Education & Research

As we have stated on our home page that Thrombocytopenia is life-threatening condition that can possibly go undetected or dormant in your system without you being aware of its existence. To learn more about this condition please visit the websites below at the bottom of this page.

Abstract:
Thrombotic thrombocytopenia purpura (TTP) is a rare, life-threatening disease with an incidence of approximately 2 persons per million per year. It is characterized by severe deficiency of the von Willebrand cleaving protease, ADAMTS13 (a disintegrin and metalloproteinase with a thrombospondin type 1 motif, member 13), leading to formation of platelet-rich thrombi in the microvasculature. Prompt initiation of appropriate therapy, particularly plasma exchange, may be life-saving. Diagnosis of TTP is challenging because of its diverse clinical manifestations, overlap in clinical presentation with other thrombotic microangiopathies, and limited availability of ADAMTS13 testing. Clinical prediction scores have been developed to estimate the pretest probability of severe ADAMTS13 deficiency and may be used as an adjunct to clinical judgment to guide initial management decisions. An ADAMTS13 activity level of less than 10% supports the diagnosis of TTP in appropriate clinical contexts, but many centers do not offer testing in-house and must send out the test to a reference laboratory with a turnaround time of several days. In such instances, initial management decisions must be made without the benefit of laboratory testing. In patients with TTP, inhibitor tests may be useful for distinguishing immune-mediated from congenital TTP. In this article, we review the epidemiology, natural history, and clinical presentation of TTP and laboratory assays for TTP including ADAMTS13 activity and inhibitor assays. We also describe an evidence-based approach to the evaluation of a patient with suspected TTP that integrates clinical and laboratory assessment.
 
Introduction:

Thrombotic thrombocytopenia purpura (TTP) is a rare form of thrombotic microangiopathy (TMA) characterized by microangiopathic hemolytic anemia (MAHA), severe thrombocytopenia, and ischemic end-organ damage resulting from formation of platelet-rich thrombi in the microvasculature. TTP is distinguished from other TMAs by severe deficiency of ADAMTS13 (a disintegrin and metalloproteinase with a thrombospondin type 1 motif, member 13), a plasma protein that cleaves von Willebrand factor (VWF) multimers. Without the proteolytic activity of ADAMTS13, the uncleaved ultralarge VWF multimers accumulate and induce excessive platelet adhesion and aggregation, leading to formation of disseminated microthrombosis and the clinical features of TTP. In patients with congenital TTP (cTTP), severe ADAMTS13 deficiency results from biallelic mutations in the ADAMTS13 gene, whereas immune-mediated TTP (iTTP) is associated with anti-ADAMTS13 autoantibodies, which neutralize or induce clearance of the ADAMTS13 protein.

Despite its rarity, timely recognition of TTP is critical, as emergent initiation of therapeutic plasma exchange (PEX) may be life-saving. Diagnosis of TTP is nonetheless challenging. The spectrum of clinical presentation can be remarkably variable, from subtle nonspecific symptoms to major neurological abnormalities. Distinction of TTP from other TMA syndromes is not always readily discernible because of the overlapping clinical manifestations of TTP with other TMAs. Measurement of ADAMTS13 activity is an important means of confirming the diagnosis, but results may not be available rapidly enough to guide initial management decisions. It is therefore incumbent on the clinician to identify patients most likely to benefit from plasma exchange based on immediately available data. In this article, we review recent evidence on the epidemiology, natural history, and clinical manifestations of TTP as well as the utility of ADAMTS13 laboratory testing, and we suggest an evidence-based approach to the diagnosis of TTP that integrates clinical and laboratory information.

Epidemiology and Natural History of TTP

The estimated incidence of TTP is 2 per million per year. National and regional registries have provided important insights on the demographic and clinical features of this rare disease.

iTTP occurs far more commonly in adulthood, with a median age at onset around the fourth decade of life. Women were more likely to be affected across all studies, with a female to male ratio of 2 to 3:1. Blacks have a sevenfold higher incidence than nonblacks. TTP presenting in infancy strongly favors diagnosis of the congenital form. In the French registry, however, genetic mutations in ADAMTS13 were identified in approximately 3% of patients with adult-onset TTP (first episode of TTP at age ≥18 years). Interestingly, all such cases occurred in association with a first pregnancy. Thus, all women who present with a first episode of TTP during pregnancy should be evaluated for the hereditary form of the disease.

iTTP may occur in isolation (ie, primary TTP) or in association with a predisposing condition (ie, secondary TTP). Predisposing conditions include other autoimmune diseases (eg, systemic lupus erythematosus), malignancy, infection (eg, HIV), pregnancy, and certain drugs. Predisposing conditions have been identified in 27% to 69% of patients with TMA and severe ADAMTS13 deficiency., A breakdown of various predisposing conditions as a proportion of all cases of TTP is illustrated in Figure 1. A focused history, physical examination, and laboratory evaluation to exclude these conditions should be undertaken in all patients presenting with TTP. In the French registry, platelet count lower than 20 × 109/L, a positive anti-ADAMTS13 antibody titer, and the presence of gastrointestinal symptoms were predictive of primary TTP, whereas severe anemia (hemoglobin < 7 g/dL) and presence of fever were associated with secondary TTP. In the United Kingdom TTP Registry, neurological involvement was more common and more severe in primary TTP, with a greater percentage of cases presenting with stroke and coma. 

