Case report: rapid and durable response to PDGFR targeted therapy in a child with refractory multiple infantile myofibromatosis and a heterozygous germline mutation of the PDGFRB gene

Warning

This publication doesn't include Faculty of Economics and Administration. It includes Faculty of Medicine. Official publication website can be found on muni.cz.
Authors

MÚDRY Peter SLABÝ Ondřej NERADIL Jakub ŠOUKALOVÁ Jana MELICHÁRKOVÁ Kristýna ROHLEDER Ondřej JEŽOVÁ Marta SEEHOFNEROVÁ Anna PONECHAL MICHU Elleni VESELSKÁ Renata ŠTĚRBA Jaroslav

Year of publication 2017
Type Article in Periodical
Magazine / Source BMC Cancer
MU Faculty or unit

Faculty of Medicine

Citation
Web https://bmccancer.biomedcentral.com/articles/10.1186/s12885-017-3115-x
Doi http://dx.doi.org/10.1186/s12885-017-3115-x
Field Oncology and hematology
Keywords Infantile myofibromatosis; tyrosine kinase inhibitor; PDGFR; chemotherapy; theranostics; case report
Description Infantile myofibromatosis belongs to a family of soft tissue tumors. The majority of these tumors have benign behavior but resistant and malignant courses are known, namely in tumors with visceral involvement. The standard of care is surgical resection. Observations suggest that low dose chemotherapy is beneficial. The treatment of resistant or relapsed patients with multifocal disease remains challenging. Patients that harbor an actionable mutation in the kinase domain are potential subjects for targeted tyrosine kinase inhibitor therapy. An infant boy with inborn generalized infantile myofibromatosis that included bone, intracranial, soft tissue and visceral involvement was treated according to recent recommendations with low dose chemotherapy. The presence of a partial but temporary response led to a second line of treatment with six cycles of chemotherapy, which achieved a partial response again but was followed by severe toxicity. The generalized progression of the disease was observed later. Genetic analyses were performed and revealed a PDGFRB gene c. 1681C>A missense heterozygous germline mutation, high PDGFR beta phosphokinase activity within the tumor and the heterozygous germline Slavic Nijmegen breakage syndrome 657del5 mutation in the NBN gene. Targeted treatment with sunitinib, the PDGFR beta inhibitor, plus low dose vinblastine led to an unexpected and durable response without toxicities or limitations to daily life activities. The presence of the Slavic NBN gene mutation limited standard chemotherapy dosing due to severe toxicities. Sister of the patient suffred from skull base tumor with same genotype and histology. The same targeted therapy led to similar quick and durable response. Progressive and resistant incurable infantile myofibromatosis can be successfully treated with the new approach described herein. Detailed insights into the biology of the patient's tumor and genome are necessary to understand the mechanisms of activity of less toxic and effective drugs except for up to date population-based chemotherapy regimens.
Related projects:

You are running an old browser version. We recommend updating your browser to its latest version.