Advanced Clinical Nursing

Chronic Kidney Disease (CKD)
Advanced Nursing Guide

Comprehensive GCC-focused guide covering KDIGO staging, dialysis, transplant, complications management, and exam preparation for DHA, DOH & SCFHS.

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KDIGO CKD Definition

KDIGO 2012 Definition

CKD is defined as abnormalities of kidney structure or function, present for >3 months, with implications for health. Requires either: kidney damage markers (albuminuria ≥30 mg/g, haematuria, structural abnormality, biopsy findings, transplant history) OR GFR <60 mL/min/1.73m².

CGA Staging System

CKD is staged using three parameters: Cause + GFR category + Albuminuria category. All three must be documented for complete staging.

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GFR Staging (G1–G5)

StageGFR (mL/min/1.73m²)DescriptionMonitoring
G1≥90Normal/high — only CKD if damage markers presentAnnual, treat underlying cause
G260–89Mildly decreased — only CKD if damage markers presentAnnual, optimise CVD risk
G3a45–59Mildly to moderately decreasedEvery 6 months
G3b30–44Moderately to severely decreasedEvery 3–6 months
G415–29Severely decreased — prepare for RRTEvery 3 months, refer nephrology
G5<15Kidney failure — RRT or conservative pathwayMonthly, or per dialysis schedule
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Albuminuria Categories (A1–A3)

CategoryACR (mg/g)ACR (mg/mmol)Description
A1<30<3Normal to mildly increased
A230–3003–30Moderately increased (microalbuminuria)
A3>300>30Severely increased (macroalbuminuria/proteinuria)
Clinical Significance

A3 albuminuria independently predicts CKD progression, cardiovascular events, and mortality. First morning spot urine ACR is preferred over 24-hour urine collection.

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KDIGO Risk Heat Map

Combined GFR and Albuminuria prognosis for CKD progression and mortality:

A1
<30 mg/g
A2
30–300 mg/g
A3
>300 mg/g
G1 (≥90)
Low
Moderate
High
G2 (60–89)
Low
Moderate
High
G3a (45–59)
Moderate
High
Very High
G3b (30–44)
High
Very High
Very High
G4 (15–29)
Very High
Very High
Very High
G5 (<15)
Very High
Very High
Very High
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Main Causes of CKD

  • Diabetic nephropathy: 40–50% of CKD — leading cause in GCC due to T2DM epidemic
  • Hypertensive nephrosclerosis: 25–30%; uncontrolled BP causes glomerulosclerosis
  • Glomerulonephritis: IgA nephropathy commonest in adults worldwide; FSGS, membranous
  • Polycystic kidney disease (PKD): ADPKD most common inherited kidney disease
  • Obstructive uropathy: BPH, renal calculi, retroperitoneal fibrosis
  • Lupus nephritis: class III/IV require aggressive immunosuppression
  • Renovascular disease: renal artery stenosis — atherosclerosis or FMD
GCC Context

Saudi Arabia, UAE and Kuwait have among the world's highest diabetes prevalence (20–25%). This directly translates to very high CKD and ESRD rates in the region.

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Pathophysiology of CKD Progression

Key Mechanisms
  • Glomerular hyperfiltration: initial compensation by remaining nephrons → intraglomerular hypertension
  • Proteinuria: protein leak activates tubular inflammation and fibrosis signalling (TGF-β pathway)
  • Tubulointerstitial fibrosis: progressive scarring replaces functional nephron mass
  • RAAS activation: angiotensin II drives hypertension, inflammation, fibrosis
  • Endothelial dysfunction: accelerates cardiovascular risk and glomerular damage
  • Nephron loss: progressive decline in GFR → uraemic syndrome
Acute-on-Chronic Risk
  • Dehydration — commonest acute insult in GCC climate
  • NSAIDs, contrast nephropathy, aminoglycosides
  • Urinary tract obstruction
  • Intercurrent infection / sepsis
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Anaemia of CKD

