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- Title
Exploring predictive molecules of acute adverse events in response to volumetric‑modulated arc therapy for prostate cancer using urinary metabolites.
- Authors
Obara, Hideki; Tatara, Yota; Monzen, Satoru; Murakami, Sho; Yamamoto, Hiroki; Kimura, Naoki; Suzuki, Masashi; Komai, Fumio; Narita, Masataka; Hatayama, Yoshiomi; Aoki, Masahiko
- Abstract
Volumetric-modulated arc therapy (VMAT) is a radiotherapy technique used to treat patients with localized prostate cancer, which is frequently associated with acute adverse events (AEs) that can affect subsequent treatment. Notably, the radiation dose of VMAT can be tailored to each patient. In the present study, a retrospective analysis was performed to predict acute AEs in response to a therapeutic high radiation dose rate based on urinary metabolomic molecules, which are easily collected as noninvasive biosamples. Urine samples from 11 patients with prostate cancer who were treated with VMAT (76 Gy/38 fractions) were collected. The study found that seven patients (~64%) exhibited genitourinary toxicity (Grade 1) and four patients had no AEs. A total of 630 urinary metabolites were then analyzed using a mass spectrometer (QTRAP6500+; AB SCIEX), and 234 relevant molecules for biological and clinical applications were extracted from the absolute quantified metabolite values using the MetaboINDICATOR tool. In the Grade 1 acute AE group, there was a significant negative correlation (rs=-0.297, P<0.05) between the number of VMAT fractions and total phospholipase A2 activity in the urine. Additionally, patients with Grade 1 AEs exhibited a decrease in PC aa C40:1, a phospholipid. These findings suggested that specific lipids found in urinary metabolites may serve as predictive biomarkers for acute AEs in response to external radiotherapy.
- Subjects
VOLUMETRIC-modulated arc therapy; PROSTATE cancer patients; BIOMOLECULES; PHOSPHOLIPASE A2; RADIATION doses
- Publication
Molecular & Clinical Oncology, 2024, Vol 21, Issue 3, pN.PAG
- ISSN
2049-9450
- Publication type
Article
- DOI
10.3892/mco.2024.2760