fbpx
Wikipedia

Henoch–Schönlein purpura

October 15, 2023

Henoch–Schönlein purpura (HSP), also known as IgA vasculitis, is a disease of the skin, mucous membranes, and sometimes other organs that most commonly affects children. In the skin, the disease causes palpable purpura (small, raised areas of bleeding underneath the skin), often with joint pain and abdominal pain. With kidney involvement, there may be a loss of small amounts of blood and protein in the urine (hematuria and proteinuria), but this usually goes unnoticed; in a small proportion of cases, the kidney involvement proceeds to chronic kidney disease. HSP is often preceded by an infection, such as a throat infection.

Henoch–Schönlein purpura
Other namesIgA vasculitis,[1] anaphylactoid purpura,[2] purpura rheumatica,[2] Schönlein–Henoch purpura[2]
Typical purpura on lower legs and buttocks
Pronunciation
SpecialtyRheumatology, Immunology

HSP is a systemic vasculitis (inflammation of blood vessels) and is characterized by deposition of immune complexes containing the antibody immunoglobulin A (IgA); the exact cause for this phenomenon is unknown. In children, it usually resolves within several weeks and requires no treatment apart from symptom control but may relapse in a third of cases and cause irreversible kidney damage in about one in a hundred cases. In adults, the prognosis is different from in children. The average duration of cutaneous lesions is 27.9 months.[3] For many, it tends to be relapsing–remitting over a long period of time, rather than self-limiting and there tend to be more complications.[4]

Signs and symptoms Edit

 
Typical purpura on lower leg
 
More severe case of HSP on child's foot, leg, and arm

Purpura, arthritis, and abdominal pain are known as the "classic triad" of Henoch–Schönlein purpura.[5] Purpura occur in all cases, joint pains and arthritis in 80%, and abdominal pain in 62%. Some include gastrointestinal hemorrhage as a fourth criterion; this occurs in 33% of cases, sometimes, but not necessarily always, due to intussusception.[6] The purpura typically appear on the legs and buttocks, but may also be seen on the arms, face and trunk. The abdominal pain is colicky in character, and may be accompanied by nausea, vomiting, constipation or diarrhea. There may be blood or mucus in the stools.[7] The joints involved tend to be the ankles, knees, and elbows, but arthritis in the hands and feet is possible; the arthritis is nonerosive and hence causes no permanent deformity.[5] Forty percent have evidence of kidney involvement, mainly in the form of hematuria (blood in the urine), but only a quarter will have this in sufficient quantities to be noticeable without laboratory tests.[6] Problems in other organs, such as the central nervous system (brain and spinal cord) and lungs may occur, but is much less common than in the skin, bowel and kidneys.[8]

Of the 40% of patients who develop kidney involvement, almost all have evidence (visible or on urinalysis) of blood in the urine. More than half also have proteinuria (protein in the urine), which in one eighth is severe enough to cause nephrotic syndrome (generalised swelling due to low protein content of the blood). While abnormalities on urinalysis may continue for a long time, only 1% of all HSP patients develop chronic kidney disease.[8] Hypertension (high blood pressure) may occur. Protein loss and high blood pressure, as well as the features on biopsy of the kidney if performed, may predict progression to advanced kidney disease. Adults are more likely than children to develop advanced kidney disease.[8][9]

Pathophysiology Edit

Henoch–Schönlein purpura is a small-vessel vasculitis in which complexes of immunoglobulin A (IgA) and complement component 3 (C3) are deposited on arterioles, capillaries, and venules (hence it is a type III hypersensitivity reaction). The activation of the alternative complement pathway results in the deposition of IgA aggregates or IgA complexes in target organs (with deposition of C3).[10] This leads to the production of inflammatory mediators, including vascular prostaglandins like prostacyclin, which may play a key role in the development of IgAV and its organ-specific clinical manifestations.[11] As with IgA nephropathy, serum levels of IgA are high in HSP and there are identical findings on renal biopsy; however, IgA nephropathy has a predilection for young adults while HSP is more predominant among children. Further, IgA nephropathy typically only affects the kidneys while HSP is a systemic disease. HSP involves the skin and connective tissues, scrotum, joints, gastrointestinal tract and kidneys.[12] The genetic basis remains unclear except for involvement of the human leukocyte antigen region of the genome.[13] It is hypothesized to involve autoimmunity triggered by infections. Streptococcus strains and Parainfluenza virus are the most commonly associated pathogens, and in children Human Parvovirus B19 is a frequent viral trigger[14]

Diagnosis Edit

 
Immunostaining showing IgA in the glomerulus of a patient with Henoch–Schönlein nephritis

The diagnosis is based on the combination of the symptoms, as very few other diseases cause the same symptoms together. Blood tests may show elevated creatinine and urea levels (in kidney involvement), raised IgA levels (in about 50%[12]), and raised C-reactive protein (CRP) or erythrocyte sedimentation rate (ESR) results; none are specific for Henoch–Schönlein purpura. The platelet count may be raised, and distinguishes it from diseases where low platelets are the cause of the purpura, such as idiopathic thrombocytopenic purpura and thrombotic thrombocytopenic purpura.[5]

If there is doubt about the cause of the skin lesions, a biopsy of the skin may be performed to distinguish the purpura from other diseases that cause it, such as vasculitis due to cryoglobulinemia; on microscopy, the appearances are of a hypersensitivity vasculitis, and immunofluorescence demonstrates IgA and C3 (a protein of the complement system) in the blood vessel wall.[5] However, overall serum complement levels are normal.

