Lupus nephritis: Difference between revisions

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*SLE predominantly affects women of childbearing age (female-to-male ratio 9:1); lupus nephritis typically presents at ages 20-40 years<ref name="Medscape_LN"/>
*SLE predominantly affects women of childbearing age (female-to-male ratio 9:1); lupus nephritis typically presents at ages 20-40 years<ref name="Medscape_LN"/>
*Higher incidence and more severe disease in African Americans, Hispanics, and Asians
*Higher incidence and more severe disease in African Americans, Hispanics, and Asians
*Males with SLE have a '''higher rate of renal involvement''' and '''worse prognosis''' than females
*Males with SLE have a higher rate of renal involvement and worse prognosis than females
*Children with SLE have '''more frequent and more aggressive''' renal disease than adults
*Children with SLE have more frequent and more aggressive renal disease than adults
*Lupus nephritis usually arises within the first 5 years of SLE diagnosis; may be the presenting manifestation of SLE
*Lupus nephritis usually arises within the first 5 years of SLE diagnosis; may be the presenting manifestation of SLE
*Delayed diagnostic biopsy >6 months is associated with a 9-fold increased risk of ESKD<ref name="TenTips">Ten tips in lupus nephritis management. ''Rheumatology''. 2025. PMC11770280.</ref>
*Delayed diagnostic biopsy >6 months is associated with a 9-fold increased risk of ESKD<ref name="TenTips">Ten tips in lupus nephritis management. ''Rheumatology''. 2025. PMC11770280.</ref>
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*'''Class IV is the most common biopsy finding''' and carries the worst untreated prognosis
*Class IV is the most common biopsy finding and carries the worst untreated prognosis
*Mixed classes (III/V or IV/V) have features of both proliferative and membranous disease
*Mixed classes (III/V or IV/V) have features of both proliferative and membranous disease
*Class can transform — mild disease may progress to severe proliferative disease; repeat biopsy may be needed for flares
*Class can transform — mild disease may progress to severe proliferative disease; repeat biopsy may be needed for flares
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===Mechanism===
===Mechanism===
*Anti-dsDNA and other autoantibodies form immune complexes → deposit in mesangium and glomerular capillary walls
*Anti-dsDNA and other autoantibodies form immune complexes → deposit in mesangium and glomerular capillary walls
*Complement activation (classical pathway) → C3, C4 consumption → '''low serum C3 and C4'''
*Complement activation (classical pathway) → C3, C4 consumption → low serum C3 and C4
*Inflammation → cellular proliferation, crescent formation, fibrinoid necrosis
*Inflammation → cellular proliferation, crescent formation, fibrinoid necrosis
*Chronic inflammation → sclerosis and irreversible nephron loss
*Chronic inflammation → sclerosis and irreversible nephron loss
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*Hypertension (new or worsening)
*Hypertension (new or worsening)
*Rising creatinine, decreased urine output
*Rising creatinine, decreased urine output
*Often concurrent with '''other signs of lupus flare:''' fever, malar rash, arthritis, oral ulcers, pleurisy, pericarditis, cytopenias
*Often concurrent with other signs of lupus flare: fever, malar rash, arthritis, oral ulcers, pleurisy, pericarditis, cytopenias


====SLE presenting with renal disease as the first manifestation====
====SLE presenting with renal disease as the first manifestation====
*Young woman with '''unexplained nephritic or nephrotic syndrome'''
*Young woman with unexplained nephritic or nephrotic syndrome
*May have undiagnosed SLE — look for constitutional symptoms, rash, arthritis, photosensitivity, oral ulcers, alopecia, serositis
*May have undiagnosed SLE — look for constitutional symptoms, rash, arthritis, photosensitivity, oral ulcers, alopecia, serositis
*'''Any young woman with GN should be tested for SLE'''
*Any young woman with GN should be tested for SLE


