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2020 ISTH TTP Pocket Guideline with GPS

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Issue link: https://eguideline.guidelinecentral.com/i/1314283

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15 Statement 16 ➤ We did not systematically search and review the evidence on cyclophosphamide for TTP patients. Patients with refractory TTP unresponsive to standard treatments may be considered for other immunosuppressive treatments with scant supporting evidence, including cyclophosphamide. In these cases, cyclophosphamide is usually administered at doses of 500 mg intravenously, once daily over 2 hours. Typically, a single dose is used, as additional doses can cause severe bone marrow suppression. Statement 17 ➤ We did not systematically search and review the evidence on splenectomy for TTP patients. This procedure has been largely superseded by other treatments such as rituximab. It is generally not used, but may have a role in selected TTP patients as a prophylactic strategy. Statement 18 ➤ We did not systematically search and review the evidence on azathioprine for TTP patients. Clinicians sometimes consider azathioprine to inhibit ADAMTS13 autoantibody production that leads to normalization of plasma ADAMTS13 activity and prevents relapse in patients with refractory TTP unresponsive to standard treatments. Statement 19 ➤ We did not systematically search and review the evidence on antiplatelet agents for TTP patients. Antiplatelet agents were used in nonpregnant patients with TTP, particularly in the setting of macrothrombotic complications (e.g., ischemic stroke and myocardial infarction). Otherwise, antiplatelets are not generally used in TTP; their role in preventing relapse is not supported in the literature, and they may be harmful in the acute phase of TTP when the platelet count is <50 × 109/L. Input from cardiologists, neurologists, and/ or other vascular medicine specialists is usually sought if antiplatelet agents are considered in the treatment of TTP complications. Statement 20 ➤ We did not systematically search and review the evidence on eculizumab for TTP patients. Increased complement activation is demonstrated in TTP. Therefore, clinicians sometimes consider an anti-C5 monoclonal antibody (i.e. eculizumab) in very selected TTP patients with refractory disease or unresponsive to all other treatment options. This strategy should be pursued with caution.

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