Goodpasture's syndrome

Goodpasture's syndrome
Classification and external resources
ICD-10	M31.0 (ILDS M31.010)
ICD-9	446.21
OMIM	233450
DiseasesDB	5363
eMedicine	med/923 ped/888
MeSH	D019867

Goodpasture’s syndrome (also known as Goodpasture’s disease and anti-glomerular basement antibody disease) is a rare disease characterized by glomerulonephritis and hemorrhaging of the lungs.^[1] Although many diseases can present with these symptoms, the name Goodpasture’s syndrome is usually reserved for the autoimmune disease triggered when the patient’s immune system attacks Goodpasture antigen (a type II hypersensitivity reaction^[2]), which is found in the kidney and lung, and in time, causing damage to these organs. The disease bears the name of the American pathologist Dr. Ernest Goodpasture of Vanderbilt University, whose 1919 description is regarded as the first report on the existence of the condition.^[3][4]

The GBM antigen responsible for this disease is a component of the non-collagenous domain (NC1) of the alpha-3 chain of collagen type IV.

Contents [hide] 1 Signs and symptoms 1.1 Lung disease 1.2 Kidney disease 2 Diagnosis 3 Possible causes 4 Pathophysiology 5 Treatment 6 Epidemiology 7 Prognosis 8 See also 9 References 10 External links

[edit] Signs and symptoms

Goodpasture’s syndrome can cause people to cough up blood or feel a burning sensation when urinating. But its first signs may be vague, such as fatigue, nausea, difficulty breathing, or skin pallor. These signs are followed by kidney involvement, represented first by small amounts of blood in the urine, protein in the urine, and other clinical and laboratory findings.^[5]

Other patients present with both lung and kidney disease; however, some patients present with one of these diseases alone. The first lung symptoms usually develop days to months before kidney damage is evident.

[edit] Lung disease

Lung symptoms may present as nothing more serious than a dry cough and minor breathlessness; and such mild symptoms may last for many years before more severe ones develop. At its most serious, however, lung damage may cause severe impairment of oxygenation so that intensive care is required. Deterioration between the two extremes may occur very rapidly, often at the same time as rapid deterioration occurs in the kidney. The patient often does not seek medical attention until he or she begins coughing up blood (hemoptysis). The patient may be anemic due to loss of blood through lung hemorrhaging over a long period. In Goodpasture’s syndrome, unlike many other conditions that cause similar symptoms, lung hemorrhaging most often occurs in smokers and those with damage from lung infection or exposure to fumes.

[edit] Kidney disease

The kidney portion of the disease mostly affects the glomeruli causing a form of nephritis. It is usually not detected until a rapid advance of the disease occurs and kidney function can be completely lost in a matter of days, a condition known as rapidly progressive (Crescentic) glomerulonephritis, or RPGN. Blood spills into the urine causing hematuria, the volume of urine output decreases and urea and other products usually excreted by the kidney are retained and build up in the blood. This is acute renal failure. Renal failure does not cause symptoms until more than 80% of kidney function has been lost. Symptoms include loss of appetite and malaise at first and then, when the damage is more advanced, breathlessness, high blood pressure and edema (swelling caused by fluid retention). The kidney involvement usually presents as nephritic syndrome, i.e. hematuria, a reduced glomerular filtration rate, and high blood pressure. This is in contrast to nephrotic syndrome, a rarer outcome of Goodpasture's, characterized by an abnormally large amount of protein in the urine (proteinuria), coupled with severe edema.

[edit] Diagnosis

Because of the vagueness of early symptoms and rapid progression of the disease, diagnosis is often not reached until very late in the course of the disease. A Kidney biopsy (linear IgG deposits along basement membrane) is often the fastest way to secure the diagnosis and gain information about the extent of the disease and likely effect of treatment. Tests for anti-GBM antibodies may also be useful, combined with tests for antibodies to neutrophil cytoplasmic antigens, which are also directed against the patient’s own proteins.

[edit] Possible causes

Viral infections, especially influenza, and kidney surgery are generally regarded as proven causes.

Other possible causes include the presence of an inherited component and exposure to certain chemicals, including hydrocarbon solvents and the weed killer Paraquat.^[5]

[edit] Pathophysiology

As with many autoimmune conditions, the precise cause of Goodpasture’s Syndrome is not yet known. It is believed to be a type II hypersensitivity reaction to Goodpasture’s antigens on the basement membrane of the glomerulus of the kidneys and the pulmonary alveolus, specifically the non-collagenous domain of the alpha-3 chain of Type IV collagen. The immune system wrongly recognizes these motifs as foreign and produces antibodies (IgG) toward them, eliciting an immune response.

Renal failure is due to anti-glomerular basement membrane (anti-GBM).

[edit] Treatment

Like many autoimmune diseases, Goodpasture’s syndrome responds well to treatment with corticosteroids and immunosuppressants. These drugs dampen the body's normal immune response and the patient may become more susceptible to infections. The concentration of anti-GBM antibodies in the blood may be reduced by apheresis to remove blood plasma and replace a portion of the plasma with an isotonic salt and protein solution. This course of treatment usually lasts between three and six months.

Unfortunately, none of these treatments can reverse permanent kidney damage and for patients who have suffered from the syndrome, renal transplant may be needed once the disease has subsided.

[edit] Epidemiology

Goodpasture’s syndrome is rare. In European populations, the incidence is between 1 in 1,000,000 and 1 in 2,000,000. It is less likely to be found in non-European populations. While cases have occurred in patients between the ages of 4 and 80, it is most common between ages 18 and 30 and again between 50 and 65. Unlike many other autoimmune diseases, males are surprisingly six times more affected than females.

