protein intake was 1.1 g/kg/day in Korean patients with non-dialysis CKD, and dietary protein intake decreased with decreasing eGFR_cr [21]. Another study showed that the mean protein intake was 0.73 g/kg/day in older Koreans, and protein intake was not associated with CKD [22]. In the USA, the average dietary protein intake tends to decrease as CKD progresses [23], and the dietary protein intake in CKD was above the target level for patients with CKD and marginally below the recommended level in the general population [23].

A low-protein diet may preserve kidney function by decreasing kidney capillary hypertension and glomerular hyperfiltration. While experimental evidence suggests that protein restriction can ameliorate glomerular sclerosis, reduce proteinuria, and preserve GFR [24,25], not all clinical studies have shown that low-protein diets provide beneficial effects in patients with CKD. The Modification of Diet in Renal Disease (MDRD) study, the largest controlled trial of dietary protein management in patients with CKD, failed to show a beneficial effect of a low-protein diet. These findings should be interpreted with caution, as the MDRD study had several limitations, including a short follow-up duration and moderately low rate of diet adherence [26]. Nonetheless, most controlled trials and meta-analyses support the beneficial effects of dietary protein restriction [27-31]. A low-protein diet attenuated kidney function decline and delayed the initiation of dialysis in patients with advanced CKD [29,30]. Moreover, dietary protein restriction may improve metabolic dysfunction in CKD. A low-protein diet may improve metabolic acidosis in patients with CKD. Acid is produced by metabolism of proteins. As kidney function declines, there is a tendency toward impairment of acid secretion, which results in chronic metabolic acidosis [11]. Metabolic acidosis impairs protein metabolism, increases muscle catabolism, and aggravates uremic symptoms [32]. A study of supplemented very low-protein diet demonstrated that dietary protein restriction improved metabolic acidosis in patients with advanced CKD [30]. Dietary modification is essential in the management of hyperphosphatemia in patients with CKD, because dietary protein, especially animal protein, is a major source of phosphorus [11]. Dietary protein restriction may be beneficial for control of hyperphosphatemia, which results in better control of CKD-MBD.

A major component of CKD management is inhibition of the renin–angiotensin–aldosterone system (RAAS), which reduces glomerular hyperfiltration and slows the progression of CKD. The combination of RAAS inhibition and dietary protein restriction has been considered to have additive protective effects on kidney disease progression. The additive action of RAAS inhibition and dietary protein restriction can be explained by similar effects in kidney vessels, with a decrease in glomerular pressure and a reduction in kidney fibrosis through inhibition of the transforming growth factor-β pathway [24]. In addition, a low-protein diet could directly inhibit kidney RAAS activation independently of kidney hemodynamics [33]. Many studies on the effects of low-protein diets were conducted before widespread use of RAAS inhibition; thus, there is limited evidence regarding the effects of low-protein diet in combination with RAAS inhibition. Two studies showed that a low-protein diet combined with an angiotensin-converting enzyme (ACE) inhibitor resulted in a further reduction in proteinuria [34,35]. Compared to the group treated with ACE inhibitor alone, protein restriction further reduced proteinuria by 33%. Although, the evidence is insufficient to support the combination of RAAS inhibitors and dietary protein restriction, a low-protein diet is generally recommended in patients with CKD receiving RAAS inhibitors [24].

The major concerns associated with low-protein diets in clinical practice are the risk of PEW and adherence to dietary restrictions [3,11]. Several studies evaluating low-protein diets in patients with CKD have shown acceptable safety with no serious complications, and low rates of PEW and malnutrition. A clinical trial evaluating low-protein diets over 30 months in patients with CKD G4, G5 found that most patients showed acceptable adherence to the prescribed dietary protein restriction, and only 0.7% of participants developed malnutrition [36]. Another study reported that protein restriction in patients with CKD had no effect on body composition or skeletal muscle mass [37]. A diet consisting of 0.6 to 0.8 g/kg/day protein with adequate energy intake (30 to 35 kcal/kg/day) may satisfy dietary needs in patients with CKD, especially if half of the protein is from sources with “high biological value protein” containing the essential amino acids in appropriate ratios and amounts, such as eggs, milk, meat, and fish [3]. While adherence to dietary protein restriction is difficult to predict, good patient–physician communication, education on simplified dietary approaches, and periodic surveillance by a dietitian may improve adherence [11,38].

