Nephrology focuses on diagnosing and treating kidney diseases. The kidneys filter waste, balance fluids, regulate blood pressure, and manage acute and chronic conditions.
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The cornerstone of treating diabetic nephropathy is tight blood sugar control. Maintaining an HbA1c target (typically around 7%) significantly slows the progression of kidney damage. This requires a tailored approach to medication, diet, and monitoring.
As kidney function declines, the risk of hypoglycemia (low blood sugar) increases because insulin stays in the body longer. Insulin doses often need to be reduced. Medications like metformin may need to be stopped or dose-adjusted. Continuous Glucose Monitoring (CGM) is highly recommended to manage levels without dangerous lows safely.
Sodium-glucose cotransporter-2 (SGLT2) inhibitors are a game-changing class of medication. Drugs like dapagliflozin and empagliflozin work by blocking sugar reabsorption in the kidney, causing it to be excreted in urine.
Beyond lowering blood sugar, they have profound direct protective effects on the kidneys. They lower glomerular pressure, reduce inflammation, and prevent scarring. They are now considered standard of care for diabetic nephropathy, independent of their glucose-lowering effect.
Controlling hypertension is as critical as controlling diabetes. The target blood pressure is typically lower than for the general population, often <130/80 mmHg, to protect the fragile kidney vessels.
ACE inhibitors (such as lisinopril) or ARBs (such as losartan) are the first-line treatment. These drugs do double duty: they lower systemic blood pressure and selectively dilate the efferent vessels of the kidneys, reducing the pressure inside the filter. This specific mechanism reduces proteinuria and preserves function.
For patients who continue to have protein leakage despite standard treatment, a newer class of drugs called non-steroidal mineralocorticoid receptor antagonists (like finerenone) offers hope. These drugs block the overactivation of mineralocorticoid receptors, which drives inflammation and fibrosis in the kidney.
They are used in conjunction with SGLT2 inhibitors and ACE/ARBs to provide a multi-layered shield against progression. Monitoring for high potassium is necessary during this therapy.
GLP-1 receptor agonists are injectable diabetes medications that also show kidney benefits. They improve blood sugar, promote significant weight loss, and reduce oxidative stress in the kidneys.
Weight loss reduces the burden of hyperfiltration on the kidneys. These drugs are an excellent option for patients who need to manage both obesity and nephropathy risk, providing a metabolic and renal benefit.
Treatment extends to managing the complications of failed kidneys. Anemia is treated with erythropoiesis-stimulating agents (ESAs) and iron supplements to stimulate red blood cell production and combat fatigue.
Bone mineral disease is managed with phosphate binders (taken with meals to block phosphorus absorption) and active Vitamin D supplements. This prevents the body from stealing calcium from the bones, reducing fracture risk and bone pain.
A renal dietitian is essential for ongoing treatment. The diet changes as the disease progresses. In the early stages, the focus is on blood sugar and heart health. In later stages, protein, potassium, and phosphorus must be strictly controlled.
Low-protein diets may be prescribed to reduce the workload on the kidneys. Sodium restriction is universal to help control blood pressure and fluid retention. The diet is treated as a prescription, vital for delaying dialysis.
When eGFR drops below 20-30, preparation for End Stage Renal Disease (ESRD) begins. This involves education about dialysis modalities (hemodialysis vs. peritoneal dialysis) and preemptive transplant evaluation.
Creating a vascular access (fistula) months in advance is a crucial step in treatment. This ensures a mature, safe access point is ready when dialysis becomes necessary, avoiding the need for risky emergency catheters.
Follow-up is rigorous. Patients require labs every 3 to 4 months to monitor kidney function, electrolytes, and blood counts. This surveillance enables timely medication adjustments.
Monitoring also includes checking for cardiovascular disease, foot health, and eye health. Diabetic nephropathy care is a lifelong commitment to surveillance to catch complications early and adjust the course.
Statins are routinely prescribed to manage cholesterol. Since heart disease is the primary cause of death in kidney patients, aggressive lipid control is a form of kidney treatment. It prevents plaque buildup in the renal arteries and reduces systemic inflammation.
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No. In diabetic nephropathy, ACE inhibitors and ARBs are prescribed to protect the kidneys, not just to lower blood pressure. Even if your pressure is normal, these drugs reduce the internal pressure in the kidneys and stop protein leakage. Stopping them can accelerate kidney damage.
They are generally safe but can increase the risk of genital yeast infections and, rarely, diabetic ketoacidosis. They are not recommended for people with very low kidney function (low eGFR) initiating treatment, though guidelines are expanding. Your doctor will determine if they are right for you.
Acetaminophen (Tylenol) is generally the safest option for kidney patients. You should avoid NSAIDs like ibuprofen (Advil, Motrin) and naproxen (Aleve) as they can cause acute kidney injury and worsen chronic disease.
Yes, eating less protein reduces the amount of waste your kidneys have to filter, which can lower the pressure inside the kidney filters and slow the disease. However, you must ensure you don’t become malnourished, so work with a dietitian.
In the early stages, you might go once a year. As the disease progresses to stages 3 and 4, visits will increase to every 3 to 6 months. In late stage 4 or 5, you may need monthly visits to manage complications and prepare for dialysis or transplant.
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