On the basis of symptoms, it is possible to distinguish HSP from hypersensitivity vasculitis (HV). In a series comparing 85 HSP patients with 93 HV patients, five symptoms were found to be indicative of HSP: palpable purpura, abdominal angina, digestive tract hemorrhage (not due to intussussception), hematuria and age less than 20. The presence of three or more of these indicators has an 87% sensitivity for predicting HSP.[15]

Biopsy of the kidney may be performed both to establish the diagnosis or to assess the severity of already suspected kidney disease. The main findings on kidney biopsy are increased cells and Ig deposition in the mesangium (part of the glomerulus, where blood is filtered), white blood cells, and the development of crescents. The changes are indistinguishable from those observed in IgA nephropathy.[12]

 
Microphotograph of a histological section of human skin prepared for direct immunofluorescence using an anti-IgA antibody, the skin is a biopsy of a patient with Henoch–Schönlein purpura. IgA deposits are found in the walls of small superficial capillaries (yellow arrows). The pale wavy green area on top is the epidermis, the bottom fibrous area is the dermis.

HSP can develop after infections with streptococci (β-haemolytic, Lancefield group A), hepatitis B, herpes simplex virus, parvovirus B19, Coxsackievirus, adenovirus, Helicobacter pylori,[8] measles, mumps, rubella, Mycoplasma and numerous others.[12] Drugs linked to HSP, usually as an idiosyncratic reaction, include the antibiotics vancomycin and cefuroxime, ACE inhibitors enalapril and captopril, anti-inflammatory agent diclofenac, as well as ranitidine and streptokinase. Several diseases have been reported to be associated with HSP, often without a causative link. Only in about 35% of cases can HSP be traced to any of these causes.[12]

The exact cause of HSP is unknown, but most of its features are due to the deposition of abnormal antibodies in the wall of blood vessels, leading to vasculitis. These antibodies are of the subclass IgA1 in polymers; it is uncertain whether the main cause is overproduction (in the digestive tract or the bone marrow) or decreased removal of abnormal IgA from the circulation.[12] It is suspected that abnormalities in the IgA1 molecule may provide an explanation for its abnormal behaviour in both HSP and the related condition IgA nephropathy. One of the characteristics of IgA1 (and IgD) is the presence of an 18 amino acid-long "hinge region" between complement-fixating regions 1 and 2. Of the amino acids, half is proline, while the others are mainly serine and threonine. The majority of the serines and the threonines have elaborate sugar chains, connected through oxygen atoms (O-glycosylation). This process is thought to stabilise the IgA molecule and make it less prone to proteolysis. The first sugar is always N-acetyl-galactosamine (GalNAc), followed by other galactoses and sialic acid. In HSP and IgAN, these sugar chains appear to be deficient. The exact reason for these abnormalities is not known.[8][12]

Classification Edit

Multiple standards exist for defining Henoch–Schönlein purpura, including the 1990 American College of Rheumatology (ACR) classification[16][17] and the 1994 Chapel Hill Consensus Conference (CHCC).[18] Some have reported the ACR criteria to be more sensitive than those of the CHCC.[19]

More recent classifications, the 2006 European League Against Rheumatism (EULAR) and Pediatric Rheumatology Society (PReS) classification, include palpable purpura as a mandatory criterion, together with at least one of the following findings: diffuse abdominal pain, predominant IgA deposition (confirmed on skin biopsy), acute arthritis in any joint, and renal involvement (as evidenced by the presence of blood and/or protein in the urine).[20]

Differential diagnosis Edit

Henoch–Schönlein purpura may present with an atypical manifestation, which can be confused with papular urticaria, systemic lupus erythematosus, meningococcemia, dermatitis herpetiformis, and acute hemorrhagic edema of infancy.[21]

Treatment Edit

As of 2017, the optimal way to treat Henoch–Schönlein purpura remains controversial.[22] Analgesics may be needed for the abdominal and joint pains. Wound care is warranted if skin death and ulcerations occur.[22] It is uncertain as to whether HSP needs treatment beyond controlling the symptoms. Most people do not receive therapy because of the high spontaneous recovery rate. Experts disagree on whether to routinely use corticosteroids as treatment for HSP.[22] However, if they are given early in the disease episode, the duration of symptoms may be shortened, and abdominal pain can improve significantly.[22] Moreover, the chance of severe kidney problems may be reduced.[23] A systematic review did not find any evidence that steroid treatment (prednisone) is effective at decreasing the likelihood of developing long-term kidney disease.[24]

Evidence of worsening kidney damage would normally prompt a kidney biopsy. Treatment may be indicated on the basis of the appearance of the biopsy sample; various treatments may be used, ranging from steroids by mouth to a combination of intravenous methylprednisolone (steroid), cyclophosphamide and dipyridamole followed by prednisone. Other regimens include steroids/azathioprine, and steroids/cyclophosphamide (with or without heparin and warfarin). Intravenous immunoglobulin (IVIG) is occasionally used.[12]

There is no good evidence that treating children who have HSP with antiplatelet agent prevents persistent kidney disease.[25] There is also no evidence that treating children or adults with cyclophosphamide prevents severe kidney disease.[25] Heparin treatment is not justified.[25]

