Summary

This document provides an overview of drug-induced kidney injury. It covers various mechanisms, clinical presentations, and management strategies for different categories of nephrotoxic drugs. The document includes information on acute tubular injury, osmotic nephropathy, and hemodynamically mediated kidney injury, encompassing different drugs' roles.

Full Transcript

I. Tubular Epithelial Cell Damage A. Acute Tubular Injury/Necrosis 1. Aminoglycoside Nephrotoxicity ○ Mechanism: Accumulates in the proximal tubules, causing oxidative stress and cellular necrosis. The drug enters through endocytosis due to its cationic nature,...

I. Tubular Epithelial Cell Damage A. Acute Tubular Injury/Necrosis 1. Aminoglycoside Nephrotoxicity ○ Mechanism: Accumulates in the proximal tubules, causing oxidative stress and cellular necrosis. The drug enters through endocytosis due to its cationic nature, leading to tubular obstruction. ○ Clinical Presentation: Gradual increase in serum creatinine (SCr), decreased urine output, seen 5-7 days after treatment. ○ Diagnostics: Rising SCr and BUN, decreased creatinine clearance. ○ Management: Discontinue therapy, use alternative antibiotics like penicillin. ○ Mnemonic: "AGNs cause Acute Glomerular Nephritis slowly" 2. Radiographic Contrast Media Nephrotoxicity ○ Mechanism: Causes renal vasoconstriction via the release of adenosine and endothelin, leading to ischemia and reduced renal blood flow. ○ Clinical Presentation: Non-oliguric AKI, with SCr peaking 3-4 days after exposure. ○ Management: Avoid nephrotoxic agents, hydrate, use low-osmolar contrast. 3. Mnemonic: "Contrast = Constricts renal flow" 4. Cisplatin Nephrotoxicity ○ Mechanism: Cisplatin accumulates in proximal tubular cells, causing oxidative damage and necrosis. ○ Clinical Presentation: Polyuria, decreased serum magnesium (hypomagnesemia), hypokalemia, and hypocalcemia. ○ Management: Adjust doses, manage electrolyte disturbances. ○ Mnemonic: "Cisplatin Cells Plunder Mg and Ca" 5. Amphotericin B Nephrotoxicity ○ Mechanism: Binds to ergosterol in the kidney’s cell membrane, causing increased permeability and necrosis. It also induces vasoconstriction in afferent arterioles. ○ Clinical Presentation: Nonoliguric AKI, electrolyte wasting. ○ Management: Switch to liposomal Amphotericin, replace electrolytes. ○ Mnemonic: "Ampho tears membranes, spills electrolytes" B. Osmotic Nephropathy ○ Drugs involved: Mannitol, intravenous immunoglobulin (IVIG) containing sucrose. ○ Mechanism: High osmolar drugs cause cellular swelling and vacuolization in proximal tubular cells. ○ Presentation: Oliguria 2-4 days after exposure; cellular swelling is evident. ○ Management: Discontinue the offending agent. II. Hemodynamically Mediated Kidney Injury This results from drugs that impair kidney blood flow, affecting renal hemodynamics. 1. ACEIs and ARBs ○ Mechanism: These drugs dilate efferent arterioles, reducing glomerular pressure and thereby lowering glomerular filtration rate (GFR). ○ Risk Factors: Patients with renal artery stenosis, CHF, or pre-existing kidney disease. ○ Clinical Presentation: AKI with rise in serum creatinine. ○ Management: Monitor SCr, discontinue if creatinine rises >30%. INITIATE LOW DOSE ○ Mnemonic: "ACE/ARB Arrest Efferent pressure" 2. NSAIDs and COX-2 Inhibitors ○ Mechanism: Inhibit prostaglandin synthesis, reducing afferent arteriolar dilation, which leads to ischemia in conditions of reduced renal blood flow. ○ Clinical Presentation: : AKI within 2-7 days, weight gain, diminished urine output, elevated BUN, SCr, and blood pressure. ○ Management: Stop NSAIDs and provide supportive care. Kidney function typically recovers in 3-5 days. ○ Mnemonic: "NSAIDs & Cox inh. Narrow Prostaglandin flow" 3. Cyclosporine & Tacrolimus ○ Mechanism: Causes vasoconstriction of afferent arterioles through increased thromboxane A2 and endothelin production, leading to reduced renal plasma flow and GFR. ○ Clinical Presentation: Hypertension, hyperkalemia, decreased GFR. ○ Management: Dose reduction, calcium channel blockers. ○ Mnemonic: "Cyclic pressure on afferents" 4. SGLT-2 ○ Mechanism: SGLT-2 