MEMBRANOUS GLOMERULONEPHRITIS (OR NEPHROPATHY)

Membranous nephropathy (MN) is the most common cause of nephrotic syndrome in Caucasian adults. The majority of cases diagnosed are idiopathic, although cases associated with hepatitis B infections, malignancy, systemic lupus erythematosus, and drugs (such as penicillamine and gold) have been reported (Lewis & Neilson, 2011). The pathology is thought to be related to antibodies to a podocyte protein. Light microscopy may reveal thickened glomerular basement membranes. Immunofluorescent microscopy shows deposits of IgG and sometimes C3. Electron microscopy displays thick densities on the capillary loops and effacement on the podocyte (Adler & Salant, 2003). MN affects more males than females, and is most likely to occur in the fourth to fifth decades of life. Clinically, most patients present with edema and nephrotic-range proteinuria. Hematuria is seen in about half of patients. Mild hypertension may be noted in some patients. Increased plasma creatinine concentrations are seen in patients with advanced disease, and these patients are also more likely to have hypertension. Hypercoagulopathy is a recognized complication of all the nephropathies, but the risk is increased in MN (Couser & Cattran, 2010; Lewis & Neilson, 2011).

The natural history of MN is variable. It is estimated that 25% to 50% of patients presenting with nephrotic syndrome will develop ESRD within 10 to 15 years from diagnosis. Other patients have a very benign course, characterized by spontaneous remissions. As with most of the glomerulopathies, long-term studies on outcome and progression to kidney disease are limited. The variability in the natural course of the disease makes the evaluation and selection of therapy both difficult and controversial (Couser & Cattran, 2010). Factors that are associated with increased risk of progression to ESRD include male gender, age >50 years, proteinuria >8 g/d, increased plasma creatinine at the time of presentation, interstitial fibrosis seen on biopsy, and hypertension (Couser & Cattran, 2010). Conventional treatment is focused on management of blood pressure (BP), proteinuria, edema, and hyperlipidemia. Patients at high risk for developing progressive kidney disease may benefit from a 6-month course of a combination of corticosteroids and an oral alkylating agent (Couser & Cattran, 2010; KDIGO, 2012).

FOCAL SEGMENTAL GLOMERULOSCLEROSIS

Focal segmental glomerulosclerosis (FSGS) is notable for scarring or sclerosing of the glomeruli. “Focal” refers to the fact that not all the glomeruli are involved. It is more common in African Americans and there is an increased incidence in males. It is one of the primary glomerulopathies, so the majority of cases are thought to be idiopathic. However, systemic diseases are also associated with FSGS. FSGS is associated with HIV1; parvovirus; cytomegalovirus (CMV); obesity; and drugs, including pamidronate, heroin, lithium, anabolic steroids, and interferons (Markowitz, Nasr, Stokes, & D’Agati, 2010). The likely pathology in hereditary FSGS is injury to the podocyte, perhaps by a T-cell mediated factor that affects permeability. Light microscopy shows sclerotic and hyalinotic features in the glomerular tuft. Immunofluorescent microscopy is normal except for IgM and C3 in the sclerotic lesions. Electron microscopy shows widespread effacement of the foot processes and deterioration of the podocytes (Adler & Salant, 2003; Appel & D’Agati, 2010; Markowitz et al., 2010).

DIABETIC NEPHROPATHY (DIFFUSE AND NODULAR GLOMERULOSCLEROSIS)

Diabetic glomerular disease is the most common cause of end-stage kidney disease (ESRD) requiring dialysis (USRDS, 2012). The risk of developing diabetic nephropathy in those with type 1 diabetes (T1DM) and type 2 (T2DM) diabetes appears to be genetically mediated. The risk for developing ESRD for type 1 and type 2 diabetics is similar, with an incidence of about 50% after 30 years of disease. The higher incidence of the latter means that the majority of individuals with ESRD have T2DM. Diabetic nephropathy is described as a diffuse and nodular glomerulosclerosis. Diffuse thickening in the glomerular basement membrane is observed with the light or electron microscope in patients with diabetic nephropathy.