Prognosis Edit

Overall prognosis is good in most patients, with one study showing recovery occurring in 94% and 89% of children and adults, respectively (some having needed treatment).[26] In children under ten, the condition recurs in about a third of all cases, usually within the four months of the initial attack.[6] Recurrence is more common in older children and adults.[8]

Kidney involvement Edit

In adults, kidney involvement progresses to end-stage kidney disease (ESKD) more often than in children. In a UK series of 37 patients, 10 (27%) developed advanced kidney disease. Proteinuria, hypertension at presentation, and pathology features (crescentic changes, interstitial fibrosis and tubular atrophy) predicted progression.[9] About 20% of children that exhibit nephrotic or nephritic features experience long permanent renal impairment.[27]

The findings on renal biopsy correlate with the severity of symptoms: those with asymptomatic hematuria may only have focal mesangial proliferation while those with proteinuria may have marked cellular proliferation or even crescent formation. The number of crescentic glomeruli is an important prognostic factor in determining whether the patient will develop chronic renal disease.[8]

In ESKD, some eventually need hemodialysis or equivalent renal replacement therapy (RRT). If a kidney transplant is found for a patient on RRT, the disease will recur in the graft (transplanted kidney) in about 35% of cases, and in 11%, the graft will fail completely (requiring resumption of the RRT and a further transplant).[12]

Epidemiology Edit

HSP occurs more often in children than in adults,[26] and usually follows an upper respiratory tract infection. Half of affected patients are below the age of six, and 90% are under ten. It occurs about twice as often in boys as in girls.[8] The incidence of HSP in children is about 20 per 100,000 children per year, making it the most common vasculitis in children.[28]

Cases of HSP may occur anytime throughout the year, but some studies have found that fewer cases occur during the summer months.[29]

History Edit

The disease is named after Eduard Heinrich Henoch (1820–1910), a German pediatrician (nephew of Moritz Heinrich Romberg) and his teacher Johann Lukas Schönlein (1793–1864), who described it in the 1860s. Schönlein associated the purpura and arthritis, and Henoch the purpura and gastrointestinal involvement. The English physician William Heberden (1710–1801) and the dermatologist Robert Willan (1757–1812) had already described the disease in 1802 and 1808, respectively, but the name Heberden–Willan disease has fallen into disuse. William Osler was the first to recognise the underlying allergic mechanism of HSP.[30]

