Membranous nephropathy

Initial evaluation should start with a thorough history and physical exam followed by laboratory testing. Renal biopsy remains the diagnostic standard. Because both primary and secondary membranous nephropathy (MN) can present with nephrotic syndrome or proteinuria, further workup is needed in all patients to look for secondary causes.

History

Patients typically present with edema or hypertension. The edema can be mild or severe and most commonly begins in the legs. Edema of MN is more likely to affect the face than edema due to other causes such as cardiac failure. Patients may also report foamy urine and nonspecific symptoms of malaise, anorexia, and fatigue. They may also present with the incidental finding of proteinuria on urinary dipstick or abnormal renal function on serologic testing. A thorough history includes assessing for risk factors of secondary MN including a history of hepatitis B or C and autoimmune disease, and a full drug history. Systematic review may reveal symptoms suggestive of solid organ malignancy.

Examination

Physical exam findings may include:

• High BP

• Xanthelasma due to hypercholesterolemia

• White banding of the nails (Muehrcke lines) due to hypoalbuminemia

• Localized edema or anasarca (extreme generalized edema)

• Specific findings of underlying disease (i.e., features of systemic lupus erythematosus (SLE), hepatitis, or malignancy).

Initial investigations

All patients with suspected MN should have the following tests performed:

• Serum creatinine and creatinine clearance: to assess renal function. Glomerular filtration rate can be calculated using the value of serum creatinine [ Glomerular Filtration Rate Estimate by the IDMS-Traceable MDRD Study Equation Opens in new window ] ​

• BUN: may demonstrate abnormal renal function

• Urine microscopy: may show oval fat bodies and fatty casts

• Urine protein to creatinine ratio: may be followed by 24-hour urine collection, which may reveal significant proteinuria (>3.5 g/24 hours) indicative of nephrotic syndrome

• Serum albumin: hypoalbuminemia will be seen in nephrotic syndrome

• Lipid profile: hyperlipidemia is commonly seen in nephrotic syndrome.

Investigation for primary membranous nephropathy

Patients can be tested for m-type phospholipase A2 receptor (PLA2R) autoantibodies if primary MN is suspected. Approximately 80% of patients with primary MN have autoantibodies against PLA2R; therefore, these antibodies are highly suggestive of primary MN.[9]Qin W, Beck LH Jr, Zeng C, et al. Anti-phospholipase A2 receptor antibody in membranous nephropathy. J Am Soc Nephrol. 2011 Jun;22(6):1137-43. http://www.ncbi.nlm.nih.gov/pubmed/21566055?tool=bestpractice.com ​ Two tests for anti-PLA2R autoantibodies have been approved by the Food and Drug Administration (FDA), and are now commercially available.

Patients can also be tested for thrombospondin type 1 domain–containing 7A (THSD7A) autoantibodies, which present in around 10% of patients.​[19]Tomas NM, Beck LH Jr, Meyer-Schwesinger C, et al. Thrombospondin type-1 domain-containing 7A in idiopathic membranous nephropathy. N Engl J Med. 2014 Dec 11;371(24):2277-87. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4278759 http://www.ncbi.nlm.nih.gov/pubmed/25394321?tool=bestpractice.com ​​

Patients with MN should be evaluated for associated conditions regardless of whether anti-PLA2R antibodies and/or anti-THSD7A antibodies are present.[20]Kidney Disease: Improving Global Outcomes (KDIGO) Glomerular Diseases Work Group. KDIGO 2021 clinical practice guideline for the management of glomerular diseases. Kidney Int. 2021 Oct;100(4s):S1-S276. https://www.doi.org/10.1016/j.kint.2021.05.021 http://www.ncbi.nlm.nih.gov/pubmed/34556256?tool=bestpractice.com

Investigations for secondary causes

Specific laboratory testing for secondary causes should include:

• Hepatitis B and C serology

• Liver function tests: if elevated, may suggest underlying hepatitis

• Complement levels (C3, C4, and CH50): may be low if MN is associated with SLE

• ANA: to exclude underlying SLE

• Antidouble-stranded DNA or anti-Smith antigen if results from antinuclear antibody testing are positive: highly specific tests for SLE

• Anti-SS-B, anti-SS-A: elevated levels suggest underlying Sjogren syndrome

• Syphilis serology: may be required in high-risk groups

• Investigations for underlying malignancy: if history or clinical exam leads to clinical suspicion of a solid organ tumor, then appropriate screening should be arranged. Not routinely recommended for every patient.

Imaging

Bilateral renal ultrasound with Doppler evaluation of the renal arteries should be performed to assess for other possible causes of decreased renal function. Specifically, ultrasound is useful to assess the size of the kidneys to rule out hydronephrosis; to evaluate systolic arterial pressures to rule out renal artery stenosis; and to evaluate resistive indices for microvascular disease.

Renal biopsy

Patients are referred to a specialist for consideration of a renal biopsy. Definitive diagnosis is based on biopsy findings, and it remains the most sensitive and specific test.

Light microscopy

• Thickening of the glomerular basement membrane (GBM) is diffuse throughout all glomeruli in the absence of significant hypercellularity.

Immunofluorescence microscopy

• IgG is seen in a diffuse granular pattern, with C3 along the GBM.

Electron microscopy

• Stage 1: light microscopy is normal; small electron-dense subepithelial deposits with segmental distribution can be observed; focal foot process effacement is a constant feature.

• Stage 2: subepithelial electron-dense deposits are seen with small GBM extensions (spikes); GBM spikes can be seen with silver staining (segments of GBM between dense deposits).

• Stage 3: dense deposits are incorporated in the GBM; thickening of the GBM is detectable by light microscopy.

• Stage 4: GBM is markedly thickened, with the initial electron-dense deposits now electron lucent.​[21]Ehrenreich T, Churg J. Pathology of membranous nephropathy. Pathol Annu. 1968;3:145-86.​​