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NEPHROTIC SYNDROME BY DR. Hayam Hebah Associate professor of Internal Medicine AL Maarefa college
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objectives Definition of NS Pathophysiology Complications c/p and investigations Different causes of NS Management
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Definition: hypercholesterolemia Edema and generalised fluid retention Hypoalbuminemia(<3 g/L) Overt proteinuria: usually >3.5 g/24 hrs Nephrotic syndrome
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PATHOPHYSIOLOGY
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COMPLICATIONS
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Metabolic consequences of proteinuria Intravascular volume depletion with hypotension, or intravascular expansion with hypertension may occur Hypercoagulability( due to loss of coagulation inhibitors as antithrombin III, protein C&S and increase in liver synthesis of procoagulant factors. Infection due to urinary loss of Igs and resulting hypogammaglobulins. Hyperlipidemia and atherosclerosis Hypocalcemia and bone abnormalities Failure to thrive may be caused by anorexia, hypoproteinemia, increased protein catabolism, or frequent infectious complications. Edema of the gut may cause defective absorption, leading to chronic malnutrition
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Infection Infection is a major concern in nephrotic syndrome Increased susceptibility to infection with : --Streptococcus pneumoniae, ---Haemophilus influenzae ---Escherichia coli ---- other gram-negative organisms. ----- Varicella infection is also common. Complications of infection are: bacterial sepsis, cellulitis, pneumonia, and peritonitis.
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Proposed explanations for high incidence of infection include the following: 1.Urinary immunoglobulin losses 2.Edema fluid acting as a culture medium 3.Protein deficiency 4.Decreased bactericidal activity of the leukocytes 5.Immunosuppressive therapy 6.Decreased perfusion of the spleen caused by hypovolemia 7.Urinary loss of a complement factor (properdin factor B) that opsonizes certain bacteria
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Bone problems: Hypocalcemia d.t low serum albumin low bone density and abnormal bone histology caused by urinary losses of vitamin D–binding proteins, with consequent hypovitaminosis D and, as a result, reduced intestinal calcium absorption Osteomalacia Low bone mass may be found in relation to cumulative steroid dose
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Hypercoagulability Venous thrombosis and pulmonary embolism are well- known complications Hypercoagulability in these cases appears to derive from urinary loss of anticoagulant proteins, such as antithrombin III and plasminogen, along with the simultaneous increase in clotting factors, especially factors I, VII, VIII, and X. This high incidence may justify the routine use of preventive anticoagulation treatment during the first 6 months of a persistent nephrotic syndrome. There is also an increased risk of arterial thrombotic events, including coronary and cerebrovascular ones.This arterial risk was related to usual risk factors for arterial disease, such as hypertension, diabetes, smoking, and reduced GFR.
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Hypovolemia Hypovolemia is Observed only when the patient's serum albumin level is less than 1.5 g/dL. Symptoms include vomiting, abdominal pain, and diarrhea. The signs include cold hands and feet, delayed capillary filling, oliguria, and tachycardia. Hypotension is a late feature.
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CAUSES OF NEPHROTIC SYNDROME
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Causes of nephrotic syndrome: Primary:- Minimal change disease Focal segmental glomerulosclerosis Membranous nephropathy Secondary: Diabetic nephropathy Lupus nephritis Amyloidosis Drugs malignancy
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Congenital NS: Congenital and hereditary focal glomerulosclerosis may result from mutations of genes that code for podocyte proteins, including nephrin, podocin, or the cation channel 6 protein
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Drugs causing NS: 1. minimal-change nephropathy with NSAID use. 2.membranous nephropathy with the administration of gold and penicillamine 3.focal glomerulosclerosis in association with intravenous bisphosphonates. 4.Lithium and interferon therapy also are implicated in focal glomerulosclerosis of the collapsing type. 5.anticancer agents, such as bevacizumab, that inhibit vascular endothelial growth factor (VEGF)
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EPIDEMIOLOGY
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Age:
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Sex: -----most cases of NS occur more in males except in SLE,females are more liable. Race: Because diabetes is major cause of nephrotic syndrome, American Indians, Hispanics, and African Americans have a higher incidence of nephrotic syndrome than do white persons. HIV nephropathy is seen with greater frequency in African Americans. Focal glomerulosclerosis appears to be overrepresented in African-American children, as compared with white children.