The introduction of plasma exchange dramatically reduced mortality associated with TTP, but the disease remains fatal in 5% to 16% of cases (Table 1). Compared with other TMAs, patients with TTP have a more favorable prognosis, including shorter hospitalization, more rapid platelet count recovery, and higher overall survival.

Among patients with TTP, approximately 95% achieve normalization of the platelet count with acute treatment and 87% ultimately achieve remission. However, exacerbation (a fall in platelet count requiring resumption of plasma exchange within 30 days) and relapse (recurrent TTP after 30 days) remain frequent clinical problems, occurring in 53% and 30% to 50% of patients, respectively.

Compared with initial episodes, relapses tend to be less severe (eg, less severe anemia and thrombocytopenia, less frequent cardiac and neurological involvement, lower lactate dehydrogenase),,, likely because of earlier recognition on the part of the patient and clinician. Relapsed patients also require fewer plasma exchange treatments. However, there were no differences with respect to response, exacerbation, and mortality rates between relapse and initial episodes.

 
 

Thrombotic Thrombocytopenic Purpura is a rare blood disorder that is considered a true medical emergency. TTP is diagnosed at a rate of 3-4 in 1 million people per year. Potentially fatal complications can result from internal blood
clotting, with damage to critical organs such as the brain and heart.
Due to a deficiency in the ADAMTS13 enzyme, blood becomes “sticky” and forms clots in blood vessels throughout the body. These clots are made up of platelets, one of the elements in blood. Vital blood flow to the body’s organs is restricted, placing the organs at risk for damage due to a lack of oxygen and nutrients from the blood. Moreover, since platelets are being used to form numerous unnecessary blood clots, their availability to perform their normal function, which is to seal injury sites to prevent excess bleeding, is compromised.

TYPES OF TTP
Hereditary TTP (hTTP)
1% of TTP cases are due to an inherited deficiency or abnormality of the ADAMTS 13 enzyme.
Immune-mediated TTP (iTTP)
99% of TTP cases have no defined cause. In all cases, there is a decreased level of the ADAMTS 13 enzyme as a result of antibodies attacking the enzyme.
SYMPTOMS
• fatigue
• fever
• bleeding (from nose, gums)
• diarrhea
• chest pain
• abdominal pain
• neurologic symptoms (confusion, headaches, visual changes)
• thrombocytopenia (bruising, purpura, petechiae)
 
DIAGNOSIS
A medical history and a physical exam, in combination with a complete blood count (CBC), lactate dehydrogenase level (LDH) and blood smear are used to determine a diagnosis of TTP. More recently an ADAMTS 13 enzyme level test may be used to help confirm the diagnosis. Importantly, diagnosis and immediate treatment should not await the results of an ADAMTS 13 assay.
TREATMENT
Hereditary TTP (hTTP)
Monthly prophylactic plasma is sometimes administered to patients to replenish and maintain adequate levels of functioning ADAMTS 13, the enzyme which the patient is unable to produce themselves.Immune-mediated TTP (iTTP)
Most patients receive steroids, e.g. prednisone, to slow the immune system and therefore the progression of this autoimmune disorder. The side effects of steroids can be challenging.
In all cases of iTTP, plasma exchange is the basic treatment of choice. Plasma exchange involves the use of automated machinery which permits the removal of the patient’s plasma and replacement with donor plasma during a 3 to 4 hour treatment. Plasma exchange both removes antibodies and replenishes normal plasma proteins. To treat iTTP, a series of daily or every other day plasma exchanges is used. Rituximab is increasingly used to achieve and maintain remission.
Other medications and/or removal of the spleen are used when patients fail to achieve remission from first line therapy.
PROGNOSIS
Without treatment, 95% of patients succumb to the disease; however, with treatment 80 – 90% of iTTP patients achieve remission. Of these, about 30% will relapse. Early detection of such a flare of the disease is critical to minimize the risk of death or irreversible injury to vital organs.
Pregnancy may be a trigger for women with both hTTP and iTTP. Women considering pregnancy should discuss their individual case with their TTP specialist. Research is showing an ADAMTS 13 assay to be helpful in evaluating the risk of relapse during pregnancy, and in suggesting a risk mitigating prophylaxis treatment. The mortality of thrombotic thrombocytopenic purpura is 90%. Early treatment (with plasma exchange and corticosteroids) decreases the mortality to 15%. The longer the patient waits for treatment, the more likely they are to have adverse outcomes. Early suspicion of the disease followed by administrations of plasma exchange/corticosteroids significantly reduces mortality. The primary cause of demise can occur with coronary thrombosis leading to an acute myocardial infarction, congestive heart failure, and sudden death.
 
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