See also Edit

References Edit

  1. ^ J. C. Jennette; R. J. Falk; P. A. Bacon; et al. (January 2013). "2012 Revised International Chapel Hill Consensus Conference Nomenclature of Vasculitides". Arthritis & Rheumatism. 65 (1): 1–11. doi:10.1002/art.37715. PMID 23045170.
  2. ^ a b c Rapini RP, Bolognia JL, Jorizzo JL (2007). Dermatology. St. Louis: Mosby. ISBN 978-1-4160-2999-1.
  3. ^ Sais G, Vidaller A, Jucglà A, Servitje O, Condom E, Peyri J (1998). "Prognostic factors in leukocytoclastic vasculitis: a clinicopathologic study of 160 patients". Arch Dermatol. 134 (3): 309–15. doi:10.1001/archderm.134.3.309. PMID 9521029.
  4. ^ "Treatment Challenges, Uncertainty Abound with IgA Vasculitis". The Rheumatologist. 2016.
  5. ^ a b c d Kraft DM, Mckee D, Scott C (1998). . American Family Physician. 58 (2): 405–8, 411. PMID 9713395. Archived from the original on 2011-06-06. Retrieved 2007-12-15.
  6. ^ a b c Saulsbury FT (1999). "Henoch–Schönlein purpura in children. Report of 100 patients and review of the literature". Medicine (Baltimore). 78 (6): 395–409. doi:10.1097/00005792-199911000-00005. PMID 10575422.
  7. ^ Fauci AS (1987). "269:The Vasculitis Syndromes". In Braunwald E, Isselbacher KJ, Petersdorf RG, Wilson JD, Martin JB, Fauci AS (eds.). Harrison's Book of Internal Medicine. Vol. 2 (11th ed.). McGraw Hill. p. 1441. ISBN 978-0-07-079454-2.
  8. ^ a b c d e f g h Saulsbury FT (2001). "Henoch–Schönlein purpura". Current Opinion in Rheumatology. 13 (1): 35–40. doi:10.1097/00002281-200101000-00006. PMID 11148713.
  9. ^ a b Shrestha S, Sumingan N, Tan J, et al. (2006). "Henoch Schönlein purpura with nephritis in adults: adverse prognostic indicators in a UK population". QJM. 99 (4): 253–65. doi:10.1093/qjmed/hcl034. PMID 16565522.
  10. ^ Song, Yan; Huang, Xiaohan; Yu, Guizhen; Qiao, Jianjun; Cheng, Jun; Wu, Jianyong; Chen, Jianghua (2021). "Pathogenesis of IgA Vasculitis: An Up-To-Date Review". Frontiers in Immunology. 12: 771619. doi:10.3389/fimmu.2021.771619. PMC 8630619. PMID 34858429.
  11. ^ Turi, S.; Belch, J. J.; Beattie, T. J.; Forbes, C. D. (1986). "Abnormalities of vascular prostaglandins in Henoch-Schonlein purpura". Archives of Disease in Childhood. 61 (2): 173–177. doi:10.1136/adc.61.2.173. PMC 1777583. PMID 2420289.
  12. ^ a b c d e f g h i Rai A, Nast C, Adler S (1 December 1999). "Henoch–Schönlein purpura nephritis". Journal of the American Society of Nephrology. 10 (12): 2637–44. doi:10.1681/ASN.V10122637. PMID 10589705.
  13. ^ López-Mejías, Raquel; Castañeda, Santos; Genre, Fernanda; Remuzgo-Martínez, Sara; Carmona, F. David; Llorca, Javier; Blanco, Ricardo; Martín, Javier; González-Gay, Miguel A. (March 2018). "Genetics of immunoglobulin-A vasculitis (Henoch–Schönlein purpura): An updated review". Autoimmunity Reviews. 17 (3): 301–315. doi:10.1016/j.autrev.2017.11.024. PMID 29353097.
  14. ^ Hetland, L.; Susrud, K.; Lindahl, K.; Bygum, A. (2017). "Henoch-Schönlein Purpura: A Literature Review". Acta Dermato Venereologica. 97 (10): 1160–1166. doi:10.2340/00015555-2733. PMID 28654132.
  15. ^ Michel BA, Hunder GG, Bloch DA, Calabrese LH (1992). "Hypersensitivity vasculitis and Henoch–Schönlein purpura: a comparison between the 2 disorders". Journal of Rheumatology. 19 (5): 721–8. PMID 1613701.
  16. ^ Mills JA, Michel BA, Bloch DA, et al. (1990). "The American College of Rheumatology 1990 criteria for the classification of Henoch–Schönlein purpura". Arthritis and Rheumatism. 33 (8): 1114–21. doi:10.1002/art.1780330809. PMID 2202310.
  17. ^ American College of Rheumatology. . Archived from the original on 2016-03-03. Retrieved 2007-12-15.
  18. ^ Jennette JC, Falk RJ, Andrassy K, et al. (1994). "Nomenclature of systemic vasculitides. Proposal of an international consensus conference". Arthritis and Rheumatism. 37 (2): 187–92. doi:10.1002/art.1780370206. PMID 8129773.
  19. ^ Murali NS, George R, John GT, et al. (2002). "Problems of classification of Henoch Schonlein purpura: an Indian perspective". Clinical and Experimental Dermatology. 27 (4): 260–3. doi:10.1046/j.1365-2230.2002.01063.x. PMID 12139664. S2CID 45849349.
  20. ^ Ozen S, Ruperto N, Dillon MJ, et al. (July 2006). "EULAR/PReS endorsed consensus criteria* for the classification of childhood vasculitides". Annals of the Rheumatic Diseases. 65 (7): 936–41. doi:10.1136/ard.2005.046300. PMC 1798210. PMID 16322081.
  21. ^ Lawee D (2008). "Atypical clinical course of Henoch–Schonlein purpura". Can Fam Physician (Review. Case Reports.). 54 (8): 1117–20. PMC 2515239. PMID 18697972.
  22. ^ a b c d Hetland, LE; Susrud, KS; Lindahl, KH; Bygum, A (November 2017). "Henoch–Schönlein Purpura: A Literature Review". Acta Dermato-Venereologica (Review). 97 (10): 1160–66. doi:10.2340/00015555-2733. PMID 28654132.
  23. ^ Weiss PF, Feinstein JA, Luan X, Burnham JM, Feudtner C (2007). "Effects of corticosteroid on Henoch–Schönlein purpura: a systematic review". Pediatrics. 120 (5): 1079–87. doi:10.1542/peds.2007-0667. PMC 3525094. PMID 17974746.
  24. ^ Hahn, Deirdre; Hodson, Elisabeth M.; Craig, Jonathan C. (2023-02-28). "Interventions for preventing and treating kidney disease in IgA vasculitis". The Cochrane Database of Systematic Reviews. 2023 (2): CD005128. doi:10.1002/14651858.CD005128.pub4. ISSN 1469-493X. PMC 9972777. PMID 36853224.
  25. ^ a b c Hahn, Deirdre; Hodson, Elisabeth M.; Willis, Narelle S.; Craig, Jonathan C. (2015-08-07). "Interventions for preventing and treating kidney disease in Henoch–Schönlein purpura (HSP)". The Cochrane Database of Systematic Reviews. 2015 (8): CD005128. doi:10.1002/14651858.CD005128.pub3. ISSN 1469-493X. PMC 9588174. PMID 26258874.
  26. ^ a b Blanco R, Martínez-Taboada VM, Rodríguez-Valverde V, García-Fuentes M, González-Gay MA (1997). "Henoch–Schönlein purpura in adulthood and childhood: two different expressions of the same syndrome". Arthritis and Rheumatism. 40 (5): 859–64. doi:10.1002/art.1780400513. PMID 9153547.
  27. ^ Watson, L; Richardson, AR; Holt, RC; Jones, CA; Beresford, MW (January 2012). "Henoch schonlein purpura--a 5-year review and proposed pathway". PLOS ONE. 7 (1): e29512. Bibcode:2012PLoSO...729512W. doi:10.1371/journal.pone.0029512. PMC 3250434. PMID 22235302.
  28. ^ Gardner-Medwin JM, Dolezalova P, Cummins C, Southwood TR (2002). "Incidence of Henoch–Schönlein purpura, Kawasaki disease, and rare vasculitides in children of different ethnic origins". Lancet. 360 (9341): 1197–202. doi:10.1016/S0140-6736(02)11279-7. PMID 12401245. S2CID 25018798.
  29. ^ Saulsbury FT (2002). . Cleveland Clinic Journal of Medicine. 69 (Suppl 2): SII87–9. doi:10.3949/ccjm.69.suppl_2.sii87. PMID 12086273. Archived from the original on 2020-03-27. Retrieved 2012-08-26.
  30. ^ Schönlein-Henoch purpura at Who Named It?