Kimmelstiel–Wilson lesions are nodules that can be seen in more advanced stages of diabetic renal disease in light microscopy. Immunofluoroscent microscopy may show deposition of IgG in a linear pattern. Renal biopsies from both T1DM and T2DM are similar (Lewis & Neilson, 2011). The exact mechanism of diabetic glomerular disease is not clearly understood. One theory is that advanced glycosylation end products (produced by the glycosylation of proteins) accumulate and alter the mesangial matrix (Lewis & Neilson, 2011; Ritz & Wolf, 2010). Diabetic nephropathy develops in stages: initially patients are noted to have an increase in glomerular filtration (hyperfiltration), then microalbuminuria and then proteinuria. Increased glucose concentrations may contribute to increased pressures within the glomerulus, which are detrimental. The onset of overt diabetic nephropathy is usually about 15 years after the initial renal changes and ESRD about 25 years after (Lewis & Neilson, 2011; Ritz & Wolf, 2010).

Clinically, patients with diabetic nephropathy may initially present with microalbuminuria, with proteinuria occurring later in the course of disease, and that proteinuria can be in the nephrotic range. Patients with diabetic nephropathy typically have normal to enlarged kidneys on ultrasound. Conversely, small kidney size is seen in nondiabetic causes of glomerular disease. Diagnosis of diabetic nephropathy may be made without a renal biopsy in many patients, but the practitioner is cautioned that diabetics may have other causes of renal disease (Ritz & Wolf, 2010; Lewis & Neilson, 2011). Strict glycemic, BP, and lipid control in this group is critical (Ritz & Wolf, 2010; Lewis & Neilson, 2011).

AMYLOIDOSIS

Patients with renal amyloidosis usually present with severe proteinuria, severe edema, and low albumin concentrations. Multiple organ involvement is often observed. Patients may present with hepatosplenomegaly; congestive heart failure; gastrointestinal, cutaneous, or nerve disease; and/or carpal tunnel syndrome. Initially, the plasma creatinine concentration may be normal or moderately elevated. This can often progress rapidly to ESRD. The pathogenesis is thought to be related to deposits of beta-pleated amyloid fibrils in the glomeruli, renal vasculature, and interstitium. In primary amyloid disease, amyloid L is deposited. Amyloid A is seen in secondary disease. Secondary disease has been associated with multiple myeloma, tuberculosis, rheumatoid arthritis, familial Mediterranean fever (FMF), chronic infection, and chronic inflammation. Primary amyloidosis is the most likely diagnosis in patients over 40 years of age. The prognosis and treatment options for primary amyloidosis are limited. Treatment of amyoid L has included high-dose melphalan with autologous stem cell transplant. More recently, some trials with mephalan and high-dose dexamethasone have shown promise in some patients (Palladini et al., 2007). Treatment of the cause(s) of secondary amyloidosis (e.g., infection) may lead to its resolution and thus a more favorable outcome for organ health (Gertz et al., 2005).

Nephritic Glomerular Diseases

IMMUNOGLOBULIN A NEPHROPATHY (IgAN, BERGER’S DISEASE)

Alport’s Syndrome

Alport’s syndrome is an X-chromosome-linked disorder associated with hearing loss and lenticular opacities. It is usually identified at birth or during the neonatal period. Males often progress to ESRD in late adolescence. Females tend to have a more benign course. Histologically, thinning of the glomerular basement membrane is observed early in the disease course. Later, splitting or laminating of the basement membrane is more diagnostic of Alport’s syndrome. Asymptomatic hematuria and proteinuria or gross intermittent hematuria are typically seen early. Although family history of deafness favors the diagnosis of Alport’s over IgAN, disease presentation may be quite similar in other respects (Adler & Salant, 2003; Kashtan, 2010).

POSTINFECTIOUS GLOMERULONEPHRITIS