The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma

The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma

Radiotherapy using high linear energy transfer (LET) radiation results in effectively killing tumor cells while minimizing dose (biological effective) to normal tissues to block toxicity. It is well known that high LET radiation leads to lower cell survival per absorbed dose than low LET radiation....

Full description

Bibliographic Details
Main Authors: Ju Yeon Oh, Yeon-Joo Lee, Sei Sai, Tatsuya Ohno, Chang-Bae Kong, Sun Ha Lim, Eun Ho Kim
Format: Article
Language:English
Published: MDPI AG 2020-05-01
Series:International Journal of Molecular Sciences
Subjects:
autophagy
linear energy transfer
neutron beam
osteosarcoma
radiosensitivity
unfolded protein response
Online Access:https://www.mdpi.com/1422-0067/21/11/3766
id doaj-cd01a3090a6c44aca3eeb61e9692fd2f
record_format Article
spelling doaj-cd01a3090a6c44aca3eeb61e9692fd2f2020-11-25T03:25:56ZengMDPI AGInternational Journal of Molecular Sciences1661-65961422-00672020-05-01213766376610.3390/ijms21113766The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for OsteosarcomaJu Yeon Oh0Yeon-Joo Lee1Sei Sai2Tatsuya Ohno3Chang-Bae Kong4Sun Ha Lim5Eun Ho Kim6Laboratory of Biochemistry, Division of Life Sciences, Korea University, Seongbuk-gu, Seoul 02841, KoreaDivision of Radiation Biomedical Research, Korea Institute of Radiological and Medical Sciences, Seoul 01812, KoreaDepartment of Basic Medical Sciences for Radiation Damages, National Institute of Radiological Sciences, National Institutes for Quantum and Radiological Science and Technology, Chiba 263–8555, JapanGunma University Heavy Ion Medical Center, 3–39–22 Showa-machi, Maebashi, Gunma 371–8511, JapanDepartment of Orthopedic Surgery, Korea Institute of Radiological and Medical Sciences, Seoul 139–706, KoreaDepartment of Biochemistry, School of Medicine, Daegu Catholic University, Duryugongwon-ro, Nam-gu, Daegu 42472, KoreaDepartment of Biochemistry, School of Medicine, Daegu Catholic University, Duryugongwon-ro, Nam-gu, Daegu 42472, KoreaRadiotherapy using high linear energy transfer (LET) radiation results in effectively killing tumor cells while minimizing dose (biological effective) to normal tissues to block toxicity. It is well known that high LET radiation leads to lower cell survival per absorbed dose than low LET radiation. High-linear energy transfer (LET) neutron treatment induces autophagy in tumor cells, but its precise mechanisms in osteosarcoma are unknown. Here, we investigated this mechanism and the underlying signaling pathways. Autophagy induction was examined in gamma-ray-treated KHOS/NP and MG63 osteosarcoma cells along with exposure to high-LET neutrons. The relationship between radiosensitivity and autophagy was assessed by plotting the cell surviving fractions against autophagy levels. Neutron treatment increased autophagy rates in irradiated KHOS/NP and MG63 cells; neutrons with high-LETs showed more effective inhibition than those with lower LET gamma-rays. To determine whether the unfolded protein response and Akt-mTOR pathways triggered autophagy, phosphorylated eIF2α and JNK levels, and phospho-Akt, phosphor-mTOR, and phospho-p70S6 levels were, respectively, investigated. High-LET neutron exposure inhibited Akt phosphorylation and increased Beclin 1 expression during the unfolded protein response, thereby enhancing autophagy. The therapeutic efficacy of high-LET neutron radiation was also assessed in vivo<i> </i>using an orthotopic mouse model. Neutron-irradiated mice showed reduced tumor growth without toxicity relative to gamma-ray-treated mice. The effect of high-LET neutron exposure on the expression of signaling proteins LC3, p-elF2a, and p-JNK was investigated by immunohistochemistry. Tumors in high-LET-neutron radiation-treated mice showed higher apoptosis rates, and neutron exposure significantly elevated LC3 expression, and increased p-elF2a and p-JNK expression levels. Overall, these results demonstrate that autophagy is important in radiosensitivity, cell survival, and cellular resistance against high-LET neutron radiation. This correlation between cellular radiosensitivity and autophagy may be used to predict radiosensitivity in osteosarcoma.https://www.mdpi.com/1422-0067/21/11/3766autophagylinear energy transferneutron beamosteosarcomaradiosensitivityunfolded protein response
collection DOAJ
language English
format Article
sources DOAJ
author Ju Yeon Oh
Yeon-Joo Lee