External links Edit

 
Wikimedia Commons has media related to Henoch–Schönlein purpura.

October 15, 2023
henoch, schönlein, purpura, also, known, vasculitis, disease, skin, mucous, membranes, sometimes, other, organs, that, most, commonly, affects, children, skin, disease, causes, palpable, purpura, small, raised, areas, bleeding, underneath, skin, often, with, j. Henoch Schonlein purpura HSP also known as IgA vasculitis is a disease of the skin mucous membranes and sometimes other organs that most commonly affects children In the skin the disease causes palpable purpura small raised areas of bleeding underneath the skin often with joint pain and abdominal pain With kidney involvement there may be a loss of small amounts of blood and protein in the urine hematuria and proteinuria but this usually goes unnoticed in a small proportion of cases the kidney involvement proceeds to chronic kidney disease HSP is often preceded by an infection such as a throat infection Henoch Schonlein purpuraOther namesIgA vasculitis 1 anaphylactoid purpura 2 purpura rheumatica 2 Schonlein Henoch purpura 2 Typical purpura on lower legs and buttocksPronunciation ˈ h ɛ n e k ˈ ʃ ɜː n l aɪ n ˈ ʃ oʊ n SpecialtyRheumatology ImmunologyHSP is a systemic vasculitis inflammation of blood vessels and is characterized by deposition of immune complexes containing the antibody immunoglobulin A IgA the exact cause for this phenomenon is unknown In children it usually resolves within several weeks and requires no treatment apart from symptom control but may relapse in a third of cases and cause irreversible kidney damage in about one in a hundred cases In adults the prognosis is different from in children The average duration of cutaneous lesions is 27 9 months 3 For many it tends to be relapsing remitting over a long period of time rather than self limiting and there tend to be more complications 4 Contents 1 Signs and symptoms 2 Pathophysiology 3 Diagnosis 3 1 Classification 3 2 Differential diagnosis 4 Treatment 5 Prognosis 5 1 Kidney involvement 6 Epidemiology 7 History 8 See also 9 References 10 External linksSigns and symptoms Edit nbsp Typical purpura on lower leg nbsp More severe case of HSP on child s foot leg and armPurpura arthritis and abdominal pain are known as the classic triad of Henoch Schonlein purpura 5 Purpura occur in all cases joint pains and arthritis in 80 and abdominal pain in 62 Some include gastrointestinal hemorrhage as a fourth criterion this occurs in 33 of cases sometimes but not necessarily always due to intussusception 6 The purpura typically appear on the legs and buttocks but may also be seen on the arms face and trunk The abdominal pain is colicky in character and may be accompanied by nausea vomiting constipation or diarrhea There may be blood or mucus in the stools 7 The joints involved tend to be the ankles knees and elbows but arthritis in the hands and feet is possible the arthritis is nonerosive and hence causes no permanent deformity 5 Forty percent have evidence of kidney involvement mainly in the form of hematuria blood in the urine but only a quarter will have this in sufficient quantities to be noticeable without laboratory tests 6 Problems in other organs such as the central nervous system brain and spinal cord and lungs may occur but is much less common than in the skin bowel and kidneys 8 Of the 40 of patients who develop kidney involvement almost all have evidence visible or on urinalysis of blood in the urine More than half also have proteinuria protein in the urine which in one eighth is severe enough to cause nephrotic syndrome generalised swelling due to low protein content of the blood While abnormalities on urinalysis may continue for a long time only 1 of all HSP patients develop chronic kidney disease 8 Hypertension high blood pressure may occur Protein loss and high blood pressure as well as the features on biopsy of the kidney if performed may predict progression to advanced kidney disease Adults are more likely than children to develop advanced kidney disease 8 9 Pathophysiology EditHenoch Schonlein purpura is a small vessel vasculitis in which complexes of immunoglobulin A IgA and complement component 3 C3 are deposited on arterioles capillaries and venules hence it is a type III hypersensitivity reaction The activation of the alternative complement pathway results in the deposition of IgA aggregates or IgA complexes in target organs with deposition of C3 10 This leads to the production of inflammatory mediators including vascular prostaglandins like prostacyclin which may play a key role in the development of IgAV and its organ specific clinical manifestations 11 As with IgA nephropathy serum levels of IgA are high in HSP and there are identical findings on renal biopsy however IgA nephropathy has a predilection for young adults while HSP is more predominant among children Further IgA nephropathy typically only affects the kidneys while HSP is a systemic disease HSP involves the skin and connective tissues scrotum joints gastrointestinal tract and kidneys 12 The genetic basis remains unclear except for involvement of the human leukocyte antigen region of the genome 13 It is hypothesized to involve autoimmunity triggered by infections Streptococcus strains and Parainfluenza virus are the