Docetaxel chemotherapy response in PC3 prostate cancer mouse model detected by rotating frame relaxations and water diffusion - UTU Tutkimustietojärjestelmä

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Docetaxel chemotherapy response in PC3 prostate cancer mouse model detected by rotating frame relaxations and water diffusion

Tekijät: Laakso Hanne, Ylä-Herttuala Elias, Sierra Alejandra, Jambor Ivan, Poutanen Matti, Liljenbäck Heidi, Virtanen Helena, Merisaari Harri, Aronen Hannu, Minn Heikki, Roivainen Anne, Liimatainen Timo

Kustantaja: WILEY

Julkaisuvuosi: 2021

Journal: NMR in Biomedicine

Tietokannassa oleva lehden nimi: NMR IN BIOMEDICINE

Lehden akronyymi: NMR BIOMED

Artikkelin numero: e4483

Vuosikerta: 34

Numero: 4

Sivujen määrä: 12

ISSN: 0952-3480

eISSN: 1099-1492

DOI: https://doi.org/10.1002/nbm.4483

Verkko-osoite: https://analyticalsciencejournals.onlinelibrary.wiley.com/doi/10.1002/nbm.4483

Rinnakkaistallenteen osoite: https://research.utu.fi/converis/portal/detail/Publication/53301755

Tiivistelmä

MRI is a common method of prostate cancer diagnosis. Several MRI-derived markers, including the apparent diffusion coefficient (ADC) based on diffusion-weighted imaging, have been shown to provide values for prostate cancer detection and characterization. The hypothesis of the study was that docetaxel chemotherapy response could be picked up earlier with rotating frame relaxation times T_RAFF2 and T_RAFF4 than with the continuous wave T1ρ, adiabatic T_1ρ, adiabatic T_2ρ, T₁, T₂ or water ADC. Human PC3 prostate cancer cells expressing a red fluorescent protein were implanted in 21 male mice. Docetaxel chemotherapy was given once a week starting 1 week after cell implantation for 10 randomly selected mice, while the rest served as a control group (n = 11). The MRI consisted of relaxation along a fictitious field (RAFF) in the second (RAFF2) and fourth (RAFF4) rotating frames, T₁ and T₂, continuous wave T1ρ, adiabatic T1ρ and adiabatic T2ρ relaxation time measurements and water ADC. MRI was conducted at 7 T, once a week up to 4 weeks from cell implantation. The tumor volume was monitored using T₂-weighted MRI and optical imaging. The histology was evaluated after the last imaging time point. Significantly reduced RAFFn, T1ρ,T2ρ and conventional relaxation times 4 weeks after tumor implantation were observed in the treated tumors compared with the controls. The clearest short- and long-term responses were obtained with T₁, while no clear improvement in response to treatment was detected with novel methods compared with conventional methods or with RAFFn compared with all others. The tumor volume decreased after a two-week time point for the treated group and increased significantly in the control group, which was supported by increasing red fluorescent light emission in the control tumors. Decreased relaxation times were associated with successful chemotherapy outcomes. The results indicate altered relaxation mechanisms compared with higher dose chemotherapies previously published.

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