Sei Sai
Tatsuya Ohno
Chang-Bae Kong
Sun Ha Lim
Eun Ho Kim
spellingShingle Ju Yeon Oh
Yeon-Joo Lee
Sei Sai
Tatsuya Ohno
Chang-Bae Kong
Sun Ha Lim
Eun Ho Kim
The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
International Journal of Molecular Sciences
autophagy
linear energy transfer
neutron beam
osteosarcoma
radiosensitivity
unfolded protein response
author_facet Ju Yeon Oh
Yeon-Joo Lee
Sei Sai
Tatsuya Ohno
Chang-Bae Kong
Sun Ha Lim
Eun Ho Kim
author_sort Ju Yeon Oh
title The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
title_short The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
title_full The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
title_fullStr The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
title_full_unstemmed The Unfolded Protein Response: Neutron-Induced Therapy Autophagy as a Promising Treatment Option for Osteosarcoma
title_sort unfolded protein response: neutron-induced therapy autophagy as a promising treatment option for osteosarcoma
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1661-6596
1422-0067
publishDate 2020-05-01
description Radiotherapy using high linear energy transfer (LET) radiation results in effectively killing tumor cells while minimizing dose (biological effective) to normal tissues to block toxicity. It is well known that high LET radiation leads to lower cell survival per absorbed dose than low LET radiation. High-linear energy transfer (LET) neutron treatment induces autophagy in tumor cells, but its precise mechanisms in osteosarcoma are unknown. Here, we investigated this mechanism and the underlying signaling pathways. Autophagy induction was examined in gamma-ray-treated KHOS/NP and MG63 osteosarcoma cells along with exposure to high-LET neutrons. The relationship between radiosensitivity and autophagy was assessed by plotting the cell surviving fractions against autophagy levels. Neutron treatment increased autophagy rates in irradiated KHOS/NP and MG63 cells; neutrons with high-LETs showed more effective inhibition than those with lower LET gamma-rays. To determine whether the unfolded protein response and Akt-mTOR pathways triggered autophagy, phosphorylated eIF2α and JNK levels, and phospho-Akt, phosphor-mTOR, and phospho-p70S6 levels were, respectively, investigated. High-LET neutron exposure inhibited Akt phosphorylation and increased Beclin 1 expression during the unfolded protein response, thereby enhancing autophagy. The therapeutic efficacy of high-LET neutron radiation was also assessed in vivo<i> </i>using an orthotopic mouse model. Neutron-irradiated mice showed reduced tumor growth without toxicity relative to gamma-ray-treated mice. The effect of high-LET neutron exposure on the expression of signaling proteins LC3, p-elF2a, and p-JNK was investigated by immunohistochemistry. Tumors in high-LET-neutron radiation-treated mice showed higher apoptosis rates, and neutron exposure significantly elevated LC3 expression, and increased p-elF2a and p-JNK expression levels. Overall, these results demonstrate that autophagy is important in radiosensitivity, cell survival, and cellular resistance against high-LET neutron radiation. This correlation between cellular radiosensitivity and autophagy may be used to predict radiosensitivity in osteosarcoma.
topic autophagy
linear energy transfer
neutron beam
osteosarcoma
radiosensitivity
unfolded protein response
url https://www.mdpi.com/1422-0067/21/11/3766
work_keys_str_mv AT juyeonoh theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT yeonjoolee theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT seisai theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT tatsuyaohno theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT changbaekong theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT sunhalim theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT eunhokim theunfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT juyeonoh unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT yeonjoolee unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT seisai unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT tatsuyaohno unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT changbaekong unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT sunhalim unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
AT eunhokim unfoldedproteinresponseneutroninducedtherapyautophagyasapromisingtreatmentoptionforosteosarcoma
_version_ 1724594900031242240

Similar Items