Pathophysiology
  • EPO deficiency: reduced production by peritubular fibroblasts as GFR declines
  • Iron deficiency: absolute (poor intake/blood loss) or functional (hepcidin-mediated)
  • Shortened RBC survival: uraemic toxin-mediated haemolysis
  • Marrow suppression: uraemic inhibitors impair erythropoiesis
Targets & Thresholds
  • Start EPO work-up when Hb <100 g/L (KDIGO)
  • Target Hb: 100–120 g/L (avoid >130 — increased thrombosis/CVD risk)
  • Iron: ferritin >200 µg/L + TSAT >20% before starting ESA
  • Dialysis patients: ferritin target 200–500 µg/L
Treatment
  • IV iron: preferred in dialysis (ferric carboxymaltose, iron sucrose, ferric derisomaltose)
  • ESA: darbepoetin alfa (weekly/fortnightly SC) or epoetin alfa/beta (3×/week SC)
  • HIF-PHI: roxadustat — newer oral agent stimulates EPO production
  • Blood transfusion: avoid if possible (sensitisation risk pre-transplant)
ESA Hypertension Risk

Monitor BP closely when initiating ESA — can worsen hypertension. Reduce ESA dose or add antihypertensive. Avoid rapid Hb rise (>20 g/L over 4 weeks).

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Renal Bone Disease (CKD-MBD)

Pathophysiology Sequence
  • Reduced GFR → phosphate retention → hyperphosphataemia
  • Reduced 1,25(OH)₂D (active Vit D) production by kidney
  • Low calcium + high phosphate → PTH ↑ (secondary hyperparathyroidism)
  • PTH mobilises Ca²⁺ from bone → renal osteodystrophy
  • Vascular calcification from Ca×P product elevation
Laboratory Monitoring
  • Phosphate: target 0.8–1.5 mmol/L
  • Calcium: target normal range (2.1–2.5 mmol/L)
  • PTH: target 2–9× upper limit normal in G5D
  • 25-OH Vitamin D: maintain >50 nmol/L
Management
  • Dietary phosphate restriction: avoid processed foods, cola drinks, fast food
  • Phosphate binders (take with meals):
    — Calcium carbonate (avoid if hypercalcaemia)
    — Sevelamer hydrochloride (non-calcium, preferred)
    — Lanthanum carbonate (chew with meals)
  • Active Vitamin D: alfacalcidol or calcitriol — monitor Ca to avoid hypercalcaemia
  • Cinacalcet (calcimimetic): lowers PTH by sensitising CaSR — causes hypocalcaemia, nausea
  • Parathyroidectomy: for refractory secondary/tertiary HPT

Hyperkalaemia Management

EMERGENCY: Hyperkalaemia (K⁺ >6.5 mmol/L or ECG changes)
  • Calcium gluconate 10% 10 mL IV: membrane stabilisation — acts in minutes (NOT corrects K⁺)
  • Insulin 10 units + 50% Dextrose 50 mL IV: shifts K⁺ into cells (onset 20 min)
  • Salbutamol 10–20 mg nebuliser: β₂ agonist shifts K⁺ intracellularly
  • Sodium bicarbonate: if severe acidosis — some K⁺ shift
  • Dialysis: definitive treatment for refractory hyperkalaemia
Dietary Restriction (High-K⁺ Foods to Avoid)
  • Bananas, oranges, dates, dried fruits, avocado
  • Potatoes (leach by peeling, dicing, boiling in large water)
  • Tomatoes, tomato paste, tomato juice
  • Nuts, chocolate, legumes, bran cereals
  • Salt substitutes (contain KCl)
Chronic Management
  • Patiromer (Veltassa): K⁺ binder in colon — take 6 hours from other medications
  • Sodium zirconium cyclosilicate (Lokelma): rapid onset K⁺ binder
  • Resonium A (sodium polystyrene sulphonate): older agent, less preferred
  • Review nephrotoxic medications (ACE-I/ARB doses, K⁺-sparing diuretics)
  • Treat constipation (↓ faecal K⁺ excretion)
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Fluid Management & Oedema