====Lupus nephritis flare====
====Lupus nephritis flare====
*Known LN patient with '''worsening proteinuria, rising creatinine, new hematuria, or declining complement levels'''
*Known LN patient with worsening proteinuria, rising creatinine, new hematuria, or declining complement levels
*May be triggered by medication noncompliance, infection, pregnancy, UV exposure
*May be triggered by medication noncompliance, infection, pregnancy, UV exposure
*'''Rising anti-dsDNA + falling C3/C4''' often precedes clinical flare by weeks
*Rising anti-dsDNA + falling C3/C4 often precedes clinical flare by weeks


====Rapidly progressive glomerulonephritis (RPGN)====
====Rapidly progressive glomerulonephritis (RPGN)====
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*Cytopenias: from cyclophosphamide, mycophenolate, azathioprine; may present with neutropenic fever
*Cytopenias: from cyclophosphamide, mycophenolate, azathioprine; may present with neutropenic fever
*Steroid side effects: hyperglycemia, psychosis, adrenal crisis on abrupt withdrawal, AVN of femoral head
*Steroid side effects: hyperglycemia, psychosis, adrenal crisis on abrupt withdrawal, AVN of femoral head
*Thrombotic microangiopathy (TMA): may occur in LN, especially with '''antiphospholipid antibodies''' — presents with microangiopathic hemolytic anemia, thrombocytopenia, renal failure; consider concurrent antiphospholipid syndrome
*Thrombotic microangiopathy (TMA): may occur in LN, especially with antiphospholipid antibodies — presents with microangiopathic hemolytic anemia, thrombocytopenia, renal failure; consider concurrent antiphospholipid syndrome


===Key clinical signs suggesting SLE in an undiagnosed patient===
===Key clinical signs suggesting SLE in an undiagnosed patient===
*Malar (butterfly) rash — erythematous rash over cheeks/nasal bridge sparing nasolabial folds
*Malar (butterfly) rash — erythematous rash over cheeks/nasal bridge sparing nasolabial folds
*'''Photosensitivity'''
*Photosensitivity
*Oral/nasal ulcers (often painless)
*Oral/nasal ulcers (often painless)
*Arthritis/arthralgias (symmetric, non-erosive)
*Arthritis/arthralgias (symmetric, non-erosive)
*Serositis (pleuritis, pericarditis)
*Serositis (pleuritis, pericarditis)
*'''Alopecia'''
*Alopecia
*'''Raynaud phenomenon'''
*Raynaud phenomenon
*Cytopenias: leukopenia, lymphopenia, thrombocytopenia, hemolytic anemia (Coombs-positive)
*Cytopenias: leukopenia, lymphopenia, thrombocytopenia, hemolytic anemia (Coombs-positive)


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===Nephritic/nephrotic syndrome in a young patient===
===Nephritic/nephrotic syndrome in a young patient===
*Lupus nephritis (this page)
*Lupus nephritis (this page)
*IgA nephropathy — most common GN worldwide; synpharyngitic hematuria; '''normal complement'''
*IgA nephropathy — most common GN worldwide; synpharyngitic hematuria; normal complement
*Post-streptococcal GN — post-infectious latent period; low C3 (normalizes in 6-8 weeks)
*Post-streptococcal GN — post-infectious latent period; low C3 (normalizes in 6-8 weeks)
*ANCA-associated vasculitis (GPA, MPA) — ANCA positive; '''normal complement'''
*ANCA-associated vasculitis (GPA, MPA) — ANCA positive; normal complement
*Anti-GBM disease — anti-GBM antibodies; '''normal complement'''; may have pulmonary hemorrhage
*Anti-GBM disease — anti-GBM antibodies; normal complement; may have pulmonary hemorrhage
*MPGN / C3 glomerulopathy — persistently low C3
*MPGN / C3 glomerulopathy — persistently low C3
*[[Focal segmental glomerulosclerosis]] — nephrotic; biopsy diagnosis; normal complement
*[[Focal segmental glomerulosclerosis]] — nephrotic; biopsy diagnosis; normal complement
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===Lupus nephritis complement pattern===
===Lupus nephritis complement pattern===
*'''Low C3 AND low C4''' is characteristic of active lupus nephritis (classical pathway activation)
*Low C3 AND low C4 is characteristic of active lupus nephritis (classical pathway activation)
*Distinguishes from PSGN (low C3, usually normal or slightly low C4) and ANCA/anti-GBM disease (normal complement)
*Distinguishes from PSGN (low C3, usually normal or slightly low C4) and ANCA/anti-GBM disease (normal complement)