most commonly associated pathogens and in children Human Parvovirus B19 is a frequent viral trigger 14 Diagnosis Edit nbsp Immunostaining showing IgA in the glomerulus of a patient with Henoch Schonlein nephritisThe diagnosis is based on the combination of the symptoms as very few other diseases cause the same symptoms together Blood tests may show elevated creatinine and urea levels in kidney involvement raised IgA levels in about 50 12 and raised C reactive protein CRP or erythrocyte sedimentation rate ESR results none are specific for Henoch Schonlein purpura The platelet count may be raised and distinguishes it from diseases where low platelets are the cause of the purpura such as idiopathic thrombocytopenic purpura and thrombotic thrombocytopenic purpura 5 If there is doubt about the cause of the skin lesions a biopsy of the skin may be performed to distinguish the purpura from other diseases that cause it such as vasculitis due to cryoglobulinemia on microscopy the appearances are of a hypersensitivity vasculitis and immunofluorescence demonstrates IgA and C3 a protein of the complement system in the blood vessel wall 5 However overall serum complement levels are normal On the basis of symptoms it is possible to distinguish HSP from hypersensitivity vasculitis HV In a series comparing 85 HSP patients with 93 HV patients five symptoms were found to be indicative of HSP palpable purpura abdominal angina digestive tract hemorrhage not due to intussussception hematuria and age less than 20 The presence of three or more of these indicators has an 87 sensitivity for predicting HSP 15 Biopsy of the kidney may be performed both to establish the diagnosis or to assess the severity of already suspected kidney disease The main findings on kidney biopsy are increased cells and Ig deposition in the mesangium part of the glomerulus where blood is filtered white blood cells and the development of crescents The changes are indistinguishable from those observed in IgA nephropathy 12 nbsp Microphotograph of a histological section of human skin prepared for direct immunofluorescence using an anti IgA antibody the skin is a biopsy of a patient with Henoch Schonlein purpura IgA deposits are found in the walls of small superficial capillaries yellow arrows The pale wavy green area on top is the epidermis the bottom fibrous area is the dermis HSP can develop after infections with streptococci b haemolytic Lancefield group A hepatitis B herpes simplex virus parvovirus B19 Coxsackievirus adenovirus Helicobacter pylori 8 measles mumps rubella Mycoplasma and numerous others 12 Drugs linked to HSP usually as an idiosyncratic reaction include the antibiotics vancomycin and cefuroxime ACE inhibitors enalapril and captopril anti inflammatory agent diclofenac as well as ranitidine and streptokinase Several diseases have been reported to be associated with HSP often without a causative link Only in about 35 of cases can HSP be traced to any of these causes 12 The exact cause of HSP is unknown but most of its features are due to the deposition of abnormal antibodies in the wall of blood vessels leading to vasculitis These antibodies are of the subclass IgA1 in polymers it is uncertain whether the main cause is overproduction in the digestive tract or the bone marrow or decreased removal of abnormal IgA from the circulation 12 It is suspected that abnormalities in the IgA1 molecule may provide an explanation for its abnormal behaviour in both HSP and the related condition IgA nephropathy One of the characteristics of IgA1 and IgD is the presence of an 18 amino acid long hinge region between complement fixating regions 1 and 2 Of the amino acids half is proline while the others are mainly serine and threonine The majority of the serines and the threonines have elaborate sugar chains connected through oxygen atoms O glycosylation This process is thought to stabilise the IgA molecule and make it less prone to proteolysis The first sugar is always N acetyl galactosamine GalNAc followed by other galactoses and sialic acid In HSP and IgAN these sugar chains appear to be deficient The exact reason for these abnormalities is not known 8 12 Classification Edit Multiple standards exist for defining Henoch Schonlein purpura including the 1990 American College of Rheumatology ACR classification 16 17 and the 1994 Chapel Hill Consensus Conference CHCC 18 Some have reported the ACR criteria to be more sensitive than those of the CHCC 19 More recent classifications the 2006 European League Against Rheumatism EULAR and Pediatric Rheumatology Society PReS classification include palpable purpura as a mandatory criterion together with at least one of the following findings diffuse abdominal pain predominant IgA deposition confirmed on skin biopsy acute arthritis in any joint and renal involvement as evidenced by the presence of blood and or protein in the urine 20 Differential diagnosis Edit Henoch Schonlein purpura may present with an atypical manifestation which can be confused with papular urticaria systemic lupus erythematosus meningococcemia dermatitis herpetiformis and acute hemorrhagic edema of infancy 21 Treatment EditAs of 2017 the optimal way to treat Henoch Schonlein purpura remains controversial 22 Analgesics may be needed for the abdominal and