  • Sodium restriction: <2g/day (5g salt) — most important intervention
  • Fluid restriction: based on urine output + 500 mL/day insensible losses
  • Furosemide: higher doses needed in CKD (up to 500 mg/day); loses efficacy in ESRD
  • Metolazone: add to furosemide for synergistic diuresis (monitor K⁺, Na⁺)
  • Daily weight monitoring — report >2 kg gain in 24–48 hours
  • Oedema grading: document site, severity, pitting (1+ to 4+)
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Cardiovascular Risk & Metabolic Acidosis

CVD Risk in CKD
  • CKD patients have 5–10× higher CVD risk than general population
  • BP target: <130/80 mmHg (KDIGO 2021)
  • ACE inhibitor/ARB: first-line — reduce proteinuria and slow CKD progression; monitor K⁺/creatinine at 1–2 weeks post initiation
  • SGLT2 inhibitors: dapagliflozin/empagliflozin — additional CV and kidney protection
  • Statin therapy: recommended in CKD G1–G5 (not initiated on dialysis per SHARP trial)
  • Antiplatelet: aspirin in established CVD
Metabolic Acidosis
  • Target bicarbonate: ≥22 mmol/L
  • Sodium bicarbonate supplementation: 500 mg–1 g TDS orally
  • Acidosis accelerates muscle wasting, bone disease, and CKD progression
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Haemodialysis (HD)

HD Prescription
  • Schedule: 3× per week, 4 hours per session (minimum)
  • Adequacy: Kt/V target >1.2 per session (spKt/V)
  • URR (urea reduction ratio) target: >65%
  • Blood flow rate: 250–400 mL/min
  • Dialysate flow: 500–800 mL/min
  • Ultrafiltration rate: based on interdialytic weight gain (max 10–13 mL/kg/hr)
HD Session Nursing Procedure
  • Machine setup: priming circuit (500 mL NS), check membranes, dialysate conductivity/temperature
  • Pre-HD: weigh patient, check BP/HR, inspect access
  • Connect patient: sterile technique, 2-needle cannulation (arterial + venous)
  • Set UF rate to remove interdialytic weight gain
  • Monitoring during session: BP every 30 min, HR, UF progress, alarms
  • Heparin anticoagulation (loading dose + maintenance) or citrate lock
  • Post-HD: disconnect, pressure haemostasis, weigh, BP, document
Vascular Access Hierarchy
  • 1st: AV Fistula (AVF) — radio-cephalic or brachio-cephalic; 6+ weeks maturation; gold standard
  • 2nd: AV Graft (AVG) — synthetic (PTFE); earlier needling; higher infection/thrombosis risk
  • 3rd: Tunnelled Cuffed Catheter (TCC) — internal jugular preferred; highest infection/recirculation risk
  • Temporary catheter (non-tunnelled): emergency only
AVF Assessment
  • Thrill: palpate over anastomosis — continuous vibration (normal)
  • Bruit: auscultate — low-pitched, continuous (normal)
  • Loss of thrill/bruit = EMERGENCY — thrombosis or stenosis → urgent referral
  • No BP cuff, venepuncture, or IV access on fistula arm
  • Avoid tight clothing/watch on fistula arm
  • Elevate arm for swelling; gentle exercises to mature fistula
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HD Complications & Troubleshooting