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===Renal biopsy===
===Renal biopsy===
*'''Gold standard''' for diagnosis and classification — determines ISN/RPS class, activity/chronicity indices, and guides treatment<ref name="PMC_LN">Understanding lupus nephritis: diagnosis, management, and treatment options. ''Int J Womens Health''. 2012;4:213-222. PMC3367406.</ref>
*Gold standard for diagnosis and classification — determines ISN/RPS class, activity/chronicity indices, and guides treatment<ref name="PMC_LN">Understanding lupus nephritis: diagnosis, management, and treatment options. ''Int J Womens Health''. 2012;4:213-222. PMC3367406.</ref>
*Not performed in the ED — arranged by nephrology
*Not performed in the ED — arranged by nephrology
*Indications: new-onset proteinuria (>500 mg/day), active urinary sediment, rising creatinine, suspected flare in known LN patient
*Indications: new-onset proteinuria (>500 mg/day), active urinary sediment, rising creatinine, suspected flare in known LN patient
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**Pulmonary edema: furosemide, oxygen, positive pressure ventilation
**Pulmonary edema: furosemide, oxygen, positive pressure ventilation
**Severe AKI: urgent dialysis if refractory hyperkalemia, acidosis, volume overload, or uremic symptoms
**Severe AKI: urgent dialysis if refractory hyperkalemia, acidosis, volume overload, or uremic symptoms
*'''Fluid and sodium restriction''' if edematous or volume-overloaded
*Fluid and sodium restriction if edematous or volume-overloaded
*Loop diuretics (furosemide) for edema and volume-mediated hypertension
*Loop diuretics (furosemide) for edema and volume-mediated hypertension
*Do NOT start immunosuppressive therapy in the ED — this requires biopsy-guided decision-making by nephrology/rheumatology
*Do NOT start immunosuppressive therapy in the ED — this requires biopsy-guided decision-making by nephrology/rheumatology
*Exception: if RPGN is strongly suspected (rapidly rising creatinine + active sediment), '''pulse IV methylprednisolone''' (500-1000 mg) may be initiated after nephrology telephone consultation while biopsy is arranged — time is critical for kidney survival
*Exception: if RPGN is strongly suspected (rapidly rising creatinine + active sediment), pulse IV methylprednisolone (500-1000 mg) may be initiated after nephrology telephone consultation while biopsy is arranged — time is critical for kidney survival


