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Glomerulonephritis Information

Glomerulonephritis, also known as glomerular nephritis, abbreviated GN, is a renal disease (usually of both kidneys) characterized by inflammation of the glomeruli, or small blood vessels in the kidneys.[1] It may present with isolated hematuria and/or proteinuria (blood or protein in the urine); or as a nephrotic syndrome, a nephritic syndrome, acute renal failure, or chronic renal failure. They are categorised into several different pathological patterns, which are broadly grouped into non-proliferative or proliferative types. Diagnosing the pattern of GN is important because the outcome and treatment differs in different types. Primary causes are ones which are intrinsic to the kidney, whilst secondary causes are associated with certain infections (bacterial, viral or parasitic pathogens), drugs, systemic disorders (SLE, vasculitis) or diabetes.

Contents

Thin Basement Membrane Disease

Thin basement membrane disease is an autosomal dominant inherited disease characterized by thin glomerular basement membranes on electron microscopy. It is a benign condition that causes persistent microscopic hematuria.

Non Proliferative

This is characterised by the numbers of cells (lack of hypercellularity) in the glomeruli. They usually cause nephrotic syndrome. This includes the following types:

Minimal change GN (also known as Minimal Change Disease)

This form of GN causes 79.4% of nephrotic syndrome in children, but only 20% in adults. As the name indicates, there are no changes visible on simple light microscopy, but on electron microscopy there is fusion of podocytes (supportive cells in the glomerulus). Immunohistochemistry staining is negative. Treatment consists of supportive care for the massive fluid accumulation in the patients body (= oedema) and as well as steroids to halt the disease process (typically Prednisone 1 mg/kg). Over 90% of children respond well to steroids, being essentially cured after 3 months of treatment. Adults have a lower response rate (80%). Failure to respond to steroids ('steroid resistant') or return of the disease when steroids are stopped ('steroid dependent') may require cytotoxic therapy (such as cyclosporin) which is associated with many side-effects.

Focal Segmental Glomerulosclerosis (FSGS)

FSGS may be primary or secondary to reflux nephropathy, Alport syndrome, heroin abuse or HIV. FSGS presents as a nephrotic syndrome with varying degrees of impaired renal function (seen as a rising serum creatinine, hypertension). As the name suggests, only certain foci of glomeruli within the kidney are affected, and then only a segment of an individual glomerulus. The pathological lesion is sclerosis (fibrosis) within the glomerulus and hyalinisation of the feeding arterioles, but no increase in the number of cells (hence non-proliferative). The hyaline is an amorphous material, pink, homogeneous, resulting from combination of plasma proteins, increased mesangial matrix and collagen. Staining for antibodies and complement is essentially negative. Steroids are often tried but not shown to be effective. 50% of people with FSGS continue to have progressive deterioration of kidney function, ending in renal failure.

Membranous glomerulonephritis

Membranous glomerulonephritis (MGN), a relatively common type of glomerulonephritis in adults, frequently produces a mixed nephrotic and nephritic picture. Its cause is usually unknown, but may be associated with cancers of the lung and bowel, infection such as hepatitis and malaria, drugs including penicillamine, and connective tissue diseases such as systemic lupus erythematosus. Individuals with cerebral shunts are at risk of developing shunt nephritis, which frequently produces MGN.

Microscopically, MGN is characterized by a thickened glomerular basement membrane without a hypercellular glomerulus. Immunofluorescence demonstrates diffuse granular uptake of IgG. The basement membrane may completely surround the granular deposits, forming a "spike and dome" pattern. Tubules also display the symptoms of a typical Type III hypersensitivity reaction, which causes the endothelial cells to proliferate, which can be seen under a light microscope with a PAS stain.[2][3]

Prognosis follows the rule of thirds: one-third remain with MGN indefinitely, one-third remit, and one-third progress to end-stage renal failure. As the glomerulonephritis progresses, the tubules of the kidney become infected, leading to atrophy and hyalinisation. The kidney appears to shrink. Treatment with corticosteroids is attempted if the disease progresses.

