Henoch Schonlein Purpura (HSP)

I googled it and found this inforamtion at
http://en.wikipedia.org/wiki/Henoch-Sch%C3%B6nlein_purpura

Henoch-Schönlein purpura, also known as allergic purpura or anaphylactoid purpura and commonly abbreviated to HSP, is a systemic vasculitis (inflammation of blood vessels) characterized by deposition of immune complexes containing the antibody IgA in the skin and kidney. It occurs mainly in young children.

Typical symptoms include palpable purpura (small hemorrhages in the skin), joint pains and abdominal pain. Most cases are self-limiting and require no treatment apart from symptom control, but the disease may relapse in a third of the cases and cause irreversible kidney damage in about one in a hundred cases.[1] The exact cause of Henoch-Schönlein purpura is unknown, although it may occur after certain viral and bacterial infections, as well as an adverse drug reaction to some medications.

Contents [hide]
1 Signs and symptoms
1.1 Presentation
1.2 Kidney involvement
2 Diagnosis
3 Criteria
4 Pathophysiology
5 Treatment
6 Prognosis
6.1 Recovery and recurrence
6.2 Kidney involvement
7 Epidemiology
8 History
9 References

[edit] Signs and symptoms

[edit] Presentation

More severe case of HSP on child's foot, leg, and armPurpura, arthritis and abdominal pain are known as the classic triad of Henoch-Schönlein purpura.[2] 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 due to intussusception.[3] 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.[4] The joints involved tend to be the ankles, knees, and elbows but arthritis in the hands and feet is possible; the arthritis is non-erosive and hence causes no permanent deformity.[2] 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.[3] Problems in other organs, such as the central nervous system (brain and spinal cord) and lungs may occur, but much less commonly than the skin, bowel and kidneys.[1]

The disease tends to last about 4 weeks, and then resolves spontaneously.[1]

[edit] Kidney involvement
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.[1] 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.[1][5]

[edit] Diagnosis

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%[6]), 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.[2]

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 purpura, 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.[2]

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.[7]

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 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.[6]

[edit] Criteria
Multiple standards exist for defining Henoch-Schönlein purpura. These include the 1990 American College of Rheumatology (ACR) classification[8][9] and the 1994 Chapel Hill Consensus Conference (CHCC).[10] Some have reported the ACR criteria to be more sensitive than those of the CHCC.[11]

A more recent classification is the 2006 European League Against Rheumatism (EULAR) and Pediatric Rheumatology Society (PReS) classification. These 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 hematuria and/or proteinuria).[12]

[edit] Pathophysiology

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 (β-haemolytic, Lancefield group A), hepatitis B, herpes simplex virus, parvovirus B19, Coxsackievirus, adenovirus, Helicobacter pylori,[1] measles, mumps, rubella, mycoplasma and numerous others.[6] 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.[6]

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.[6] 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 region 1 and 2. Of the amino acids, half is proline, while the other ones 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, it appears that these sugar chains are deficient. The exact reason for these abnormalities is not known.[6][1]

[edit] Treatment
Pain killers may be needed for the abdominal pain and joint pains. It is uncertain as to whether HSP needs treatment beyond controlling the symptoms. Most patients do not receive therapy because of the high spontaneous recovery rate. Steroids are generally avoided.[1] However, if they are given early in the disease episode, the duration of symptoms may be shortened, and abdominal pain can improve significantly. Moreover, the chance of severe kidney problems is reduced.[13]

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 oral steroids to a combination of intravenous methylprednisolone (a potent 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.[6]

[edit] Prognosis

[edit] Recovery and recurrence
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).[14]

In children under ten, the condition recurs in about a third of all cases and usually within the first four months after the initial attack.[3] Recurrence is more common in older children and adults.[1]

Dear L.,

This may be an off the wall response and I'm not going to "give" you an answer but rather suggest you do some reading. I just finished reading a book called "Curing the Incurable" by Dr. Thomas Levy (get it from Amazon.) Read it and see if you don't find what is going on with your daughter in the book.

When people have odd things happening you need Columbo not a regular doctor. They don't have the time nor the talent to really figure out what is going on. Best if you figure it out yourself. The next letter had some good information but this stuck out "The exact cause of Henoch-Schönlein purpura is unknown, although it may occur after certain viral and bacterial infections, as well as an adverse drug reaction to some medications." All infections stress the body's stocks of Vitamin "C" because it is used up in fighting the infection. Sounds like your daughter is short of Vit "C". Give her lots of Vit C and read the book.

God Bless,

S.

My daughter had HSP when she was 5yr.old. We experienced the tiny, bruise-colored rash all over her, she could not walk to due joint pain, she vomitted excessively. I was scared to death! I did a lot of research on it (on my own) because the doctors didn't really seem to know a lot about it. The HSP did seem to come and go for quite a while. One day, she'd be fine, the next she'd be vomitting and achy. We went to the doctor regularly with our urine samples, etc..
Luckily, it did not affect her long-term. She is a thriving 11 yr.old now!!
Usually, in mild-cases, kids get over it in about 6 wks.
Had your daughter been vaccinated before the HSP?
You did say she had an infection, this could be the cause.
There's actually HSP support websites. Go to google.com and type in HSP.
I would reccomend no school, keeping her immune system built up as much as possible. Look in to the probiotics, natural remedies, etc..
You will get through this. It just seems to last forever when it's your child that's sick with some strange illness.
I'm thinking of you, take care and keep us filled in.
Let me know if I can be of help!

I had this when I was a child in the first grade. I remember my legs tingling constantly from this, like how they would feel after a day of roller skating. Back then, I had to spend a week in the hospital! It did spontaneously clear up with no lingering effects. But the urine samples and extra doctor visits did continue for quite awhile to make sure there was no lingering damage to the kidneys. Oatmeal baths and benadryl if the doctor allows. Extra hugs and kisses and extra rest.

Hi, I have a son that is 17 now,at age 2 ,he had a bowel intusseption, at 10 , he had mono and hives, at 16 he had cdiff and a purpura rash, he was put through 10,000 dollars worth of test and they found that he has hashimoto thyroid with goiter but also may have lupus someday, he has been tested since cdiff cleared but also antiphospholid test have cleared since cdiff cleared. I have taken him to every specialist under the sun and it boils down to if you have any kind of autoimmune problems you are prone to the body going goofy at anytime. Now, we work with an endocronoligist to keep the thyroid stable and take a multi vitamin, extra d and c and he has been symptom free now for over an year. He also had bleeding ulcers when the cdiff and urpura occured with anemia. Now we load up on yogurt , stoneyfield to keep the gut clear. Good Luck. D. p chicago
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http://www.medicinenet.com/henoch-schonlein_purpura/artic...

This site can tell you a lot more.

our daughter had that after repeated strep infections and tonsillitis. She was treated each time with antibiotics and then finally had a tonsillectomy. However the HSP continued and she got worse with the added symptom of abdominal pain and severe fatigue along with the purpura. At one time both legs were completely black like she had been beaten. we took her to a pediatric specialist and then ended up having to put her on steroids for several months after extensive testing. now she is fine. this happened when she was seven and now she is 35. At that time even the specialists did not know much about HSP. I continued to push to find the cause as our family doctor thought she was faking it. Even though I am a nurse, I had to really push to get her the medical care she needed. That is my message- be your child's medical advocate. M.