===Medication safety in the ED===
===Medication safety in the ED===
*Continue hydroxychloroquine — it should not be discontinued; it reduces flare risk and has renal-protective effects<ref name="StatPearls"/>
*Continue hydroxychloroquine — it should not be discontinued; it reduces flare risk and has renal-protective effects<ref name="StatPearls"/>
*'''Continue existing immunosuppressants''' unless the patient is septic (in which case, hold immunosuppression and consult rheumatology/nephrology)
*Continue existing immunosuppressants unless the patient is septic (in which case, hold immunosuppression and consult rheumatology/nephrology)
*Avoid NSAIDs — nephrotoxic; may worsen renal function and hypertension
*Avoid NSAIDs — nephrotoxic; may worsen renal function and hypertension
*Avoid nephrotoxic agents: aminoglycosides, IV contrast (if possible; discuss risk-benefit if imaging is critical)
*Avoid nephrotoxic agents: aminoglycosides, IV contrast (if possible; discuss risk-benefit if imaging is critical)
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**Induction: glucocorticoids + mycophenolate mofetil (first-line) OR IV cyclophosphamide (for severe/refractory disease)
**Induction: glucocorticoids + mycophenolate mofetil (first-line) OR IV cyclophosphamide (for severe/refractory disease)
**Pulse IV methylprednisolone (500-1000 mg daily for 3 days) followed by oral prednisone taper
**Pulse IV methylprednisolone (500-1000 mg daily for 3 days) followed by oral prednisone taper
**Maintenance: mycophenolate mofetil (superior to azathioprine) for '''at least 3 years'''
**Maintenance: mycophenolate mofetil (superior to azathioprine) for at least 3 years
*Class V (membranous): glucocorticoids + mycophenolate mofetil; ACE inhibitor/ARB
*Class V (membranous): glucocorticoids + mycophenolate mofetil; ACE inhibitor/ARB
*Class VI: renal replacement therapy (dialysis or transplant); immunosuppression not indicated
*Class VI: renal replacement therapy (dialysis or transplant); immunosuppression not indicated
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**New-onset lupus nephritis with significant proteinuria, active sediment, or elevated creatinine
**New-onset lupus nephritis with significant proteinuria, active sediment, or elevated creatinine
**Lupus nephritis flare with worsening renal function
**Lupus nephritis flare with worsening renal function
**RPGN or rapidly rising creatinine — '''urgent nephrology consultation'''
**RPGN or rapidly rising creatinine — urgent nephrology consultation
**Severe hypertension, hyperkalemia, pulmonary edema
**Severe hypertension, hyperkalemia, pulmonary edema
**Concurrent severe lupus flare involving other organs (cerebritis, pulmonary hemorrhage, severe cytopenias, serositis)
**Concurrent severe lupus flare involving other organs (cerebritis, pulmonary hemorrhage, severe cytopenias, serositis)
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*Discharge with close follow-up:
*Discharge with close follow-up:
**Known stable LN patient with mild abnormality on labs and no significant change from baseline
**Known stable LN patient with mild abnormality on labs and no significant change from baseline
**Ensure '''nephrology AND rheumatology follow-up within 48-72 hours'''
**Ensure nephrology AND rheumatology follow-up within 48-72 hours
**Emphasize medication compliance (especially hydroxychloroquine and immunosuppressants)
**Emphasize medication compliance (especially hydroxychloroquine and immunosuppressants)
*Counseling points:
*Counseling points:

Latest revision as of 09:36, 22 March 2026

Background

  • Lupus nephritis (LN) is renal involvement in Systemic lupus erythematosus, caused by deposition of immune complexes in the glomeruli, which activates complement and causes inflammation, scarring, and progressive kidney damage.[1]
  • It is clinically evident in 50-60% of SLE patients and is histologically present in the majority, even those without clinical signs of renal disease.[2]
  • Lupus nephritis is a major determinant of SLE prognosis — untreated proliferative disease (class III/IV) leads to end-stage kidney disease (ESKD) in a substantial proportion of patients.
  • The emergency physician encounters LN as new-onset nephritic or nephrotic syndrome in a patient with SLE features, acute renal failure during a lupus flare, or complications of immunosuppressive therapy (infection, cytopenias).
  • SLE predominantly affects women of childbearing age (female-to-male ratio 9:1); lupus nephritis typically presents at ages 20-40 years[2]
  • Higher incidence and more severe disease in African Americans, Hispanics, and Asians
  • Males with SLE have a higher rate of renal involvement and worse prognosis than females
  • Children with SLE have more frequent and more aggressive renal disease than adults
  • Lupus nephritis usually arises within the first 5 years of SLE diagnosis; may be the presenting manifestation of SLE
  • Delayed diagnostic biopsy >6 months is associated with a 9-fold increased risk of ESKD[3]

ISN/RPS Classification (determines treatment and prognosis)

