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Chemoradiation impairs myofiber hypertrophic growth in a pediatric tumor model.

Scientific reports (2020-11-13)
Nicole D Paris, Jacob G Kallenbach, John F Bachman, Roméo S Blanc, Carl J Johnston, Eric Hernady, Jacqueline P Williams, Joe V Chakkalakal
ZUSAMMENFASSUNG

Pediatric cancer treatment often involves chemotherapy and radiation, where off-target effects can include skeletal muscle decline. The effect of such treatments on juvenile skeletal muscle growth has yet to be investigated. We employed a small animal irradiator to administer fractionated hindlimb irradiation to juvenile mice bearing implanted rhabdomyosarcoma (RMS) tumors. Hindlimb-targeted irradiation (3 × 8.2 Gy) of 4-week-old mice successfully eliminated RMS tumors implanted one week prior. After establishment of this preclinical model, a cohort of tumor-bearing mice were injected with the chemotherapeutic drug, vincristine, alone or in combination with fractionated irradiation (5 × 4.8 Gy). Single myofiber analysis of fast-contracting extensor digitorum longus (EDL) and slow-contracting soleus (SOL) muscles was conducted 3 weeks post-treatment. Although a reduction in myofiber size was apparent, EDL and SOL myonuclear number were differentially affected by juvenile irradiation and/or vincristine treatment. In contrast, a decrease in myonuclear domain (myofiber volume/myonucleus) was observed regardless of muscle or treatment. Thus, inhibition of myofiber hypertrophic growth is a consistent feature of pediatric cancer treatment.

MATERIALIEN
Produktnummer
Marke
Produktbeschreibung

Sigma-Aldrich
Anti-Laminin-2 (α-2 Chain) antibody, Rat monoclonal, clone 4H8-2, purified from hybridoma cell culture
Sigma-Aldrich
Vincristin -sulfat, meets USP testing specifications