With rare exceptions, there is usually no need to treat based on platelet counts. Many older recommendations suggested a certain platelet count threshold (usually somewhere below 20.0/nL) as an indication for hospitalization or treatment. Current guidelines recommend treatment for adults with significant bleeding or counts below 30/nL, with very low certainty of evidence. Treatment recommendations sometimes differ for adult and pediatric ITP.
Steroids Initial treatment usually consists of the administration of
corticosteroids, a group of medications that suppress the immune system. The dose and mode of administration is determined by platelet count and whether there is active bleeding: in urgent situations,
infusions of
dexamethasone or
methylprednisolone may be used, while oral
prednisone or
prednisolone may suffice in less severe cases. Once the platelet count has improved, the dose of steroid is gradually reduced while the possibility of relapse is monitored. 60–90 percent will experience a relapse during dose reduction or cessation.
Anti-D Another option, suitable for
Rh-positive patients with functional
spleens is intravenous administration of
Rho(D) immune globulin [Human; Anti-D]. The mechanism of action of anti-D is not fully understood. However, following administration, anti-D-coated red blood cell complexes saturate
Fcγ receptor sites on
macrophages, resulting in preferential destruction of
red blood cells (RBCs), therefore sparing antibody-coated
platelets. There are two anti-D products indicated for use in patients with ITP: WinRho SDF and Rhophylac. The most common adverse reactions are headache (15%), nausea/vomiting (12%) chills (<2%) and fever (1%).. Following a black-box warning of possible uncontrolled hemolytic reactions, use of intravenous anti-D declined sharply. Intramuscular anti-D has been suggested as an alternative, with one case series reporting a 73% response rate.
Steroid-sparing agents There is increasing use of
immunosuppressants such as
mycophenolate mofetil and
azathioprine because of their effectiveness. In chronic refractory cases, where immune pathogenesis has been confirmed, the
off-label use of the
vinca alkaloid and
chemotherapy agent
vincristine may be attempted. However, vincristine has significant
side effects and its use in treating ITP must be approached with caution, especially in children.
Intravenous immunoglobulin Intravenous immunoglobulin (IVIg) may be infused in some cases in order to decrease the rate at which
macrophages consume
antibody-tagged platelets. However, while sometimes effective, it is costly and produces improvement that generally lasts less than a month. Nevertheless, in the case of an ITP patient already scheduled for
surgery who has a dangerously low platelet count and has experienced a poor response to other treatments, IVIg can rapidly increase platelet counts, and can also help reduce the risk of major bleeding by transiently increasing platelet counts.
Thrombopoietin receptor agonists Thrombopoietin receptor agonists are
pharmaceutical agents that stimulate platelet production in the bone marrow. In this, they differ from the previously discussed agents that act by attempting to curtail platelet destruction. Two such products are currently available: •
Romiplostim (trade name Nplate) is a
thrombopoiesis stimulating Fc-peptide fusion protein (peptibody) that is administered by
subcutaneous injection. Designated an
orphan drug in 2003 under United States law, clinical trials demonstrated romiplostim to be effective in treating chronic ITP, especially in relapsed post-splenectomy patients. Romiplostim was approved by the United States
Food and Drug Administration (FDA) for long-term treatment of adult chronic ITP on August 22, 2008. •
Eltrombopag (trade name Promacta in the US, Revolade in the EU) is an orally-administered agent with an effect similar to that of romiplostim. It too has been demonstrated to increase platelet counts and decrease bleeding in a dose-dependent manner. Developed by
GlaxoSmithKline and also designated an orphan drug by the FDA, Promacta was approved by the FDA on November 20, 2008. Thrombopoietin receptor agonists exhibited the greatest success so far in treating patients with refractory ITP. Side effects of thrombopoietin receptor agonists include headache, joint or muscle pain, dizziness, nausea or vomiting, and an increased risk of blood clots. Even though there is a consensus regarding the short-term efficacy of splenectomy, findings on its long-term efficacy and side-effects are controversial. After splenectomy, 11.6–75 percent of ITP cases relapsed, and 8.7–40 percent of ITP cases had no response to splenectomy. The use of splenectomy to treat ITP has diminished since the development of steroid therapy and other pharmaceutical remedies.
Platelet transfusion Platelet transfusion alone is normally not recommended except in an emergency and is usually unsuccessful in producing a long-term platelet count increase. This is because the underlying autoimmune mechanism that is destroying the patient's platelets will also destroy donor platelets, and so platelet transfusions are
not considered a long-term treatment option.
H. pylori eradication In adults, particularly those living in areas with a high prevalence of
Helicobacter pylori (which normally inhabits the stomach wall and has been associated with
peptic ulcers), identification and treatment of this infection has been shown to improve platelet counts in a third of patients. In a fifth, the platelet count normalized completely; this response rate is similar to that found in treatment with rituximab, which is more expensive and less safe. In children, this approach is not supported by evidence, except in high prevalence areas.
Urea breath testing and stool antigen testing perform better than
serology-based tests; moreover, serology may be false-positive after treatment with IVIG.
Other agents •
Dapsone (also called diphenylsulfone, DDS, or avlosulfon) is an anti-infective sulfone medication. Dapsone may also be helpful in treating lupus, rheumatoid arthritis, and as a second-line treatment for ITP. The mechanism by which dapsone assists in ITP is unclear but an increased platelet count is seen in 40–60 percent of recipients. • The off-label use of
rituximab, a
chimeric monoclonal antibody against the
B cell surface
antigen CD20, may sometimes be an effective alternative to splenectomy. However,
significant side-effects can occur, and
randomized controlled trials are inconclusive. •
Fostamatinib was approved for refractory chronic ITP in the United States in April 2018. Fostamatinib blocks the activity of the enzyme
spleen tyrosine kinase (SYK), thus reducing FcγR-mediated signal transduction and phagocytosis by monocyte/macrophages. Adverse effects include diarrhea, hypertension, and abnormal liver function tests. • In a phase 1-2 open-label study treatment with CM313, a novel anti-CD38 monoclonal antibody, rapidly boosted platelet levels in adults with ITP by inhibiting
antibody-dependent cell-mediated cytotoxicity on platelets; maintained long-term efficacy by clearing
plasma cells; and was associated with low-grade toxic effects. •
Ianalumab is a monoclonal antibody that targets the BAFF receptor
BAFF-R to inhibit B-cell signaling and deplete B cells through
antibody-dependent cellular cytotoxicity. The VAYHIT1 study was designed to evaluate the efficacy and safety of ianalumab for ITP. ==Prognosis==