Class Description Clinical significance
I Minimal mesangial Normal urinalysis; no treatment needed; excellent prognosis
II Mesangial proliferative Microscopic hematuria ± mild proteinuria; usually mild; glucocorticoids if needed
III Focal proliferative (<50% of glomeruli) Active nephritis; hematuria, proteinuria, rising creatinine; requires immunosuppression
IV Diffuse proliferative (≥50% of glomeruli) Most common and most severe; nephritic ± nephrotic features; highest risk of ESKD; aggressive immunosuppression required
V Membranous Nephrotic syndrome predominates; proteinuria may be massive; may overlap with III/IV
VI Advanced sclerotic (>90% sclerosed) ESKD; irreversible; renal replacement therapy; immunosuppression not helpful
  • Class IV is the most common biopsy finding and carries the worst untreated prognosis
  • Mixed classes (III/V or IV/V) have features of both proliferative and membranous disease
  • Class can transform — mild disease may progress to severe proliferative disease; repeat biopsy may be needed for flares

Mechanism

  • Anti-dsDNA and other autoantibodies form immune complexes → deposit in mesangium and glomerular capillary walls
  • Complement activation (classical pathway) → C3, C4 consumption → low serum C3 and C4
  • Inflammation → cellular proliferation, crescent formation, fibrinoid necrosis
  • Chronic inflammation → sclerosis and irreversible nephron loss

Clinical features

Presentations the EM physician will encounter

New-onset renal disease in a known SLE patient

  • Hematuria (gross or microscopic), proteinuria (detected on urinalysis)
  • Edema (periorbital, lower extremity, or generalized if nephrotic)
  • Hypertension (new or worsening)
  • Rising creatinine, decreased urine output
  • Often concurrent with other signs of lupus flare: fever, malar rash, arthritis, oral ulcers, pleurisy, pericarditis, cytopenias

SLE presenting with renal disease as the first manifestation

  • Young woman with unexplained nephritic or nephrotic syndrome
  • May have undiagnosed SLE — look for constitutional symptoms, rash, arthritis, photosensitivity, oral ulcers, alopecia, serositis
  • Any young woman with GN should be tested for SLE

Lupus nephritis flare

  • Known LN patient with worsening proteinuria, rising creatinine, new hematuria, or declining complement levels
  • May be triggered by medication noncompliance, infection, pregnancy, UV exposure
  • Rising anti-dsDNA + falling C3/C4 often precedes clinical flare by weeks

Rapidly progressive glomerulonephritis (RPGN)

  • Class IV with crescents — renal function deteriorates over days to weeks
  • Nephritic sediment + rapidly rising creatinine
  • Nephrology emergency — urgent biopsy and aggressive immunosuppression needed

Complications of immunosuppressive treatment

  • Infection: the most common cause of death in actively treated LN patients; opportunistic infections from cyclophosphamide, mycophenolate, rituximab, steroids
  • Cytopenias: from cyclophosphamide, mycophenolate, azathioprine; may present with neutropenic fever
  • Steroid side effects: hyperglycemia, psychosis, adrenal crisis on abrupt withdrawal, AVN of femoral head
  • Thrombotic microangiopathy (TMA): may occur in LN, especially with antiphospholipid antibodies — presents with microangiopathic hemolytic anemia, thrombocytopenia, renal failure; consider concurrent antiphospholipid syndrome

Key clinical signs suggesting SLE in an undiagnosed patient

  • Malar (butterfly) rash — erythematous rash over cheeks/nasal bridge sparing nasolabial folds
  • Photosensitivity
  • Oral/nasal ulcers (often painless)
  • Arthritis/arthralgias (symmetric, non-erosive)
  • Serositis (pleuritis, pericarditis)
  • Alopecia
  • Raynaud phenomenon
  • Cytopenias: leukopenia, lymphopenia, thrombocytopenia, hemolytic anemia (Coombs-positive)