Intradialytic Hypotension (IDH) — Most Common
  • Definition: SBP drop >20 mmHg or symptomatic
  • Causes: over-ultrafiltration, autonomic neuropathy, low albumin
  • Action: reduce UF to 0, Trendelenburg position, 100–200 mL NS bolus, reduce blood flow temporarily
Air Embolism
  • Signs: chest pain, dyspnoea, cough, neurological changes
  • Action: CLAMP venous line immediately, left lateral decubitus + Trendelenburg (air to apex RV), 100% O₂, urgent medical review
Access Recirculation
  • Treated blood re-enters dialyser — reduces efficiency
  • Causes: reversed needle positions, stenosis, inadequate flow
  • Check by urea recirculation test or access surveillance
Muscle Cramps
  • Due to rapid fluid removal and Na⁺ shifts
  • Action: reduce UF, saline bolus 100 mL, stretch
  • Prevention: avoid excessive interdialytic weight gain
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Peritoneal Dialysis (PD)

PD Modalities
  • CAPD (Continuous Ambulatory PD): 4 manual exchanges/day, ~2 L/dwell, dwell time 4–6 hours (night dwell 8–10 h); no machine needed
  • APD (Automated PD): overnight cycler machine (8–10 hrs), 5–8 rapid exchanges; daytime freedom; better for working patients
  • High-transport membrane: better with APD (short dwells); low-transport: better with CAPD (long dwells)
PD Advantages vs HD
  • Home therapy — independence, better QoL
  • Better preservation of residual renal function
  • Haemodynamic stability — no rapid fluid shifts
  • Dietary freedom — less restriction needed
  • Higher protein requirements: ~1.2 g/kg/day (protein losses in dialysate)
PD Catheter & Exit Site Care
  • Tenckhoff catheter — inserted surgically or laparoscopically, 2-week healing before use
  • Daily exit site cleaning with saline or chlorhexidine
  • No occlusive dressings; keep dry during shower (waterproof cover)
  • Topical mupirocin or gentamicin if S. aureus carrier
  • Inspect for: redness, swelling, crust, discharge, tunnel tenderness
PD Peritonitis — EMERGENCY
  • Signs: cloudy effluent, abdominal pain, fever, nausea
  • Action: drain effluent, send for MC&S (cell count, culture), start IP antibiotics empirically (vancomycin + aminoglycoside or ceftazidime)
  • Commonest organisms: Gram-positive cocci (S. epidermidis)
  • Catheter removal if: fungal peritonitis, refractory >5 days, tunnel infection
  • Encapsulating peritoneal sclerosis (EPS): rare but life-threatening long-term complication — abdominal cocoon
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Pre-dialysis Planning & Low-Clearance Clinic

Low-Clearance Clinic Referral
  • Initiate when eGFR 10–15 mL/min/1.73m² (G4–G5 transition)
  • Multidisciplinary: nephrologist, nurse specialist, dietitian, social worker
  • Topics: modality education (HD/PD/transplant/conservative), access planning, symptom management
Vascular Access Planning
  • Refer to vascular surgeon when eGFR <20–25 to plan AVF creation
  • AVF requires ≥6 months to mature before dialysis use
  • Preserve forearm veins: avoid cannulation, phlebotomy in non-dominant arm
  • Document vein mapping (duplex USS)
Dialysis Initiation Criteria
  • Uraemic symptoms: nausea, pericarditis, encephalopathy
  • Refractory fluid overload/hypertension
  • Hyperkalaemia refractory to medical management
  • Metabolic acidosis refractory to treatment
  • eGFR <6–8 mL/min (even if asymptomatic)
Conservative Management Pathway
  • Suitable for: elderly, frail, multiple comorbidities where dialysis may not improve QoL/survival
  • Focus: symptom control (oedema, pruritus, nausea, pain, restless legs), advance care planning, DNAR discussions
  • Median survival on conservative pathway in elderly: 6–24 months
  • Community palliative care and hospice liaison
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Kidney Transplantation