Although most international guidelines support a low-protein diet in patients with CKD, the protein requirements vary [39,40]. Most guidelines recommend 0.6 to 0.8 g/kg/day protein or very-low-protein diet with keto acid analogs for patients with moderate-to-advanced kidney disease (eGFR_cr < 45 mL/min/1.73 m²) and those with substantial proteinuria (urinary protein excretion > 0.3 g/day) [3]. Higher protein intake (1.0 to 1.2 g/kg/day) is recommended for patients with KF with replacement therapy, as additional protein is needed to prevent PEW [11]. Patients with nephrotic syndrome may benefit from a low-protein diet (0.8 g/kg/day plus 1 g/day protein for each 1 g urinary protein excretion over 5 g/day), while ensuring adequate caloric intake [4]. Furthermore, the target of protein intake should be individualized according to each patient’s clinical condition and disease severity. Modest protein restriction to 0.8 to 1.0 g/kg/day is recommended for patients with nonproteinuric CKD G1, G2, older patients with CKD G3b, and patients with slowly progressing CKD [11]. Several studies have suggested that the protein source may affect the progression of kidney disease [41,42]. Specifically, red meat intake is associated with increased risk of KF, whereas other protein sources, such as poultry, fish, eggs, or dairy products, showed no association with risk of KF [41]. In addition, dairy products were associated with lower risk of the incidence and progression of CKD [43,44]. However, there is insufficient evidence to recommend particular protein types for patients with CKD [40]. For adequate nutrition, we suggest that patients with CKD receive at least half of their protein intake from sources with “high biological value.”

SODIUM

High sodium intake has deleterious effects on blood pressure, cardiovascular health, kidney function, and CKD progression [45]. In patients with CKD, dietary sodium restriction is strongly recommended to control fluid retention, lower blood pressure, and reduce cardiovascular risk [46]. A randomized controlled trial showed that sodium restriction resulted in reduction of blood pressure, extracellular fluid volume, and proteinuria in patients with moderate-to-severe CKD [47]. In addition, sodium restriction enhanced the beneficial effects of a low-protein diet and RAAS inhibition by decreasing intraglomerular pressure, suggesting that sodium restriction may decrease proteinuria and slow the progression of CKD [3]. However, there is inconclusive evidence regarding whether dietary sodium restriction can slow the progression of kidney disease or delay the requirement for kidney replacement therapy. A longitudinal study showed that dietary sodium intake was not associated with progression of kidney disease [48], whereas another study found that sodium excretion was associated with CKD progression and all-cause mortality among 3,939 patients with CKD [49]. The highest quartile of urinary sodium excretion (≥ 4.5 g/day) was associated with a 54% increased risk of CKD progression and a 45% increased risk of mortality compared with the lowest quartile (< 2.7 g/day) [49].

Almost all guidelines recommend lowering sodium intake to 2 to 2.3 g/day in adults [39,40]. Given the risk of hyponatremia and adverse outcomes, dietary sodium intake < 1.5 g/day is not recommended for patients with advanced CKD as well as patients on dialysis [50]. In Korea, the Dietary Reference Intakes for Koreans recommends < 2 g/day sodium, corresponding to approximately 5 g/day salt [20]. In recent years, the dietary sodium intake has decreased among Koreans; however, sodium intake still remains above the recommended level. Among the general population in Korea, the mean sodium intake decreased from 4,586 mg/day in 1,998 to 3,478 mg/day in 2007 [19,20]. According to the KNHANES data for 2017 [19], the mean dietary sodium intake was 212% of the recommended intake in men and 149% in women. The survey found that the major food sources of sodium were seasonings and vegetables, such as kimchi. Patients with CKD should be encouraged to avoid processed foods and to prepare their own meals without salty seasoning. Although urinary sodium excretion from 24-hour urine collection is the gold standard for measuring salt intake, 24-hour urine collection is inconvenient. Urinary sodium excretion rate from spot urine or the sodium frequency food questionnaire could be used to evaluate and monitor dietary salt intake. However, urinary sodium excretion was not useful in monitoring the effects of low-sodium diet in patients with CKD [51]. Therefore, it is necessary to evaluate the dietary salt intake and educate patients based on the situation of each patient.