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CLINICAL PICTURE
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C/P of NS: Symptoms: 1.swelling of the face; this is followed by swelling of the entire body. 2. Foamy urine 3.A thrombotic complication, such as deep venous thrombosis of the calf veins or even a pulmonary embolus, 4.features can be related to the cause of nephrotic syndrome
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Signs: 1.Edema is the predominant feature of nephrotic syndrome. Later,increase in weight, the development of ascites, or pleural effusions. 2.Hematuria and hypertension manifest in a minority of patient 3.according to cause
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INVESTIGATIONS
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1.Urine analysis: first step,detects proteinuria. 2.Microscopic hematuria may be seen in membranous nephropathy but not in MCD. 3.QUANTITATIVE PROTEINURIA 4.Blood examination for s. creatinine and electrolytes 5.Serum albumin. 6.Lipid profile. 7.Serologic studies: Phospholipase A2 receptor 8.Ultrasonography 9.Investigations for the cause in secondary forms
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Urine quantification: 24 hours collection Protein: creatinine ratio(PCR) in a spot sample of urine Albumin : creatinine ratio(ACR)
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RENAL BIOPSY
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For childhood nephrotic syndrome, a renal biopsy is indicated for the following: Congenital nephrotic syndrome Children older than 8 years at onset Steroid resistance Frequent relapses or steroid dependency Significant nephritic manifestations Adult nephrotic syndrome of unknown origin may require a renal biopsy for diagnosis. A renal biopsy is not indicated in adults with nephrotic syndrome from an obvious cause. For example, in a patient with longstanding diabetes
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MANAGEMENT
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Management of NS: 3 steps: 1-measures to reduce proteinuria. 2- measures to treat complications of nephrotic syndrome 3-ttt of underlying cause
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GENERAL MEASURES IN ACUTE STAGE 1.Diuretics will be needed; furosemide, spironolactone, and even metolazone may be used BUT TAKE CARE OF volume depletion may occur with diuretic use. 2.Anticoagulation has been advocated by some for use in preventing thromboembolic complications, but its use in primary prevention is of unproven value. 3.Hypolipidemic agents may be used ?? 4.For proteinuria,angiotensin-converting enzyme (ACE) inhibitors and/or angiotensin II receptor blockers(ARB).These may reduce proteinuria by reducing the systemic blood pressure, by reducing intraglomerular pressure, and also by direct action on podocytes.
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Long-Term Monitoring 1. immunizations when the patient is free of relapses and has been off immunosuppression for 3 months. Pneumococcal and influenza vaccines are recommended but are not routinely used, because their efficacy is not established. 2.treatment of relapses of steroid-responsive nephrotic syndrome. The first 2 relapses are treated in the same manner as the initial presentation; frequent relapses are treated with a maintenance dose of prednisone at 0.1-0.5 mg/kg on alternate days for 3-6 months, with the drug then tapered. 3.Monitoring for steroid toxicity every 3 months in the outpatient clinic 4.monitoring of diuretic and angiotensin antagonist regimens.
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Complications of NS and its management: For edema--- salt restriction, diuretics and in severe cases salt free albumin infusions. For infections-- vaccination and antibiotics Thrombotic complications- anticoagulation for patients with DVT and arterial thrombosis Hyperlipidemia- food restriction and lipid lowering agents Steroid toxicity-- minimisation of dose of steroids and adding steroid sparing immunosuppressives Hypovolemia and ARF-- judicious fluid control. Vitamin D supplementation. Proteins 0.8-1 g/kg/d
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MINIMAL CHANGE NEPHROPATHY(MCD)
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c/p of MCD: Main cause of NS in children ¼ of cases in adults Caused by reversible dysfunction of podocytes Present with proteinuria SELECTIVE PROTEINURIA or NS Remits with high dose of corticosteroids Histologically: - N L/M - No immune deposits by IF. - Fusion of podocytes foot processes by EM. Course may be associated with relapses and remission but rarely progress to ESRD
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Treatment: 1.Corticosteroids give excellent response. 2.Immunosuppressive medications other than steroids are usually reserved for steroid- resistant patients with persistent edema, or for steroid-dependent patients with significant steroid-related adverse effects
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Cyclophosphamide for patients who have frequently relapsing steroid- sensitive nephrotic syndrome. complications: include bone marrow suppression, hair loss, azoospermia, hemorrhagic cystitis, malignancy, mutations, and infertility Cyclosporine may be preferable in a pubertal male who is at risk of developing cyclophosphamide- induced azoospermia.