Recipient Assessment (Work-Up)
  • ABO blood group and HLA typing
  • Panel Reactive Antibody (PRA): measures sensitisation — high PRA (>80%) = difficult to find compatible donor
  • Donor Specific Antibodies (DSA): HLA antibodies against specific donor — contraindication or desensitisation protocol
  • Cardiac assessment: stress echo/angiography (high CVD risk)
  • Exclude active infection, malignancy, non-compliance
  • Ideally listed before starting dialysis (pre-emptive transplant)
Live vs Deceased Donor
  • Living donor: better outcomes, shorter waiting time, elective surgery
  • Deceased donor: DBD (donation after brain death) or DCD (donation after circulatory death)
  • HLA matching: better match → less rejection risk
Immunosuppression (Triple Therapy)
  • Tacrolimus (Tac): CNI — target levels (trough) 8–12 ng/mL early, 5–8 long-term; nephrotoxic at high levels; monitor drug levels, glucose (diabetogenic)
  • Mycophenolate mofetil (MMF): antimetabolite — causes GI side effects, bone marrow suppression; teratogenic
  • Prednisolone: taper from 20 mg to 5 mg over months; cushingoid, hypertension, hyperglycaemia
  • Induction: basiliximab (IL-2R antagonist) or ATG (high-risk recipients)
Rejection Types
  • Hyperacute: preformed antibodies — minutes to hours; irreversible
  • Acute cellular (ACR): T-cell mediated; rising creatinine d7–d90; treated with methylprednisolone pulses
  • Antibody-mediated (AMR): donor-specific antibodies; treated with IVIG + plasmapheresis + rituximab; worse prognosis
  • Surveillance biopsies: 3 months, 12 months post-transplant
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Post-Transplant Complications & Nursing

Opportunistic Infections
  • CMV: commonest opportunistic infection; prophylaxis with valganciclovir 3–6 months; monitor CMV PCR
  • BK virus nephropathy: BK polyomavirus — monitor BKV PCR blood/urine; treatment = immunosuppression reduction
  • PCP (Pneumocystis jirovecii): prophylaxis with co-trimoxazole for 12 months
  • Fungal prophylaxis: nystatin for 1 month; fluconazole if high risk
  • Avoid live vaccines post-transplant (MMR, yellow fever, BCG)
Post-Operative Nursing (First 48–72 Hours)
  • Urine output: monitor hourly — target >100 mL/hr initially; replace ml-for-ml if low
  • Fluid replacement: normal saline or Hartmann's — guided by urine output
  • Wound care: drain output, dressing — graft in iliac fossa (RIF or LIF)
  • Monitor creatinine daily — fall indicates graft function
  • Delayed graft function (DGF): dialysis may be needed post-op; reassess daily
  • Tacrolimus trough level: check day 1–2 and daily until stable
Long-Term Monitoring
  • Monthly: creatinine, FK levels, FBC, glucose, BP
  • Skin cancer screening: annual dermatology review (markedly increased SCC risk)
  • PTDM (post-transplant diabetes): monitor fasting glucose especially with tacrolimus
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Daily Clinical Monitoring in CKD

<130/80
BP Target in CKD (KDIGO 2021)
<53 mmol/mol
HbA1c Target (T2DM + CKD)
<0.8 g/kg/day
Protein Intake (non-dialysis CKD)
Fluid Balance Monitoring
  • Daily weights at same time, same scale, same clothing
  • Fluid restriction: urine output (previous 24h) + 500 mL insensible losses
  • Fluid intake diary — include all oral intake (foods with high water content)
  • Document oedema: pitting scale 1–4+, site (bilateral pedal, sacral, ascites)
Blood Glucose Monitoring
  • Tight glucose control slows diabetic nephropathy progression
  • Hypoglycaemia risk increases in CKD (impaired gluconeogenesis, prolonged insulin action)
  • Beware hypoglycaemia unawareness in dialysis patients
Medication Review (Renal Dose Adjustment)
  • Metformin: review at eGFR <45, stop at eGFR <30 (lactic acidosis risk)
  • NSAIDs: CONTRAINDICATED in CKD (reduce GFR, fluid retention, hyperkalaemia)
  • Iodinated contrast: pre-hydrate with IV saline; KDIGO states contrast not contraindicated but caution in G3b+
  • Aminoglycosides: single daily dosing, extend interval per eGFR, level monitoring essential
  • DOACs: dose reduction in CKD — rivaroxaban/apixaban reduced at eGFR <50; avoid at eGFR <15
  • LMWH: enoxaparin accumulates — halve dose or use UFH when eGFR <30
  • Gabapentin/pregabalin: significant dose reduction needed; accumulates causing sedation
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Renal Dietary Counselling