POTASSIUM

As the main intracellular cation, potassium mediates intracellular electrophysiology and plays an important role in vascular and neuromuscular functions [4]. Serum potassium levels are finely regulated, as low potassium is associated with muscle weakness and hypertension, whereas high potassium can result in ventricular arrhythmia and death [4,52]. Therefore, dietary potassium intake and serum potassium levels are of significant clinical interest. However, few studies have evaluated the effects of dietary modification on serum potassium levels in patients with CKD [3,53].

Several studies have measured urine potassium excretion as a proxy for dietary potassium intake to assess its effect on clinical outcomes [49,54-56]. Nevertheless, limited data are available supporting the idea that dietary potassium restriction improves the outcomes of patients with CKD [57-59], and most recommendations are based on opinions. The 2015 American Dietary Guidelines Advisory Committee report recommends a daily potassium intake of 4,700 mg (121 mmol) for healthy adults [60]. The National Kidney Foundation Kidney Disease Outcomes Quality Initiative guidelines recommend a potassium intake of 2 to 4 g/day (51 to 102 mmol/day) for patients with CKD G3, G4, but no restrictions (> 4 g/day or > 102 mmol/day) for those with earlier-stage CKD [61]. Among the general population in Korea [19], the mean dietary potassium intake was reported to be 88% of the recommended intake in men and 72% in women, with the major food sources of potassium being cereals, vegetables, and pork. In addition to kidney function and dietary intake, several other factors affect serum potassium levels, including the use of RAAS blockers and beta-blockers, hydration status, acid-base status, glycemic control, adrenal function, catabolic state, and gastrointestinal problems, such as diarrhea, constipation, and bleeding. As there has been limited research on the effects of these factors, an individualized approach for each patient is recommended.

Previous observational studies have shown that a plant-based diet is associated with a slower decline in the eGFR_cr among patients with CKD [62,63]. Eating more plant-based foods, such as vegetables and grains, in place of animal-based foods, such as red meat, may help prevent and slow the progression of CKD, type 2 diabetes, high blood pressure, and heart disease [62,63]. Eating less animal-based foods can lower the acid load and put less stress on the kidneys [62,63]. In addition, plant-based foods that are not highly processed contain phytates. Phytates can bind phosphate, and so we can expect much less phosphate to be absorbed through plant-based foods than highly processed foods. However, a potassium-rich diet, such as a plant-based diet, may be of limited benefit in controlling serum potassium and phosphate levels in patients with kidney dysfunction. Therefore, individualized approaches with regard to dietary potassium intake in patients with CKD should target a normal- to high-potassium diet. In theory, potassium binders may be used to provide a liberalized potassium diet diet that includes fruits and vegetables if there is concern regarding hyperkalemia in patients with CKD. However, there have been no investigations as to whether potassium intake should be modified when taking potassium binders. Most recent guidelines recommend adjusting dietary potassium intake on an individual basis to maintain normal serum potassium levels in patients with CKD [40].

PHOSPHORUS

Phosphorus is an essential nutrient for maintaining homeostasis and is found in most natural and processed foods. Phosphorus intake is necessary for bone growth and mineralization, as well as for regulation of energy and acid–base homeostasis [4]. Patients with CKD typically maintain normal serum phosphorus levels during the early stages (eGFR_cr > 45 mL/min/1.73 m²) by promoting phosphorus excretion with increased fibroblast growth factor 23 (FGF-23) and parathyroid hormone (PTH) levels. However, as CKD progresses, elevated serum phosphate levels or hyperphosphatemia may occur due to resistance to FGF-23 and PTH [64].