[edit] Prognosis

In the 1970s, Goodpasture’s syndrome was most often fatal, but due to advances in diagnosis and treatment, deaths are less common now. Death from lung hemorrhage may occur before the diagnosis has been made, or in the initial stages of treatment before it has been properly controlled. With treatment, however, the patient can usually recover completely from lung damage. Kidneys, on the other hand, are less able to repair themselves and patients with kidney damage must often resort to a life on dialysis or kidney transplantation. Even with the best management there is still significant mortality from renal failure, particularly if the patient is otherwise in poor health. It must also be remembered that the immunosuppressive treatment many patients are treated with increases their risk of infection with a number of serious or fatal secondary diseases.

[edit] See also

• HLA-DR#DR2
• Pulmonary-renal syndrome

[edit] References

[edit] External links

• GBM antibodies: immunofluorescence image

[show]v · d · eVasculitis/arteritis: systemic vasculitis (M30–M31, 446) Large vessel Takayasu's arteritis · Giant cell arteritis Medium vessel Type III hypersensitivity (Polyarteritis nodosa) · Kawasaki disease Small vessel Pauci-immune c-ANCA (Wegener's granulomatosis) · p-ANCA (Churg-Strauss syndrome, Microscopic polyangiitis) Type III hypersensitivity Hypersensitivity vasculitis/Henoch–Schönlein purpura Ungrouped Acute hemorrhagic edema of infancy · Bullous small vessel vasculitis · Cutaneous small-vessel vasculitis Other Goodpasture's syndrome · Sneddon's syndrome M: VAS anat(a:h/u/t/a/l,v:h/u/t/a/l)/phys/devp/cell/prot noco/syva/cong/lyvd/tumr, sysi/epon, injr proc, drug(C2s+n/3/4/5/7/8/9)

[show]v · d · eImmune disorders: hypersensitivity and autoimmune diseases (279.5–6) Type I/allergy/atopy (IgE) Foreign Atopic dermatitis · Allergic urticaria · Hay fever · Allergic asthma · Anaphylaxis · Food allergy (Milk, Egg, Peanut, Tree nut, Seafood, Soy, Wheat), Penicillin allergy Autoimmune none Type II/ADCC (IgM, IgG) Foreign Pernicious anemia · Hemolytic disease of the newborn Autoimmune Cytotoxic Autoimmune hemolytic anemia · Idiopathic thrombocytopenic purpura  · Bullous pemphigoid  · Pemphigus vulgaris · Rheumatic fever · Goodpasture's syndrome "Type 5"/receptor Graves' disease · Myasthenia gravis Type III (Immune complex) Foreign Henoch–Schönlein purpura · Hypersensitivity vasculitis · Reactive arthritis · Rheumatoid arthritis · Farmer's lung · Post-streptococcal glomerulonephritis · Serum sickness · Arthus reaction Autoimmune Systemic lupus erythematosus · Subacute bacterial endocarditis Type IV/cell-mediated (T-cells) Foreign Allergic contact dermatitis · Mantoux test Autoimmune Diabetes mellitus type 1 · Hashimoto's thyroiditis · Guillain–Barré syndrome  · Multiple sclerosis  · Coeliac disease · Giant cell arteritis GVHD Transfusion-associated graft versus host disease Unknown/ multiple Foreign Hypersensitivity pneumonitis (Allergic bronchopulmonary aspergillosis) · Transplant rejection · Latex allergy (I+IV) Autoimmune Sjögren's syndrome · Autoimmune hepatitis · Autoimmune polyendocrine syndrome (APS1, APS2) · Autoimmune adrenalitis · Systemic autoimmune disease M: LMC cell/phys/auag/auab/comp, igrc imdf/ipig/hyps/tumr proc, drug(L3/4)

[show]v · d · eGenetic disorder, extracellular: scleroprotein disease (excluding laminin and keratin) Collagen disease COL1: Osteogenesis imperfecta · Ehlers–Danlos syndrome, types 1, 2, 7 COL2: Hypochondrogenesis · Achondrogenesis type 2 · Stickler syndrome · Marshall syndrome · Spondyloepiphyseal dysplasia congenita · Spondyloepimetaphyseal dysplasia, Strudwick type · Kniest dysplasia (see also C2/11) COL3: Ehlers–Danlos syndrome, types 3 & 4 (Sack–Barabas syndrome) COL4: Alport syndrome COL5: Ehlers–Danlos syndrome, types 1 & 2 COL6: Bethlem myopathy · Ullrich congenital muscular dystrophy COL7: Epidermolysis bullosa dystrophica · Recessive dystrophic epidermolysis bullosa · Bart syndrome · Transient bullous dermolysis of the newborn COL8: Fuchs' dystrophy 1 COL9: Multiple epiphyseal dysplasia 2, 3, 6 COL10: Schmid metaphyseal chondrodysplasia COL11: Weissenbacher–Zweymüller syndrome · Otospondylomegaepiphyseal dysplasia (see also C2/11) COL17: Bullous pemphigoid Laminin Junctional epidermolysis bullosa · Laryngoonychocutaneous syndrome Other Congenital stromal corneal dystrophy · Raine syndrome · Urbach–Wiethe disease · TECTA (DFNA8/12, DFNB21) see also fibrous proteins B structural (perx, skel, cili, mito, nucl, sclr) · DNA/RNA/protein synthesis (drep, trfc, tscr, tltn) · membrane (icha, slcr, atpa, abct, othr) · transduction (iter, csrc, itra), trfk

[show]v · d · eUrinary 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) M: URI anat/phys/devp/cell noco/acba/cong/tumr, sysi/epon, urte proc/itvp, drug (G4B), blte, urte