Important: CKD Diet Differs from Dialysis Diet

Pre-dialysis CKD patients require protein restriction (0.8 g/kg/day). Haemodialysis patients require HIGHER protein (1.2 g/kg/day) due to dialysis-related losses. Always clarify the patient's current stage before dietary advice.

Low Potassium Advice
  • Avoid: bananas, oranges, dried fruits, avocado, tomatoes, potatoes, nuts, chocolate
  • Leaching vegetables: peel, dice, boil in large amount of water, discard water
  • Avoid salt substitutes (contain KCl)
  • Restrict fruit juice and smoothies
Low Phosphate Advice
  • Avoid: processed foods, fast food, cola drinks, dark sodas, dairy excess, bran cereals
  • Organic phosphate (meat/fish) absorbed less than inorganic (additives)
  • Read food labels: avoid phosphate additives (E452, E338)
Protein
  • Non-dialysis CKD: 0.8 g/kg/day — avoid high protein diets
  • HD patients: 1.2 g/kg/day — ensure adequate intake
  • PD patients: 1.2–1.5 g/kg/day — protein losses in dialysate
Fluid & Sodium
  • Sodium: <2 g/day (5 g salt) — most important modification
  • Fluid: urine output + 500 mL (pre-dialysis); 500–800 mL/day (anuric HD)
Caloric Adequacy
  • Target 30–35 kcal/kg/day — malnutrition is common in CKD
  • Malnutrition-inflammation complex syndrome (MICS) — linked to CVD mortality
  • Renal dietitian referral essential
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Symptom Management & Quality of Life

Uraemic Pruritus
  • Affects 40–70% of dialysis patients — most distressing symptom
  • Emollients: aqueous cream, E45 — apply twice daily after bathing
  • Antihistamines: chlorphenamine at night (limited evidence)
  • Gabapentin: 100–300 mg post-dialysis — effective but accumulates (sedation risk)
  • Difelikefalin (kappa-opioid agonist): licensed specifically for dialysis pruritus
  • Improve dialysis adequacy + phosphate control
Restless Legs Syndrome (RLS)
  • Prevalence: 20–30% in dialysis patients
  • Worsens at rest/evening — disrupts sleep severely
  • Treatment: gabapentin, pramipexole (dopamine agonist), iron supplementation
Fatigue — Most Reported Symptom
  • Multifactorial: anaemia, uraemia, poor sleep, depression, dialysis schedule
  • Intradialytic exercise: cycling on recumbent bike during HD session
  • Strength training: improves muscle mass, fatigue, QoL
Psychological & Social Support
  • Depression prevalence: 25–40% in CKD/dialysis
  • Regular PHQ-9 screening; refer psychology/psychiatry
  • Employment: support return-to-work; nocturnal/home dialysis facilitates
  • Driving: assess fitness; daytime HD fatigue may impair driving
  • Travel/holiday dialysis: plan 3–6 months ahead; EDTNA/ERCA resources
Skin Care
  • Avoid prolonged sun exposure (post-transplant skin cancer risk)
  • Calcineurin inhibitor cream (tacrolimus) — avoidance on thinning skin
  • Dry skin: regular emollient application
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GCC Renal Context