In extremely rare cases, the disease has been known to run in families, usually passed down through the females. This condition, similarly, is called Familial Membranous Glomerulonephritis. There have only been about nine documented cases in the world.

Proliferative

This type is characterised by increased number of cells in the glomerulus (hypercellular). Usually present as a nephritic syndrome and usually progress to end-stage renal failure (ESRF) over weeks to years (depending on type).

IgA nephropathy (Berger's disease)

[4]

General Information

IgA nephropathy is the most common type of glomerulonephritis in adults worldwide. It usually presents as macroscopic haematuria (visibly bloody urine). It occasionally presents as a nephrotic syndrome. It often affects young males within days (24-48hrs) after an upper respiratory tract or gastrointestinal infection. Microscopic examination of biopsy specimens shows increased number of mesangial cells with increased matrix (the 'cement' which holds everything together). Immuno-staining is positive for immunoglobulin A deposits within the matrix. Prognosis is variable, 20% progress to ESRF. ACE inhibitors are the mainstay of treatment.

Summary

This is a form of GN characterised by IgA deposits in the mesangeial regions and immunocytochemistry is required for definitive diagnosis of the disease.

Presentation

  1. Recurrent gross or microscopic hematuria
  • gross hematuria occurs post-infection of the respiratory (more common), gastrointestinal, or urinary tract
  1. mild proteinuria
  2. occasionally nephrotic syndrome (although it usually has a nephritic presentation)
  3. rarely, presents with crescentic Rapidly progressive GN

Causes

The disease can be primary or secondary to liver and intestinal diseases. It also overlaps with Henoch-Schonlein purpura, a systemic renal disease in children in which similar IgA deposits occur.

Pathology

plasma polymeric IgA is increased in IgA Nephropathy, and circulating IgA-containing immune complexes can be found in the blood of some patients. Plasma IgA is usually monomeric and polymeric plasma IgA is broken down in the liver. IgA is normally found in mucus.

There are two forms of IgA and only IgA1 causes nephrogenicity.

Histology

Characteristic finding:

  1. IgA deposition in the mesangium seen by immunofloresence
  2. Electron dense deposits in electron microscopy
  3. Absence of early complement components

May find:

  1. normal glomeruli
  2. mesangioproliferative GN
  3. focal proliferative GN (healing may cause focal segmental sclerosis)
  4. overt cresentic glomerulonephritis
  5. leukocytes in glomerular capillaries

Post-infectious

Post-infectious glomerulonephritis can occur after essentially any infection, but classically occurs after infection with Streptococcus pyogenes. It typically occurs 10–14 days after a skin or pharyngeal infection with this bacterium.

Patients present with signs and symptoms of glomerulonephritis. Diagnosis is made based on these findings in an individual with a history of recent streptococcal infection. Streptococcal titers in the blood (antistreptolysin O titers) may support the diagnosis.

Light microscopy demonstrates diffuse endocapillary hypercellularity due to proliferation of endothelial and mesangial cells, as well as an influx of neutrophils and monocytes. The Bowman space is compressed, in some cases to the extent that this produces a crescent formation characteristic of crescentic glomerulonephritis.

Biopsy is seldom done as the disease usually regresses without complications. Treatment is supportive, and the disease generally resolves in 2–4 weeks.

Membranoproliferative/mesangiocapillary GN

This may be primary, or secondary to SLE, viral hepatitis, or hypocomplementemia. One sees 'hypercellular and hyperlobular' glomeruli due to proliferation of both cells and the matrix within the mesangium. Usually presents with a combined nephritic-nephrotic picture, with inevitable progression to end stage renal failure. The primary form consists of two types:

In both types, the basement membrane may develop a 'tram-track' appearance, due to duplication and splitting.

Rapidly progressive glomerulonephritis

Crescentic glomerulonephritis induced by infective endocarditis on PAS staining and immunofluorescence. PAS staining (left) demonstrated circumferential and cellular crescent formation with interstitial nephritis. Immunofluorescence (right) demonstrated C3 positive staining in mesangial area. Photomicrograph of renal biopsy showing crescent formation and tuft narrowing. Periodic acid silver methenamine stain.