inhibitors can cause volume depletion and reduce renal perfusion. They lead to prerenal AKI by reducing glomerular filtration through vasoconstriction of the afferent arteriole via tubuloglomerular feedback. ○ Clinical Presentation: AKI, volume depletion, and prerenal azotemia. ○ Diagnostics: Elevated serum creatinine and decreased GFR, urinalysis for dehydration markers. ○ Management: Discontinue the drug, ensure hydration, treat electrolyte imbalances, provide IV fluids for volume depletion. ○ Mnemonic: "SGLT Sends Glomerular Flow Low" 5. Chimeric Antigen Receptor (CAR) T-Cell Therapy ○ Mechanism: CAR T-cells trigger a cytokine release syndrome (CRS) leading to systemic inflammation, hypotension, and multi-organ toxicity, including AKI. Prerenal injury is common due to systemic hypotension, and direct tubular damage may occur due to cytokine storm. ○ Clinical Presentation: High fever, hypotension, hypoxia, multi-organ failure, and AKI, typically within days to weeks of treatment. ○ Diagnostics: AKI with rapid rise in serum creatinine, urinalysis, and signs of systemic inflammation. ○ Management: Supportive care, including vasopressors and IV fluids. Anti-interleukin-6 (IL-6) therapy (tocilizumab) and corticosteroids are used to manage severe CRS. ○ Mnemonic: "CAR-T Cells Cause Cytokine Chaos" III. Obstructive Nephropathy 1. Crystal Nephropathy ○ Drugs involved: Acyclovir, Sulfonamides, Indinavir, Methotrexate. ○ Mechanism: Precipitation of drug crystals in the renal tubules due to supersaturation or pH changes in urine. ○ Clinical Presentation: Hematuria, flank pain. ○ Management: Hydration, adjust urine pH. ○ Mnemonic: "Crystals Clog kidneys" and "Crystals Stop Inflow" Crystal nephropathy, Sulfonamides, Indinavir. 2. Vancomycin Cast Nephropathy ○ Mechanism: Vancomycin forms obstructive tubular casts, leading to nephrotoxicity.. ○ Clinical Presentation: Sudden AKI, electrolyte imbalances. ○ Management: Discontinue vancomycin, hydrate. ○ Mnemonic: "Vancomycin Volume Casts in tubules" 3. Acute Phosphate Nephropathy Mechanism: Caused by oral sodium phosphate solutions (used for bowel cleansing) leading to calcium-phosphate precipitation in the renal tubules, which results in tubular calcification and nephrocalcinosis. Clinical Presentation: AKI developing days to months after exposure. Commonly presents with normocalcemia, low-grade proteinuria, and bland urinary sediment. Diagnostics: Elevated serum phosphate, urinalysis (low-grade proteinuria), renal biopsy shows calcium-phosphate crystals. Management: Discontinue phosphate-containing agents, aggressive hydration, and electrolyte management. Dialysis may be needed in severe cases. Mnemonic: "Phosphate Packs Kidneys with Crystals" 4. Nephrolithiasis ○ Mechanism: Formation of kidney stones due to the precipitation of drugs or their metabolites in the urinary tract, often caused by sulfonamides, triamterene, and protease inhibitors. ○ Clinical Presentation: Flank pain, hematuria, and possible urinary tract obstruction without a decrease in GFR. ○ Diagnostics: Imaging (CT or ultrasound) to identify stones, urinalysis showing hematuria and crystals. ○ Management: Hydration to maintain urine output, discontinuation of the offending drug, alkalinization of urine (for certain drugs), thiazide diuretics for calcium stones, or surgical interventions (e.g., lithotripsy) for large stones. ○ Mnemonic: "Stones Stop the Flow" IV. Glomerular Disease 1. Minimal Change Disease (MCD) ○ Drugs involved: NSAIDs, Lithium, Interferons. ○ Mechanism: T-cell dysfunction leads to cytokine release, damaging the glomerular filtration barrier and causing proteinuria. ○ Clinical Presentation: Nephrotic syndrome with proteinuria, edema, and hypoalbuminemia. ○ Management: Corticosteroids, ACE inhibitors, and ARBs to control symptoms. ○ Mnemonic: "Minimal Cells Disappear (MCD)" 2. Focal Segmental Glomerulosclerosis (FSGS) ○ Drugs involved: NSAIDs, Lithium, Sirolimus. ○ Mechanism: Podocyte injury causes glomerular scarring, leading to proteinuria and nephrotic syndrome. ○ Clinical Presentation: Proteinuria, hypertension. ○ Management: ACEIs/ARBs, immunosuppressants. ○ Mnemonic: "FSGS = Focal Scars Glomeruli" 3. Membranous Nephropathy ○ Mechanism: Immune complexes deposit in the glomerular membrane, causing proteinuria and nephrotic syndrome. Triggered by autoimmune diseases or drugs like NSAIDs and gold salts. ○ Clinical Presentation: Proteinuria (foamy urine), edema, weight gain, hypoalbuminemia. ○ Diagnostics: Urinalysis (proteinuria), blood tests (low albumin), kidney biopsy (immune complex deposits). ○ Management: ACEIs/ARBs, diuretics, corticosteroids, immunosuppressants, statins for hyperlipidemia. ○ Mnemonic: "Membrane Mess by Immune Complexes" V. Tubulointerstitial Nephritis 1. Nonsteroidal Anti-inflammatory Drugs (NSAIDs) ○ Mechanism: NSAIDs reduce prostaglandin synthesis, causing decreased blood flow to the renal interstitium and leading to inflammation. ○ Clinical Presentation: AKI, fever, rash, eosinophilia, oliguria. ○ Diagnostics: Elevated serum creatinine, kidney biopsy showing inflammation. ○ Management: Discontinue NSAIDs, corticosteroids if needed. ○ Mnemonic: "NSAIDs Narrow Flow to Nephrons" 2. Proton Pump Inhibitors (PPIs) ○ Mechanism: PPIs cause a hypersensitivity reaction, resulting in acute interstitial nephritis (AIN). ○ Clinical Presentation: AIN symptoms occur weeks to months after PPI exposure, often without typical signs like fever or rash. ○ Diagnostics: Kidney biopsy confirms AIN. ○ Management: Discontinue PPI, corticosteroid therapy. ○ Mnemonic: "PPIs Prick the Kidneys" 3. Immune Checkpoint Inhibitors Mechanism: Immune-related adverse effects from these drugs can trigger AIN by attacking kidney tissues. Clinical Presentation: AKI, may lack typical AIN symptoms like rash and eosinophilia. Diagnostics: Kidney biopsy required for confirmation. Management: Discontinue offending drug, corticosteroids for severe cases. Mnemonic: "Checkpoint Inhibitors Challenge the Kidneys" A. Chronic Interstitial Nephritis 1. Lithium Mechanism: Long-term lithium use damages renal tubular cells, leading to chronic inflammation and nephrogenic diabetes insipidus. Clinical Presentation: Polyuria, polydipsia, increased BUN and creatinine, bland urine sediment. Diagnostics: Kidney biopsy, routine kidney function tests. Management: Discontinue lithium, consider using amiloride to prevent nephrogenic diabetes insipidus. Mnemonic: "Lithium Loves Tubular Damage" 2. Cyclosporine and Tacrolimus Mechanism: Calcineurin inhibitors cause vasoconstriction, leading to chronic ischemic damage in the renal interstitium. Clinical Presentation: Hypertension, hyperkalemia, decreased GFR, renal biopsy shows fibrosis. Management: Reduce dosage, switch to alternative immunosuppressants, use calcium channel blockers for vasoconstriction. Mnemonic: "Calcineurin Constricts and Causes Chronic Damage" 3. Aristolochic Acid Mechanism: Herbal products containing aristolochic acid form mutagenic compounds, causing interstitial fibrosis and tubular atrophy. Clinical Presentation: Hypertension, mild proteinuria, increased creatinine, rapid progression to end-stage kidney disease (ESKD). Management: Avoid aristolochic acid, corticosteroids may help in managing nephropathy. Mnemonic: "Aristolochic Acid Attacks Interstitium" B. Papillary Necrosis 1. Analgesic Nephropathy Mechanism: Chronic analgesic use (especially phenacetin, aspirin) depletes renal glutathione, causing papillary necrosis and interstitial nephritis. Clinical Presentation: Asymptomatic early, progressing to hematuria, proteinuria, hypertension, and renal failure. Management: Discontinue analgesics, monitor kidney function closely. Mnemonic: "Pain Pills Poison Papillae" VI. Renal Vasculitis, Thrombosis, and Cholesterol Emboli 1. Renal Vasculitis ○ Mechanism: Autoimmune attack on kidney blood vessels. ○ Management: Immunosuppressants. ○ Mnemonic: "Vasculitis Violates vessels" 2. Thrombotic Microangiopathy ○ Mechanism: Blood clot formation obstructs capillaries. ○ Management: Anticoagulants. ○ Mnemonic: "Tiny Thrombi Trouble kidneys" 3. Cholesterol Emboli ○ Mechanism: Plaque rupture leads to embolization. ○ Management: Statins, surgery. ○ Mnemonic: "Cholesterol Clots create chaos"

Use Quizgecko on...
Browser
Browser