Elevated serum phosphorus levels have been associated with increased cardiovascular risk in patients with CKD and in the general population [65,66]. A recent study described the mechanism associated with increased cardiovascular risk in hyperphosphatemia, which can cause left ventricular hypertrophy and arterial stiffness via induction of FGF-23 and vascular calcification [67,68]. However, the dietary phosphate intake, measured by 24-hour urine phosphate excretion, had no effect on the development of KF or cardiovascular mortality when the serum phosphorus concentration remained within the normal range [69].

Traditional guidelines suggest maintaining a phosphorus intake of 800 to 1,000 mg/day in patients with CKD G3–5 and KF on dialysis to keep the serum phosphate level within the normal range [70-72]. Among the general population in Korea [19], the mean dietary phosphorus intake was reported to be 170% of the recommended intake in men and 123% in women, with the major food sources of phosphorus being cereal, pork, milk, and egg. It is not clear how to limit dietary phosphorus in adult patients with CKD. In addition, the amount and bioavailability of phosphorus are influenced by the type of dietary protein, which is the primary source of phosphorus. Guidelines that recommend limiting dietary phosphorus intake often mention concerns about the risk of limiting protein intake in patients with CKD, especially those on maintenance dialysis therapy [73]. Therefore, dietary consultations should include information about protein sources that contain phosphorus and suggestions for cooking phosphate-rich foods that can achieve low phosphorus intake without compromising dietary quality [74]. In addition, patient education on hyperphosphatemia management, including adoption of a low-phosphate diet and on the appropriate use of phosphate binders, may improve phosphate control [75,76]. Nutritional management may incorporate additional plant-based sources of phosphorus, as the gastrointestinal absorption of plant-based phosphorus (20% to 50%) is lower than that from animal-based foods (40% to 60%) [77]. Moreover, phosphorus-containing food additives in processed and fast foods are of particular concern as they contain inorganic phosphorus, which shows nearly 100% intestinal absorption [74,77].

Recent guidelines emphasize individualized recommendations following the evaluation of dietary phosphorus intake to maintain serum phosphorus within the normal range in patients with CKD [40]. Restricting the intake of animal-based dietary phosphates and replacement with plant-derived dietary phosphate may be considered to reduce the pill burden of phosphate binders in patients with advanced CKD.

CALCIUM AND VITAMIN D

Calcium is an electrolyte and multivalent cation that is essential for many bodily functions. It is necessary for the functioning of muscles as well as the circulatory and digestive system, and is essential for bone formation and blood cell synthesis [4]. Calcium balance is strictly regulated by calcium absorption in the intestine, reabsorption in the kidney, and exchange in the bones. Given the important role of the kidneys in calcium balance, the serum calcium level decreases as CKD progresses [78]. Calcium level reduction can cause secondary hyperparathyroidism, which leads to MBDs, whereas extraosseous calcification resulting from excess calcium can lead to cardiovascular disease and increased mortality [79]. Maintaining a balanced serum calcium level in patients with CKD requires consideration of several factors, including kidney function, mineral-controlling hormones, bone turnover, use of vitamin D analogs, and calcium intake from supplements. For patients requiring maintenance dialysis, additional factors must be taken into consideration, including the mode of dialysis as well as the calcium concentration in the dialysate. Therefore, ensuring adequate dietary calcium is challenging and depends on unique factors affecting each patient’s calcium balance.

In 2017, Kidney Disease: Improving Global Outcomes (KDIGO) updated its CKD-MBD clinical practice guidelines to suggest restricting the dose of calcium-containing phosphate binders regardless of serum calcium level [71]. This recommendation was based on evidence from three open-label randomized controlled trials showing improved survival among dialysis patients treated with the phosphate-binding drug, sevelamer, versus calcium-containing binders [80-82]. However, other researchers raised concerns regarding small sample size, inconsistent findings, and loss to follow-up resulting in risks of bias in this study. Spoendlin et al. [83] reported an observational study suggesting that there is no cardiovascular or survival benefit of sevelamer compared to calcium acetate among incident dialysis patients 65 years or older. These conflicting results should be examined in future clinical trials and reflected in the guidelines.