Differential diagnosis

Nephritic/nephrotic syndrome in a young patient

  • Lupus nephritis (this page)
  • IgA nephropathy — most common GN worldwide; synpharyngitic hematuria; normal complement
  • Post-streptococcal GN — post-infectious latent period; low C3 (normalizes in 6-8 weeks)
  • ANCA-associated vasculitis (GPA, MPA) — ANCA positive; normal complement
  • Anti-GBM disease — anti-GBM antibodies; normal complement; may have pulmonary hemorrhage
  • MPGN / C3 glomerulopathy — persistently low C3
  • Focal segmental glomerulosclerosis — nephrotic; biopsy diagnosis; normal complement
  • Minimal change disease — nephrotic; steroid-responsive; normal complement
  • Membranous nephropathy — nephrotic; may be secondary to SLE, malignancy, hepatitis B
  • Thrombotic thrombocytopenic purpura (TTP) — MAHA, thrombocytopenia, AKI, fever, neurologic changes; can coexist with SLE
  • Antiphospholipid syndrome nephropathy — may occur with or without SLE; TMA pattern

Lupus nephritis complement pattern

  • Low C3 AND low C4 is characteristic of active lupus nephritis (classical pathway activation)
  • Distinguishes from PSGN (low C3, usually normal or slightly low C4) and ANCA/anti-GBM disease (normal complement)


Causes of Glomerulonephritis

Evaluation

ED workup

  • Urinalysis with microscopy: hematuria (dysmorphic RBCs, RBC casts), proteinuria, sterile pyuria
  • Spot urine protein:creatinine ratio: quantifies proteinuria; nephrotic range (>3.5) suggests class V or severe III/IV
  • BMP/CMP: creatinine (baseline and trending), BUN, potassium (hyperkalemia risk), bicarbonate
  • CBC: cytopenias (leukopenia, lymphopenia, thrombocytopenia, Coombs-positive hemolytic anemia — all support SLE diagnosis)
  • Albumin: low if nephrotic
  • Blood pressure: hypertension common in active disease

SLE serologic workup (initiate from ED)

Test Significance
ANA Sensitive screening test for SLE (>95% positive); not specific; negative ANA makes SLE very unlikely
Anti-dsDNA Highly specific for SLE; correlates with disease activity and renal involvement; rising titers predict flare
C3, C4 complement Low C3 AND low C4 = active lupus nephritis (classical pathway consumption); serial monitoring useful for tracking flare activity
Anti-Smith (anti-Sm) Highly specific for SLE (but less sensitive than anti-dsDNA)
Antiphospholipid antibodies (anticardiolipin, lupus anticoagulant, anti-β2-glycoprotein I) Identify concurrent antiphospholipid syndrome → increased thrombosis risk, TMA
ESR, CRP Often elevated; ESR tends to track disease activity in SLE (CRP may be normal unless infection or serositis is present)
  • Trend creatinine: compare to baseline; a rising creatinine with active sediment suggests active nephritis
  • Renal ultrasound: normal or enlarged kidneys in acute disease; small kidneys suggest chronic damage

Renal biopsy

  • Gold standard for diagnosis and classification — determines ISN/RPS class, activity/chronicity indices, and guides treatment[4]
  • Not performed in the ED — arranged by nephrology
  • Indications: new-onset proteinuria (>500 mg/day), active urinary sediment, rising creatinine, suspected flare in known LN patient
  • Biopsy results fundamentally change management — mild mesangial disease (class I/II) needs minimal treatment; diffuse proliferative disease (class IV) requires aggressive immunosuppression