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Cyclosporin: Cyclosporine is indicated when relapses occur after cyclophosphamide treatment. Cyclosporine is a highly effective maintenance therapy for patients with steroid-sensitive nephrotic syndrome who are able to stop steroids or take lower doses; however, some evidence suggests that although remission is maintained as long as cyclosporine is administered, relapses are frequent when treatment is discontinued. Cyclosporine can be nephrotoxic and can cause hirsutism, hypertension, and gingival hypertrophy.
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Prognosis of MCD The prognosis usually is very good. Most children respond to steroid therapy; still, about 50% of children have 1 or 2 relapses within 5 years. Only 30% of children never have a relapse after the initial episode. Adults have a burden of relapse similar to that of children. However, the long-term prognosis for kidney function in patients with this disease is excellent, with little risk of renal failure. Poor patient response to steroid therapy may predict a poor outcome. Children who present with hematuria and hypertension are more likely to be steroid-resistant and have a poorer prognosis than are those who do not present with these conditions.
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FOCAL SEGMENTAL GLOMERULOSCLEROSIS
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Can occur in all age groups. More in blacks Primary form present with severe NS Secondary form with HIV, obesity, heroin addiction, vasculitis, HUS, cholesterol embolism. DD with MCD as it is focal(so biopsy may not show glomeruli) Can respond to corticosteroids but mostly no response. Immunosupressives are used also. Progression to CKD is common. Recurs after transplantation.
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Histological Forms of FSGS:
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Treatment: predisone, cyclosporine, and cyclophosphamide have all been used in treatment. Corticosteroids should be the first-line agent, with cyclophosphamide or cyclosporine as backup for steroid-resistant cases. Mycophenolate and rituximab have also been used in treating focal glomerulosclerosis. However, data on the use of these latter 2 agents are not convincing
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Prognosis of FSGS Only 20% of patients undergo remission of proteinuria; an additional 10% improve but remain proteinuric. Many patients experience frequent relapses, become steroid-dependent, or become steroid-resistant ESRD develops in 25-30% of patients with focal segmental glomerulosclerosis by 5 years and in 30-40% of these patients by 10 years
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IGM NEPHROPATHY???
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MEMBRANOUS NEPHROPATHY
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Commonest cause of NS in adults. Caused by autoantibodies directed at antigens expressed on podocytes surface. Ag is the M-type phospholipase A2 receptor1. COURSE:- 1/3 spontaneous remission. -1/3 remain in nephrotic state -1/3 develop CKD May respond to corticosteroids or immunosuppressants.
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Treatment: For idiopathic membranous nephropathy, prednisone along with chlorambucil or cyclophosphamide remains important for treatment. Other agents that have been used for the treatment are cyclosporine, synthetic corticotropin, and rituximab. Rituximab has been effective in some cases of nephrotic syndrome that relapse after prednisone treatment or in cases resistant to prednisone treatment For secondary forms, treatment is of the cause.
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Prognosis of MN: Survival rates in these patients were the same as those expected for the general population. The prognosis may worsen because of (1) an increased incidence of renal failure and the complications secondary to nephrotic syndrome, including thrombotic episodes and infection, or (2) treatment-related conditions, such as infectious complications of immunosuppressive treatments.
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DIABETIC NEPHROPATHY
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LUPUS NEPHRITIS
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