Chronic Kidney Disease (CKD) is a major global public health burden, affecting more than 10% of the general population. The global prevalence estimates indicate that approximately 13.4% (11.7–15.1%) of people are living with CKD, and between 4.9 and 7.1 million individuals with end-stage kidney disease (ESKD) require renal replacement therapy. CKD is a progressive condition marked by a sustained and usually irreversible decline in renal function.
The diagnosis of CKD is primarily based on objective laboratory results, which includes the estimation of glomerular filtration rate (eGFR) using validated equations incorporating filtration biomarkers such as serum creatinine or cystatin C, as well as the assessment of urinary markers of kidney damage, particularly albuminuria. CKD can be formally defined by a persistent reduction eGFR to <60 mL/min/1.73 m² for a duration of at least three months, irrespective of the presence of kidney damage, albuminuria or haematuria.
Risk Factors
CKD arises from a combination of modifiable and non-modifiable factors.
Modifiable risk factors:
- Diabetes: Diabetes is the leading cause of CKD and high blood glucose levels impairs kidney filtration and accelerates diabetic nephropathy. It is a very common underlying cause of CKD progression to end-stage kidney disease, which requires dialysis or kidney transplantation.
- Hypertension: Uncontrolled hypertension is a major contributor to CKD progression, and sustained elevations in blood pressure may damage the blood vessels in the kidney and increase the overall risk of kidney damage.
- Cardiovascular Disease (CVD): CVD can impair kidney function by reducing blood flow to the kidney and it is also a common consequence of CKD.
- Obesity: Overweight and obesity increase the risk of CKD by contributing to hypertension, diabetes and dyslipidemia. Obesity also increases mortality for people who already have CKD.
- Smoking: Smoking contributes to CKD progression by increasing blood pressure, reducing oxygen and damaging the blood vessels.
Non-modifiable risk factors:
- Ageing: The risk of CKD increases markedly in individuals over 60 years of age, attributable to the age-related decline in renal function.
- Genetic predisposition: Family history of CKD and a personal history of CKD, particularly hereditary disorders such as Polycystic Kidney Disease (PKD), are associated with an increased risk of CKD. The severe, recurrent or poorly recovered Acute Kidney Injury (AKI) also increases the risk of progression to CKD particularly among older adults with comorbidities.
- Aboriginal and Torres Strait Islander ≥18 years: Aboriginal and Torres Strait Islander populations experience a higher prevalence of CKD, with earlier onset and more rapid disease progression.
- Low birth weight or premature birth: low birth weight or premature birth may be linked to a reduced nephron number, thereby increasing the lifelong risk of hypertension and CKD.
Pathophysiology
CKD is defined by a gradual and irreversible loss of nephrons, resulting in a gradual decline in renal function. Initial injury to nephrons may damage the glomeruli or tubules and it reduces the number of functional nephrons. Glomerular injury facilitates albuminuria, which triggers tubular inflammation and promotes interstitial fibrosis and cellular injury. Sustained inflammation further reduces microvascular supply, leading to chronic hypoxia and accelerates nephron loss, thereby worsening the renal function over the time.
The progressive decline in kidney function disrupts systemic homeostasis, leading to azotaemia, electrolyte and acid-base imbalances, anemia due to decreased erythropoietin production, mineral and bone disorders, fluid overload, hypertension and multiple other complications, reflecting the multisystem impact of CKD.
Classification
Clinical Practice Guidelines published by Kidney Disease: Improving Global Outcomes (KDIGO) categorise CKD into five stages based on eGFR (G1-G5) or albuminuria (A1-A3) (Table 1 & 2). Guideline suggests that both decreased eGFR and increased levels of albuminuria are independently related to mortality, cardiovascular complications and end-stage kidney disease.
Table 1. GFR categories in Chronic Kidney Disease
| Category | GFR (ml/min/1.73 m²) | Terms |
| G1 | ≥ 90 | Normal or high |
| G2 | 60–89 | Mildly decreased |
| G3a | 45–59 | Mildly to moderately decreased |
| G3b | 30–44 | Moderately to severely decreased |
| G4 | 15–29 | Severely decreased |
| G5 | < 15 | Kidney failure |
Table 2. Albuminuria categories in Chronic Kidney Disease
| Category | Albumin Excretion Rate (mg/24 h) | Albumin-to-Creatinine Ratio (mg/mmol) | Terms |
| A1 | < 30 | < 3 | Normal to mildly increased |
| A2 | 30–300 | 3–30 | Moderately increased |
| A3 | > 300 | > 30 | Severely increased |
Clinical Presentation
CKD is typically asymptomatic until over 90% of kidney function has declined. Early signs may include albuminuria, nocturia and polyuria. As renal impairment progresses, patients may develop uraemic symptoms such as fatigue, nausea, pruritus and cognitive changes.