The recommended daily intake of dietary calcium is 800 to 1,000 mg/day to maintain appropriate calcium levels in patients with CKD G3, G4 who are not receiving active vitamin D analogs [84]. These recommendations are consistent with the current estimated average requirement (800 to 1,000 mg/day) and recommended dietary allowance (1,000 to 1,200 mg/day) for healthy individuals according to the National Academy of Medicine in the USA [85]. Among the general population in Korea [19], the mean dietary calcium intake was reported to be 72% of the recommended intake in men and 63% in women, with the major food sources of calcium being milk, vegetables, and anchovies.

In addition to dietary intake, vitamin D is also affected by the degree of sunlight exposure and seasonal changes, making it difficult to establish dietary standards [4]. The prevalence of vitamin D deficiency (20 to 30 ng/mL) and insufficiency (< 20 ng/mL), assessed by the serum concentration of calcidiol (25-hydroxyvitamin D [25(OH) D]), is higher in patients with advanced CKD compared with healthy individuals in Korea [86]. Recognizing the increased risk of vitamin D deficiency among patients with CKD, recent guidelines recommend supplementation for vitamin D deficiency in patients with CKD, but not CKD-MBD or other clinically relevant outcomes [40,71,72]. No guidelines specify a safe dose of vitamin D supplementation for preventing side effects in patients with CKD. Therefore, vitamin D supplement regimens should be individualized, and serum calcium, phosphorus and 25(OH)D levels should be measured periodically, especially in patients taking calcium-containing phosphate binders and/or active vitamin D analogs.

CONCLUSIONS

This review was based on the best information currently available. When clinicians consider the needs of an individual patient, the resources available, and the limitations inherent to the institution or type of care, variations in practice are inevitable. Based on the articles reviewed (Table 1) [17,18,26,30,48,49,56,69,73,84,87,88], individualized strategies are recommended according to each patient’s nutritional status, clinical comorbidities, and disease severity (Table 2). Individualized approaches with periodic counseling may help to attenuate the progression of CKD and decrease mortality. Moreover, detailed nutritional care also improves quality of life. Further research to evaluate the effects of nutritional interventions on clinical outcomes in patients with CKD will yield concrete recommendations.

Conflict of Interest

No potential conflict of interest relevant to this article was reported.

Table 1.

Recent clinical studies on nutritional content for patients with CKD

Dietary constituent	Study	Sample size	Diet (variables)	Baseline eGFR_cr, mL/min/1.73 m²	Findings
Protein	Knight et al. [17]	1,624	Protein intake	Normal: > 80	A high protein diet was not associated with eGFR_cr decline in normal kidney function. However, it was associated with accelerated eGFR_cr decline in mild CKD.
	Knight et al. [17]	1,624	(divided into quintiles)	Mild CKD: 55–80
	Jhee et al. [18]	9,226	Protein intake (divided into quartiles)	Mean 93.9 ± 14.1	A high protein diet increased the risk of kidney hyperfiltration and a rapid decline of kidney function.
	Klahr et al. [26] MDRD study 1	585	Usual protein diet (1.3 g/kg/day) vs. low protein diet (0.6 g/kg/day)	25–55 (mean 38.6)	Mean eGFR_cr decline at 3 years did not differ between the diet group.
	Klahr et al. [26] MDRD study 2	255	Low protein diet (0.6 g/kg/day) vs. supplemented very low protein diet (0.3 g/kg/day with ketoacid)	13–24 (mean 18.5)	Supplemented very low protein diet marginally slower eGFR_cr decline.
	Garneata et al. [30]	207	Low protein diet (0.6 g/kg/day) vs. supplemented very low protein diet (0.3 g/kg/day with ketoacid)	< 30 (mean 18.0)	Supplemented very low protein diet decreased the risk of progression of CKD.
Sodium	Smyth et al. [48]	28,879	Urinary sodium	Mean 68.4 ± 17.6	Urinary sodium excretion was not associated with increased risk of CKD progression.
Sodium	He et al. [49]	3,939	Urinary sodium	41.5–48.5	Higher urinary sodium excretion was associated with increased risk of CKD progression.
Potassium	He et al. [49]	3,757	Urinary potassium	41.5–48.5	Higher urinary potassium excretion was associated with increased risk of CKD progression.
Potassium	Leonberg-Yoo et al. [56]	812	Urinary potassium	32.6	Higher urine potassium excretion was associated with lower risk for all-cause mortality, but not kidney failure.
Phosphorus	Selamet et al. [69]	795	Urinary phosphate	33	Higher urinary phosphate excretion is not associated with the risk of KF and mortality.
Phosphorus	Lynch et al. [73]	1,751	Prescribed dietary phosphate	Hemodialysis	Prescribed dietary phosphate restriction is not associated with improved survival among prevalent hemodialysis patients.
Calcium	Spiegel et al. [84]	12	Dietary calcium	54.8	Total elemental calcium intake should be within 800–1,200 mg/day to prevent calcium deficiency and calcium loading.
Vitamin D	Bhan et al. [87]	105	Ergocalciferol	Hemodialysis	Oral ergocalciferol can increase 25(OH)D levels without significant alterations in blood calcium, phosphate, or parathyroid hormone.
Vitamin D	Kumar et al. [88]	120	Cholecalciferol	34.6–35.8	Correction of vitamin D deficiency by cholecalciferol supplementation show positive effects on vascular function in nondiabetic early CKD patients.