Management

ED management of acute lupus nephritis/flare

  • Manage life-threatening complications first:
    • Hypertensive emergency: IV antihypertensives (nicardipine, labetalol); loop diuretics for volume overload (see Hypertensive emergency)
    • Hyperkalemia: standard protocols (see Hyperkalemia)
    • Pulmonary edema: furosemide, oxygen, positive pressure ventilation
    • Severe AKI: urgent dialysis if refractory hyperkalemia, acidosis, volume overload, or uremic symptoms
  • Fluid and sodium restriction if edematous or volume-overloaded
  • Loop diuretics (furosemide) for edema and volume-mediated hypertension
  • Do NOT start immunosuppressive therapy in the ED — this requires biopsy-guided decision-making by nephrology/rheumatology
  • Exception: if RPGN is strongly suspected (rapidly rising creatinine + active sediment), pulse IV methylprednisolone (500-1000 mg) may be initiated after nephrology telephone consultation while biopsy is arranged — time is critical for kidney survival

Medication safety in the ED

  • Continue hydroxychloroquine — it should not be discontinued; it reduces flare risk and has renal-protective effects[1]
  • Continue existing immunosuppressants unless the patient is septic (in which case, hold immunosuppression and consult rheumatology/nephrology)
  • Avoid NSAIDs — nephrotoxic; may worsen renal function and hypertension
  • Avoid nephrotoxic agents: aminoglycosides, IV contrast (if possible; discuss risk-benefit if imaging is critical)
  • ACE inhibitors/ARBs: standard chronic therapy for proteinuria reduction; may need to be held in acute AKI with hyperkalemia

Disease-specific treatment (nephrology/rheumatology-directed)

  • All classes: hydroxychloroquine (background therapy) + ACE inhibitor/ARB (for proteinuria >500 mg/day)
  • Class I/II: monitoring; glucocorticoids for flare; no immunosuppression usually needed
  • Class III/IV (and mixed III/V, IV/V):
    • Induction: glucocorticoids + mycophenolate mofetil (first-line) OR IV cyclophosphamide (for severe/refractory disease)
    • Pulse IV methylprednisolone (500-1000 mg daily for 3 days) followed by oral prednisone taper
    • Maintenance: mycophenolate mofetil (superior to azathioprine) for at least 3 years
  • Class V (membranous): glucocorticoids + mycophenolate mofetil; ACE inhibitor/ARB
  • Class VI: renal replacement therapy (dialysis or transplant); immunosuppression not indicated
  • Newer agents: belimumab (anti-BAFF; FDA-approved for LN as add-on therapy), voclosporin (calcineurin inhibitor; FDA-approved for LN), rituximab (B-cell depletion; used for refractory disease)

Disposition

  • Admit:
    • New-onset lupus nephritis with significant proteinuria, active sediment, or elevated creatinine
    • Lupus nephritis flare with worsening renal function
    • RPGN or rapidly rising creatinine — urgent nephrology consultation
    • Severe hypertension, hyperkalemia, pulmonary edema
    • Concurrent severe lupus flare involving other organs (cerebritis, pulmonary hemorrhage, severe cytopenias, serositis)
    • Infection in an immunosuppressed LN patient
  • Discharge with close follow-up:
    • Known stable LN patient with mild abnormality on labs and no significant change from baseline
    • Ensure nephrology AND rheumatology follow-up within 48-72 hours
    • Emphasize medication compliance (especially hydroxychloroquine and immunosuppressants)
  • Counseling points:
    • Never stop hydroxychloroquine without specialist guidance — discontinuation increases flare risk
    • Sun protection (UV exposure triggers SLE flares)
    • Report signs of flare: edema, decreased urine output, foamy/bloody urine, joint pain, rash, fever
    • Report signs of infection immediately (immunosuppressed patients)
    • Pregnancy planning: lupus nephritis has major implications for pregnancy; active disease should be in remission before conception; requires close coordination with maternal-fetal medicine, nephrology, and rheumatology

See Also

External Links

References

  1. 1.0 1.1 Lupus Nephritis. StatPearls.
    • NCBI. 2025.
  2. 2.0 2.1 Lupus Nephritis. Medscape. 2025.
  3. Ten tips in lupus nephritis management. Rheumatology. 2025. PMC11770280.
  4. Understanding lupus nephritis: diagnosis, management, and treatment options. Int J Womens Health. 2012;4:213-222. PMC3367406.
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