Advanced disease results in systemic manifestations including:
- CVD (heart failure, left ventricular hypertrophy, hypertension)
- Metabolic acidosis
- Bone and mineral disorders
- Anaemia due to reduced erythropoietin
- Hyperkalaemia and fluid overload
- Reduced drug clearance leading to toxicity risks
These systemic complications contribute to impaired quality of life and increased hospitalisation.
Management Principles
CKD is generally irreversible, but timely and effective management can slow its progression, reduce the risk of CVD and manage complications. Individuals with advanced chronic kidney disease experience a significant polypharmacy burden (average of 12 medications per day). Approximately 70–80% of patients are prescribed five or more medications and which increases the risk of polypharmacy-related adverse effects. With early detection and appropriate management, the progression of CKD may be reduced by up to 50%. Patients with CKD should be referred to nephrologists no later than the point at which the eGFR reaches 30 mL/min. (Coritisidis GN et al., 2011)
Pharmacological Management
| Drug class | Role in CKD | Key considerations |
| ACEi/ARBs | First-line for reducing proteinuria and BP | Titrate to highest tolerated dose |
| SGLT2 inhibitors | – Recommended with or without diabetes.
– Slow progression and improve CVD outcomes |
– Avoid initiation at eGFR <25 mL/min/1.73m²
– Dapagliflozin can be used until 15 mL/min/1.73m² |
| Non-steroidal MRAs (finerenone) | Persistent albuminuria in T2DM despite ACEi/ARB | Avoid if potassium >5.0 mmol/L or eGFR <25 mL/min/1.73m² |
| GLP-1 receptor agonists | Improve glycaemia and reduce CVD risk | TGA-approved for reducing kidney decline in T2DM and CKD |
| Statins ± ezetimibe | CVD risk reduction | Recommended in most adults with CKD not on dialysis |
Abbreviations: Angiotensin-converting enzyme inhibitors (ACEi) and angiotensin receptor blockers (ARBs) blood pressure (BP); Sodium-glucose co-transporter 2 inhibitors (SGLT2i); Mineralocorticoid receptor antagonists (MRA); Glucagon-like peptide-1 (GLP-1)
The STOP-ACEi trial of 411 participants with chronic kidney disease, investigated that discontinuing renin-angiotensin system inhibitors (RASi), including ACEi and ARBs did not result in clinical benefit in patients with advanced and progressive CKD. (Bhandari et al., 2024)
Non-Pharmacological Care
Lifestyle modification remains a cornerstone of CKD management, as it improves the clinical outcomes and slows the rate of disease progression. Important lifestyle strategies include smoking cessation, adequate physical activity, healthy diet and limiting alcohol intake.
Smoking cessation is strongly recommended, as tobacco use accelerates renal decline through vascular injury, oxidative stress and promoting systemic inflammation. Nutritional intervention should be individualised and adjusted according to the metabolic changes associated with each stage of CKD. In earlier stages, a general healthy balanced diet is recommended, including balanced nutrition, sodium intake reduction, and limiting highly processed foods. In later stages, dietitian involvement is essential, as patients may need to restrict foods high in potassium and phosphate to prevent complications such as hyperkalaemia and bone disease. Alcohol consumption should be no more than 10 standard drinks per week and no more than 4 drinks on a single day. Regular physical activity is also strongly encouraged. The goal is to achieve 2.5–5 hours of moderate to intensity aerobic exercise each week, along with strength training to maintain muscle mass and physical function.
Conclusion
CKD represents a major public health challenge in Australia, affecting a substantial proportion of the population and contributing markedly to morbidity and mortality. According to the Australian Institute of Health and Welfare (AIHW), CKD contributed to approximately 11% of all deaths in 2022, emphasising its significant burden on national health outcomes.
CKD imposes a significant economic burden, particularly in advanced stages requiring dialysis or transplantation. It is also associated with high rates of hospitalisation and healthcare services. Cardiovascular complications are the predominant drivers of both morbidity and mortality among CKD patients, highlighting the need for integrated care strategies that address both renal and cardiovascular health. With early recognition and appropriate treatment, progression to kidney failure can often be significantly delayed and improve the quality of life and reducing healthcare burden.