CKD, chronic kidney disease; eGFR_cr, estimated glomerular filtration rate based on serum creatinine; MDRD, Modification of Diet in Renal Disease; KF, kidney failure; 25(OH)D, 25-hydroxyvitamin D.

Table 2.

Nutritional recommendations for patients with CKD

Dietary constituent	Nutritional recommendations
Protein	For patients with CKD G3b, G4, G5 or patients with proteinuria (urinary protein excretion > 0.3 g/day), a protein intake of 0.6–0.8 g/kg/day is recommended.
	For patients on dialysis, 1.0–1.2 g/kg/day is recommended.
	For patients with nephrotic syndrome, 0.8 g/kg/day + 1 g/day protein for each 1 g urinary protein excretion over 5 g/day is recommended.
	For patients with nonproteinuric CKD G1, G2, older patients with CKD G3b, and patients with slowly progressing CKD, 0.8–1.0 g/kg/day is recommended.
Sodium	Less than 2 g/day sodium (approximately 5 g salt) is recommended.
Potassium	Individualized regimens to maintain serum potassium levels within the normal range is recommended.
	In patients with CKD who exhibit hyperkalemia, consider lowering dietary potassium intake to maintain serum potassium levels within the normal range.
Phosphorus	In patients with CKD G3–5 and KF with replacement therapy, 0.8–1 g/day or individualized regimens are recommended to maintain serum phosphate within the normal range.
	In patients with CKD who exhibit hyperphosphatemia, consider lowering dietary phosphorus intake to maintain serum phosphate levels within the normal range.
	Increase vegetable-based phosphors intake and avoid processed foods as much as possible.
Calcium	In patients with CKD G3, G4 not taking active vitamin D analogs, 800–1,000 mg/day of elemental calcium may be prescribed to maintain normal calcium levels.
Calcium	In patients with KF with replacement therapy, adjust calcium intake (i.e., dietary calcium, calcium supplements or calcium-based binders) depending on concurrent use of vitamin D analogs and calcimimetics in order to avoid hypercalcemia.
Vitamin D	In patients with CKD who exhibit 25(OH)D deficiency, vitamin D supplementation in the form of cholecalciferol or ergocalciferol may be considered only for deficiency/insufficiency, but not for CKDMBD or other clinically relevant outcomes.
Vitamin D	Vitamin D supplementation regimens should be determined based on individualized strategies, and serum calcium, phosphorus and 25(OH)D levels should be measured periodically, especially in patients taking calcium-containing phosphate binders and/or active vitamin D analogs.

Recommended dietary intake based on current guidelines and recommendations [3,4,39,40,71].

CKD, chronic kidney disease; KF, kidney failure; 25(OH)D, 25-hydroxyvitamin D; MBD, mineral and bone disorder.

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