This protocol can be used to create patient-derived xenografts that recapitulate the histopathology of venous malformations. This was further allowed to carry our preclinical therapeutic testing. This technique provides a fast and reliable NVivo s
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We present a detailed protocol to generate a murine xenograft model of venous malformation. This model is based on the subcutaneous injection of patient-derived endothelial cells containing hyper-activating TIE2 and/or PIK3CA gene mutations. Xenograft lesions closely recapitulate the histopathological features of VM patient tissue.