AI Article Synopsis
- ALXN4100TPO, a TPO receptor agonist, significantly increases platelet counts and improves survival in lethally irradiated mice while preventing radiation-induced thrombocytopenia.
- The study involved a safety assessment through a single subcutaneous dose in mice, with results showing marked increases in platelet counts, enhanced bone marrow activity, and no severe side effects.
- Serum levels of ALXN4100TPO peaked 24 hours post-administration with a half-life of 13 days, and elevated endogenous TPO levels were noted at higher doses.
Article Abstract
ALXN4100TPO, a thrombopoietin (TPO) receptor agonist, increases platelets, abrogates radiation-induced thrombocytopenia and affords significant survival benefit to lethally irradiated mice. This preliminary nonclinical safety study assessed effects of a single subcutaneous (sc) administration of ALXN4100TPO in CD2F1 mice randomized into naïve, control antibody (ALXN4200, 100 mg/kg), low (1 mg/kg), medium (10 mg/kg), or high (100 mg/kg) ALXN4100TPO doses. End points included clinical observations, body weight changes, hematology, histopathology, pharmacokinetics, pharmacodynamics by measuring platelet counts, and endogenous TPO (eTPO) levels. Salient findings were prominent increase in platelet counts and end cells of myeloid and lymphoid lineages; elevated megakaryopoiesis in bone marrow; and extramedullary hematopoiesis in spleen and liver. Serum ALXN4100TPO levels were maximum 24 hours after administration, with a half-life of 13 days. Endogenous TPO levels were elevated in 10 and 100 mg/kg ALXN4100TPO-treated groups. In conclusion, ALXN4100TPO (1-100 mg/kg, sc) treatment in CD2F1 mice resulted in profound pharmacological changes in the hematopoietic tissue; however, no life-threatening adverse events were observed.
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| http://dx.doi.org/10.1177/1091581813482336 | DOI Listing |
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