Teclistamab Shows Promise in Treating Severe Autoimmune Blood Disorder
Researchers in Germany have reported encouraging results using the bispecific antibody teclistamab for patients suffering from severe immune thrombocytopenia (ITP), a rare autoimmune blood disorder. ITP occurs when the immune system mistakenly targets and destroys platelets, increasing the risk of serious bleeding. Standard therapies for ITP include corticosteroids, immunoglobulins, Rituximab, and platelet transfusions. However, these treatments are not always effective in patients with severe or treatment-resistant cases.
The new approach involves teclistamab, a bispecific antibody that brings T-cells and plasma cells into close proximity, resulting in the targeted destruction of antibody-producing plasma cells responsible for the autoimmune attack. Teclistamab is already approved for use in multiple myeloma since 2023 due to its dual-binding capability: one site binds to the B-cell maturation antigen (BCMA) found on plasma cells, while the other binds to a surface molecule on T-cells. This mechanism facilitates the immune system's ability to eliminate the malfunctioning B-cells producing harmful autoantibodies.
A team of scientists from Berlin's Charité hospital and University Medicine Greifswald administered teclistamab to three patients with severe, treatment-refractory ITP. Following the initiation of the immunotherapy, all three patients demonstrated rapid normalization of their blood counts. Within four, nine, and twenty-three days after the start of treatment, platelet numbers in the patients' blood returned to normal ranges. Additionally, acute bleeding symptoms subsided quickly, allowing for a gradual reduction and discontinuation of previous medications, including corticosteroids.
The patients have remained stable and medication-free for periods spanning five to nine months following the intervention. Side effects were generally mild and manageable, consisting mainly of temporary low-grade fever or a brief decline in certain immune cell populations. In one case, a patient who also suffered from autoimmune hemolytic anemia--also known as Evans syndrome--experienced normalization of red blood cell counts in addition to improvement in platelet levels.
Although the results are promising, researchers caution against declaring a cure at this stage, as long-term stability of blood parameters will require further monitoring. The current remission periods are encouraging, but continued follow-up is necessary to determine the durability and safety of the response. Plans are underway to conduct additional clinical studies to assess teclistamab's long-term safety profile and its potential efficacy in larger patient groups and in other autoimmune conditions.
The findings, which were published in the journal "Blood Immunology & Cellular Therapy," highlight the potential of targeted immunotherapies in addressing severe autoimmune diseases that are unresponsive to conventional treatments. The study provides a foundation for future research into the broader application of bispecific antibodies in autoimmune hematological disorders.