joint pains Wound care is warranted if skin death and ulcerations occur 22 It is uncertain as to whether HSP needs treatment beyond controlling the symptoms Most people do not receive therapy because of the high spontaneous recovery rate Experts disagree on whether to routinely use corticosteroids as treatment for HSP 22 However if they are given early in the disease episode the duration of symptoms may be shortened and abdominal pain can improve significantly 22 Moreover the chance of severe kidney problems may be reduced 23 A systematic review did not find any evidence that steroid treatment prednisone is effective at decreasing the likelihood of developing long term kidney disease 24 Evidence of worsening kidney damage would normally prompt a kidney biopsy Treatment may be indicated on the basis of the appearance of the biopsy sample various treatments may be used ranging from steroids by mouth to a combination of intravenous methylprednisolone steroid cyclophosphamide and dipyridamole followed by prednisone Other regimens include steroids azathioprine and steroids cyclophosphamide with or without heparin and warfarin Intravenous immunoglobulin IVIG is occasionally used 12 There is no good evidence that treating children who have HSP with antiplatelet agent prevents persistent kidney disease 25 There is also no evidence that treating children or adults with cyclophosphamide prevents severe kidney disease 25 Heparin treatment is not justified 25 Prognosis EditOverall prognosis is good in most patients with one study showing recovery occurring in 94 and 89 of children and adults respectively some having needed treatment 26 In children under ten the condition recurs in about a third of all cases usually within the four months of the initial attack 6 Recurrence is more common in older children and adults 8 Kidney involvement Edit In adults kidney involvement progresses to end stage kidney disease ESKD more often than in children In a UK series of 37 patients 10 27 developed advanced kidney disease Proteinuria hypertension at presentation and pathology features crescentic changes interstitial fibrosis and tubular atrophy predicted progression 9 About 20 of children that exhibit nephrotic or nephritic features experience long permanent renal impairment 27 The findings on renal biopsy correlate with the severity of symptoms those with asymptomatic hematuria may only have focal mesangial proliferation while those with proteinuria may have marked cellular proliferation or even crescent formation The number of crescentic glomeruli is an important prognostic factor in determining whether the patient will develop chronic renal disease 8 In ESKD some eventually need hemodialysis or equivalent renal replacement therapy RRT If a kidney transplant is found for a patient on RRT the disease will recur in the graft transplanted kidney in about 35 of cases and in 11 the graft will fail completely requiring resumption of the RRT and a further transplant 12 Epidemiology EditHSP occurs more often in children than in adults 26 and usually follows an upper respiratory tract infection Half of affected patients are below the age of six and 90 are under ten It occurs about twice as often in boys as in girls 8 The incidence of HSP in children is about 20 per 100 000 children per year making it the most common vasculitis in children 28 Cases of HSP may occur anytime throughout the year but some studies have found that fewer cases occur during the summer months 29 History EditThe disease is named after Eduard Heinrich Henoch 1820 1910 a German pediatrician nephew of Moritz Heinrich Romberg and his teacher Johann Lukas Schonlein 1793 1864 who described it in the 1860s Schonlein associated the purpura and arthritis and Henoch the purpura and gastrointestinal involvement The English physician William Heberden 1710 1801 and the dermatologist Robert Willan 1757 1812 had already described the disease in 1802 and 1808 respectively but the name Heberden Willan disease has fallen into disuse William Osler was the first to recognise the underlying allergic mechanism of HSP 30 See also EditCutaneous small vessel vasculitisReferences Edit J C Jennette R J Falk P A Bacon et al January 2013 2012 Revised International Chapel Hill Consensus Conference Nomenclature of Vasculitides Arthritis amp Rheumatism 65 1 1 11 doi 10 1002 art 37715 PMID 23045170 a b c Rapini RP Bolognia JL Jorizzo JL 2007 Dermatology St Louis Mosby ISBN 978 1 4160 2999 1 Sais G Vidaller A Jucgla A Servitje O Condom E Peyri J 1998 Prognostic factors in leukocytoclastic vasculitis a clinicopathologic study of 160 patients Arch Dermatol 134 3 309 15 doi 10 1001 archderm 134 3 309 PMID 9521029 Treatment Challenges Uncertainty Abound with IgA Vasculitis The Rheumatologist 2016 a b c d Kraft DM Mckee D Scott C 1998 Henoch Schonlein purpura a review American Family Physician 58 2 405 8 411 PMID 9713395 Archived from the original on 2011 06 06 Retrieved 2007 12 15 a b c Saulsbury FT 1999 Henoch Schonlein purpura in children Report of 100 patients and review of the literature Medicine Baltimore 78 6 395 409 doi 10 1097 00005792 199911000 00005 PMID 10575422 Fauci AS 1987 269 The Vasculitis Syndromes In Braunwald E Isselbacher KJ Petersdorf RG Wilson JD Martin JB Fauci AS eds Harrison s Book of