Epidemiology
  • Saudi Arabia: highest dialysis prevalence per million population in the MENA region; rapid growth year-on-year
  • UAE, Qatar, Kuwait: rapidly expanding dialysis programmes; increasing living donor transplants
  • King Salman Medical City (Riyadh): major tertiary dialysis centre
  • King Faisal Specialist Hospital: leading transplant centre in KSA
  • GCC T2DM prevalence: 20–25% (among highest globally) — driving ESRD epidemic
  • Saudi Center for Organ Transplantation (SCOT): deceased donor programme coordination
Nursing Licensing (GCC)
  • SCFHS (Saudi Arabia): classification exam includes renal nursing topics at staff nurse/advanced practice level
  • DHA (Dubai): nursing licence exam — CKD management, dialysis nursing common question areas
  • DOH (Abu Dhabi): similar curriculum focus on chronic disease management
  • HAAD/DOH — haemodialysis technician pathway distinct from nursing
SGLT2 Inhibitors in CKD — Landmark Trials
CREDENCE Trial (2019) — Canagliflozin

Reduced relative risk of ESRD/doubling creatinine/renal death by 34% in patients with T2DM + CKD (eGFR 30–90 + ACR >300). First agent to show renal protection beyond RAAS blockade.

DAPA-CKD Trial (2020) — Dapagliflozin

30% reduction in composite kidney/CV outcome regardless of diabetes status. Led to indication expansion: dapagliflozin (Farxiga) indicated for CKD regardless of T2DM, eGFR 25–75.

EMPA-KIDNEY Trial (2022) — Empagliflozin

Broadest CKD population studied (eGFR 20–45 OR eGFR 45–90 + ACR ≥200). Significant reduction in kidney disease progression and CV death.

Mechanism: SGLT2 inhibitors reduce intraglomerular pressure via tubuloglomerular feedback, reduce albuminuria, and have anti-fibrotic/anti-inflammatory properties beyond glycaemic control.
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CKD Stage & Risk Calculator

📊 CKD Stage, KDIGO Risk & Management Planner

GFR Stage
Albuminuria
CKD Stage
KDIGO Risk
Key Management Priorities
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    Practice MCQs — DHA / DOH / SCFHS Exam Style