Rapidly progressive glomerulonephritis (Crescentic GN) has a poor prognosis, with rapid progression to kidney failure over weeks. Steroid therapy is sometimes used.[5] Any of the above types of GN can be rapidly progressive. Additionally two further causes present as solely RPGN.

Histopathology: The majority of glomeruli present "crescents". Formation of crescents is initiated by passage of fibrin into the Bowman space as a result of increased permeability of glomerular basement membrane. Fibrin stimulates the proliferation of parietal cells of Bowman capsule, and an influx of monocytes. Rapid growing and fibrosis of crescents compresses the capillary loops and decreases the Bowman space which leads to renal failure within weeks or months.

See also

References

  1. ^ "glomerulonephritis" at Dorland's Medical Dictionary
  2. ^ Dr. Zaid G. Nguyen MD. University of Melbourne, Dept of Medicine
  3. ^ http://www.nlm.nih.gov/medlineplus/ency/article/000472.htm
  4. ^ Robbin's Pathology
  5. ^ Couser WG (May 1999). "Glomerulonephritis". Lancet 353 (9163): 1509–15. doi:10.1016/S0140-6736(98)06195-9. PMID 10232333. http://linkinghub.elsevier.com/retrieve/pii/S0140-6736(98)06195-9.
· · Urinary system · Pathology · Urologic disease / Uropathy (N00–N39, 580–599)
Abdominal
Nephropathy/ (nephritis+ nephrosis)
Glomerulopathy/ glomerulitis/ (glomerulonephritis+ glomerulonephrosis)
Primarily nephrotic
Non-proliferative .0 Minimal change · .1 Focal segmental · .2 Membranous
Proliferative .3 Mesangial proliferative · .4 Endocapillary proliferative .5/.6 Membranoproliferative/mesangiocapillary
By condition Diabetic · Amyloidosis
Primarily nephritic, .7 RPG
Type I RPG/Type II hypersensitivity Goodpasture's syndrome
Type II RPG/Type III hypersensitivity Post-streptococcal · Lupus (DPN) · IgA/Berger's
Type III RPG/Pauci-immune Wegener's granulomatosis · Microscopic polyangiitis
Tubulopathy/ tubulitis
Proximal RTA (RTA 2) · Fanconi syndrome
Thick ascending Bartter syndrome
Distal convoluted Gitelman syndrome
Collecting duct Liddle's syndrome · RTA (RTA 1) · Diabetes insipidus (Nephrogenic)
Renal papilla Renal papillary necrosis
Major calyx/pelvis Hydronephrosis · Pyonephrosis · Reflux nephropathy
Any/all Acute tubular necrosis
Interstitium Interstitial nephritis (Pyelonephritis, Danubian endemic familial nephropathy)
Any/all
General syndromes Renal failure (Acute renal failure, Chronic renal failure) · Uremic pericarditis · Uremia
Vascular Renal artery stenosis · Renal Ischemia · Hypertensive nephropathy · Renovascular hypertension
Other Analgesic nephropathy · Renal osteodystrophy · Nephroptosis · Abderhalden-Kaufmann-Lignac syndrome
Ureter Ureteritis · Ureterocele · Megaureter
Pelvic
Bladder Cystitis (Interstitial cystitis, Hunner's ulcer, Trigonitis, Hemorrhagic cystitis) · Neurogenic bladder · Bladder sphincter dyssynergia · Vesicointestinal fistula · Vesicoureteral reflux
Urethra Urethritis (Non-gonococcal urethritis) · Urethral syndrome · Urethral stricture/Meatal stenosis · Urethral caruncle
Any/all Obstructive uropathy · Urinary tract infection · Retroperitoneal fibrosis · Urolithiasis (Bladder stone, Kidney stone, Renal colic) · Malacoplakia · Urinary incontinence (Stress, Urge, Overflow)

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