Internal Medicine Vol 2 11th ed McGraw Hill p 1441 ISBN 978 0 07 079454 2 a b c d e f g h Saulsbury FT 2001 Henoch Schonlein purpura Current Opinion in Rheumatology 13 1 35 40 doi 10 1097 00002281 200101000 00006 PMID 11148713 a b Shrestha S Sumingan N Tan J et al 2006 Henoch Schonlein purpura with nephritis in adults adverse prognostic indicators in a UK population QJM 99 4 253 65 doi 10 1093 qjmed hcl034 PMID 16565522 Song Yan Huang Xiaohan Yu Guizhen Qiao Jianjun Cheng Jun Wu Jianyong Chen Jianghua 2021 Pathogenesis of IgA Vasculitis An Up To Date Review Frontiers in Immunology 12 771619 doi 10 3389 fimmu 2021 771619 PMC 8630619 PMID 34858429 Turi S Belch J J Beattie T J Forbes C D 1986 Abnormalities of vascular prostaglandins in Henoch Schonlein purpura Archives of Disease in Childhood 61 2 173 177 doi 10 1136 adc 61 2 173 PMC 1777583 PMID 2420289 a b c d e f g h i Rai A Nast C Adler S 1 December 1999 Henoch Schonlein purpura nephritis Journal of the American Society of Nephrology 10 12 2637 44 doi 10 1681 ASN V10122637 PMID 10589705 Lopez Mejias Raquel Castaneda Santos Genre Fernanda Remuzgo Martinez Sara Carmona F David Llorca Javier Blanco Ricardo Martin Javier Gonzalez Gay Miguel A March 2018 Genetics of immunoglobulin A vasculitis Henoch Schonlein purpura An updated review Autoimmunity Reviews 17 3 301 315 doi 10 1016 j autrev 2017 11 024 PMID 29353097 Hetland L Susrud K Lindahl K Bygum A 2017 Henoch Schonlein Purpura A Literature Review Acta Dermato Venereologica 97 10 1160 1166 doi 10 2340 00015555 2733 PMID 28654132 Michel BA Hunder GG Bloch DA Calabrese LH 1992 Hypersensitivity vasculitis and Henoch Schonlein purpura a comparison between the 2 disorders Journal of Rheumatology 19 5 721 8 PMID 1613701 Mills JA Michel BA Bloch DA et al 1990 The American College of Rheumatology 1990 criteria for the classification of Henoch Schonlein purpura Arthritis and Rheumatism 33 8 1114 21 doi 10 1002 art 1780330809 PMID 2202310 American College of Rheumatology 1990 criteria for the classification of Henoch Schonlein purpura Archived from the original on 2016 03 03 Retrieved 2007 12 15 Jennette JC Falk RJ Andrassy K et al 1994 Nomenclature of systemic vasculitides Proposal of an international consensus conference Arthritis and Rheumatism 37 2 187 92 doi 10 1002 art 1780370206 PMID 8129773 Murali NS George R John GT et al 2002 Problems of classification of Henoch Schonlein purpura an Indian perspective Clinical and Experimental Dermatology 27 4 260 3 doi 10 1046 j 1365 2230 2002 01063 x PMID 12139664 S2CID 45849349 Ozen S Ruperto N Dillon MJ et al July 2006 EULAR PReS endorsed consensus criteria for the classification of childhood vasculitides Annals of the Rheumatic Diseases 65 7 936 41 doi 10 1136 ard 2005 046300 PMC 1798210 PMID 16322081 Lawee D 2008 Atypical clinical course of Henoch Schonlein purpura Can Fam Physician Review Case Reports 54 8 1117 20 PMC 2515239 PMID 18697972 a b c d Hetland LE Susrud KS Lindahl KH Bygum A November 2017 Henoch Schonlein Purpura A Literature Review Acta Dermato Venereologica Review 97 10 1160 66 doi 10 2340 00015555 2733 PMID 28654132 Weiss PF Feinstein JA Luan X Burnham JM Feudtner C 2007 Effects of corticosteroid on Henoch Schonlein purpura a systematic review Pediatrics 120 5 1079 87 doi 10 1542 peds 2007 0667 PMC 3525094 PMID 17974746 Hahn Deirdre Hodson Elisabeth M Craig Jonathan C 2023 02 28 Interventions for preventing and treating kidney disease in IgA vasculitis The Cochrane Database of Systematic Reviews 2023 2 CD005128 doi 10 1002 14651858 CD005128 pub4 ISSN 1469 493X PMC 9972777 PMID 36853224 a b c Hahn Deirdre Hodson Elisabeth M Willis Narelle S Craig Jonathan C 2015 08 07 Interventions for preventing and treating kidney disease in Henoch Schonlein purpura HSP The Cochrane Database of Systematic Reviews 2015 8 CD005128 doi 10 1002 14651858 CD005128 pub3 ISSN 1469 493X PMC 9588174 PMID 26258874 a b Blanco R Martinez Taboada VM Rodriguez Valverde V Garcia Fuentes M Gonzalez Gay MA 1997 Henoch Schonlein purpura in adulthood and childhood two different expressions of the same syndrome Arthritis and Rheumatism 40 5 859 64 doi 10 1002 art 1780400513 PMID 9153547 Watson L Richardson AR Holt RC Jones CA Beresford MW January 2012 Henoch schonlein purpura a 5 year review and proposed pathway PLOS ONE 7 1 e29512 Bibcode 2012PLoSO 729512W doi 10 1371 journal pone 0029512 PMC 3250434 PMID 22235302 Gardner Medwin JM Dolezalova P Cummins C Southwood TR 2002 Incidence of Henoch Schonlein purpura Kawasaki disease and rare vasculitides in children of different ethnic origins Lancet 360 9341 1197 202 doi 10 1016 S0140 6736 02 11279 7 PMID 12401245 S2CID 25018798 Saulsbury FT 2002 Epidemiology of Henoch Schonlein purpura Cleveland Clinic Journal of Medicine 69 Suppl 2 SII87 9 doi 10 3949 ccjm 69 suppl 2 sii87 PMID 12086273 Archived from the original on 2020 03 27 Retrieved 2012 08 26 Schonlein Henoch purpura at Who Named It External links Edit nbsp Wikimedia Commons has media related to Henoch Schonlein purpura Retrieved from https en wikipedia org w index php title Henoch Schonlein purpura amp oldid 1170066029, wikipedia, wiki, book, books, library,

article

, read, download, free, free download, mp3, video, mp4, 3gp, jpg, jpeg, gif, png, picture, music, song, movie, book, game, games.