    1. According to KDIGO 2012, CKD is defined as kidney damage or GFR <60 mL/min/1.73m² for at least:
    • A. 1 month
    • B. 6 weeks
    • C. 3 months
    • D. 6 months
    The KDIGO 2012 definition requires the abnormality to be present for >3 months to distinguish CKD from acute kidney injury. The duration threshold is important for clinical classification.
    2. A patient on haemodialysis has a thrill that has disappeared from their AV fistula. What is the MOST appropriate immediate nursing action?
    • A. Apply warm compression and monitor for 2 hours
    • B. Elevate the arm and reassess next dialysis session
    • C. Urgently refer to vascular surgery/interventional radiology
    • D. Increase blood flow rate during next session
    Loss of thrill (and bruit) from an AVF indicates acute thrombosis or severe stenosis. This is a vascular emergency requiring urgent assessment within hours — delay risks permanent access loss. Time-sensitive thrombectomy or thrombolysis is most effective within 24–48 hours.
    3. Which phosphate binder is preferred in a CKD patient with hypercalcaemia and secondary hyperparathyroidism?
    • A. Calcium carbonate
    • B. Calcium acetate
    • C. Sevelamer hydrochloride
    • D. Aluminium hydroxide
    Sevelamer is a non-calcium, non-aluminium phosphate binder — preferred when calcium is already elevated (to avoid worsening hypercalcaemia and vascular calcification). Aluminium hydroxide is avoided long-term due to aluminium toxicity risk.
    4. A PD patient presents with cloudy dialysate effluent and mild abdominal discomfort. Temperature is 37.8°C. What is the FIRST action?
    • A. Admit for IV antibiotics and await culture results
    • B. Increase exchange frequency and reassess in 24 hours
    • C. Drain effluent, send for cell count and MC&S, start empirical intraperitoneal antibiotics
    • D. Remove the PD catheter immediately
    Cloudy effluent = peritonitis until proven otherwise. Protocol: drain effluent, send urgent cell count (WCC >100/mm³ with >50% neutrophils is diagnostic) and MC&S, then start empirical IP antibiotics (vancomycin + aminoglycoside or ceftazidime) without waiting for culture results. Catheter removal is reserved for refractory cases.
    5. A dialysis patient's ECG shows peaked T-waves and widened QRS complex. Serum K⁺ is 7.1 mmol/L. Which medication should be given FIRST?
    • A. Sodium bicarbonate IV
    • B. Insulin + dextrose IV
    • C. Calcium gluconate 10% IV
    • D. Salbutamol nebuliser
    With ECG changes, the priority is cardiac membrane stabilisation with calcium gluconate — it does NOT lower K⁺ but protects the myocardium within 1–3 minutes. Subsequent K⁺-lowering agents (insulin/dextrose, salbutamol) are then used. Dialysis is the definitive treatment in ESRD.
    6. According to DAPA-CKD trial, dapagliflozin is now indicated for CKD in patients:
    • A. With T2DM only, eGFR >60
    • B. On dialysis with residual urine output
    • C. Regardless of diabetes status, with eGFR 25–75 and elevated ACR
    • D. With eGFR <25 and heavy proteinuria only
    DAPA-CKD demonstrated benefit irrespective of diabetes status. Current indication: eGFR 25–75 mL/min/1.73m² with ACR ≥22.6 mg/mmol (200 mg/g). This is a paradigm shift from glucose-lowering to direct kidney-protective therapy.
    7. Which haemoglobin target is recommended for CKD patients receiving erythropoiesis-stimulating agents (ESA)?
    • A. 70–90 g/L
    • C. 100–120 g/L
    • D. 130–140 g/L
    KDIGO guidelines recommend targeting Hb 100–120 g/L with ESA therapy. Targeting Hb >130 g/L was associated with increased cardiovascular events (stroke, MI) in CHOIR and CREATE trials and should be avoided.
    8. Which drug is CONTRAINDICATED in a patient with eGFR of 25 mL/min/1.73m²?
    • A. Amlodipine
    • B. Bisoprolol
    • C. Ibuprofen (NSAID)
    • D. Omeprazole
    NSAIDs are contraindicated in CKD as they reduce renal prostaglandin synthesis, causing afferent arteriolar constriction and further GFR reduction. They also cause fluid retention, hypertension, and hyperkalaemia. Amlodipine and bisoprolol are safe. Omeprazole does not require dose adjustment.
    9. A kidney transplant recipient develops a rising creatinine on day 10 post-transplant. Tacrolimus level is therapeutic. Ultrasound shows no obstruction. Biopsy shows CD8+ T-lymphocyte infiltration. This is:
    • A. Antibody-mediated rejection (AMR)
    • B. Hyperacute rejection
    • C. Acute cellular rejection (ACR)
    • D. BK nephropathy
    CD8+ T-lymphocyte tubulitis/interstitial infiltration on biopsy = Banff acute T-cell mediated (cellular) rejection. ACR occurs days to weeks post-transplant. Treatment: IV methylprednisolone 500 mg daily for 3 days. AMR shows peritubular capillaritis + C4d staining + DSA.
    10. When creating an AV fistula, what is the minimum recommended maturation time before first use for haemodialysis?
    • A. 2 weeks
    • B. 4 weeks
    • C. 6 weeks (minimum), 3–6 months preferred
    • D. 12 months
    AVF requires time for arterialization (enlargement and wall thickening). Minimum 6 weeks but 3–6 months is preferred for optimal maturation. Early cannulation risks haematoma, pseudoaneurysm, and fistula failure. This is why access planning must begin at least 6+ months before anticipated dialysis start.