Effects of Dose Rate on the Reproductive Cell Death and Early Mitochondrial Membrane Potential in Different Human Epithelium-Derived Cells Exposed to Gamma Rays

Vo, Nguyen T. K.; Shahid, Marwan; Seymour, Colin; Mothersill, Carmel

doi:10.1177/1559325819852508

Cited by 4 publications

(6 citation statements)

References 38 publications

(58 reference statements)

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“…In Vo et al's study, 5 which used a low DR p (24-100 mGy/min, equal to the average DR because the irradiation was continuous), damage was not reported, but the surviving fraction at 2 Gy suggests rapid repair of the damages, probably less complex. In Sorensen et al's study, 21 increasing the DR p from 56.5 to 338 Gy/s did not appear to have consequences on clonogenic survival.…”

Section: In Silico Studymentioning

confidence: 97%

“…Data from 4 representative studies [5][6][7][8] have been selected to highlight the limitations inherent to the articles reviewed. These studies were those for which temporal and spatial microstructure parameters of the irradiation beams were reported (mean and instantaneous DR [DR pulse ] total dose, pulse frequency rate, and pulse width).…”

Section: In Silico Studymentioning

confidence: 99%

See 1 more Smart Citation

A Comprehensive Analysis of the Relationship Between Dose Rate and Biological Effects in Preclinical and Clinical Studies, From Brachytherapy to Flattening Filter Free Radiation Therapy and FLASH Irradiation

Beddok

Lahaye

Calugaru

et al. 2022

International Journal of Radiation Oncology*Biology*Physics

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Section: In Silico Studymentioning

confidence: 97%

Section: In Silico Studymentioning

confidence: 99%

A Comprehensive Analysis of the Relationship Between Dose Rate and Biological Effects in Preclinical and Clinical Studies, From Brachytherapy to Flattening Filter Free Radiation Therapy and FLASH Irradiation

Beddok

Lahaye

Calugaru

et al. 2022

International Journal of Radiation Oncology*Biology*Physics

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“…Noticeably, radiation-induced damage to the cell constituents occurs in a dose-dependent manner. Thus, the extent of the subsequent cell remodeling ultimately leads to either cell restoration or a complete cell loss (e.g., cell senescence or death) (64)(65)(66)(67). In this respect, considering the high energy of the penetrating radiation, the molecular damage to the cell and tissue structures from the direct radiation impact is not specific, although the consequent reactive responses to the radiation-produced injury are.…”

Section: X-ray and Gamma-photon Tissue Irradiation: Molecular Effects Induced By Ionization And The Mechanisms Of Cell Injurymentioning

confidence: 99%

“…Therefore, the concept of amplification of the radiation-induced ''primary'' oxidative stress has been further refocused on the shift of metabolic and pro-inflammatory redox pathways in irradiated cells (62,63,66,77,(81)(82)(83)(84)(85). Indeed, numerous observations indicate that the radiation-induced radiolysis can affect crucial cellular constituents and tilt calcium homeostasis, and thus can activate a cascade of metabolic responses leading to a prolonged oxidative stress which propagates systemically (64,(80)(81)(82)(83)(84)(85)(86)(87). Moreover, there are several redox mechanisms, which have been proposed to drive the metabolic oxidative stress.…”

Section: X-ray and Gamma-photon Tissue Irradiation: Molecular Effects Induced By Ionization And The Mechanisms Of Cell Injurymentioning

confidence: 99%

“…Notably, excessive generation of RLS implicated in the Michael addition/reaction can spread carbonyl (electrophilic) stress from the targeted cells to bystander cells via the gap junction network or the extracellular vesicle mechanisms, thus producing non-targeted effects including mitochondrial dysfunction, ER stress, disturbance of calcium homeostasis, and epigenetic and clastogenic dysregulations (86,100,102). Overall, while the ''radiolysis phase'' is short lived, it causes devastating systemic effects, i.e., radiation-induced damage to proteins and lipids, posttranslational modification of proteins, impairment of DNA, epigenetic alterations and formation of aberrant organelles generates an array of mediators of stress, danger and inflammation that interfere with cell communication systems and homeostatic control (55,64,87,108,109). In conjunction with these events, activation of free radical reactions, formation of ROS, RNS, RCS, RLS, the Schiff and etheno adducts, the products of protein sulfhydryl oxidation as well as depletion of antioxidants are major features of radiolysis in tissues and fluids, and therefore, are considered to be biomarkers of oxidative stress after radiation exposure.…”

Section: X-ray and Gamma-photon Tissue Irradiation: Molecular Effects Induced By Ionization And The Mechanisms Of Cell Injurymentioning

confidence: 99%

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Brain Damage and Patterns of Neurovascular Disorder after Ionizing Irradiation. Complications in Radiotherapy and Radiation Combined Injury

Gorbunov¹,

Kiang

2021

Radiation Research

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Exposure to ionizing radiation, mechanical trauma, toxic chemicals or infections, or combinations thereof (i.e., combined injury) can induce organic injury to brain tissues, the structural disarrangement of interactive networks of neurovascular and glial cells, as well as on arrays of the paracrine and systemic destruction. This leads to subsequent decline in cognitive capacity and decompensation of mental health. There is an ongoing need for improvement in mitigating and treating radiation-or combined injury-induced brain injury. Cranial irradiation per se can cause a multifactorial encephalopathy that occurs in a radiation dose-and time-dependent manner due to differences in radiosensitivity among the various constituents of brain parenchyma and vasculature. Of particular concern are the radiosensitivity and inflammation susceptibility of: 1. the neurogenic and oligodendrogenic niches in the subependymal and hippocampal domains; and 2. the microvascular endothelium. Thus, cranial or total-body irradiation can cause a plethora of biochemical and cellular disorders in brain tissues, including: 1. decline in neurogenesis and oligodendrogenesis; 2. impairment of the blood-brain barrier; and 3. ablation of vascular capillary. These changes, along with cerebrovascular inflammation, underlie different stages of encephalopathy, from the early protracted stage to the late delayed stage. It is evident that ionizing radiation combined with other traumatic insults such as penetrating wound, burn, blast, systemic infection and chemotherapy, among others, can exacerbate the radiation sequelae (and vice versa) with increasing severity of neurogenic and microvascular patterns of radiation brain damage.

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Serotonin and 5-HT3 receptors sensitize human skin cells to direct irradiation cell death but not to soluble radiation-induced bystander signals

Curtis

Seymour

et al. 2020

Environmental Research

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Effects of Dose Rate on the Reproductive Cell Death and Early Mitochondrial Membrane Potential in Different Human Epithelium-Derived Cells Exposed to Gamma Rays

Cited by 4 publications

References 38 publications

A Comprehensive Analysis of the Relationship Between Dose Rate and Biological Effects in Preclinical and Clinical Studies, From Brachytherapy to Flattening Filter Free Radiation Therapy and FLASH Irradiation

A Comprehensive Analysis of the Relationship Between Dose Rate and Biological Effects in Preclinical and Clinical Studies, From Brachytherapy to Flattening Filter Free Radiation Therapy and FLASH Irradiation

Brain Damage and Patterns of Neurovascular Disorder after Ionizing Irradiation. Complications in Radiotherapy and Radiation Combined Injury

Serotonin and 5-HT3 receptors sensitize human skin cells to direct irradiation cell death but not to soluble radiation-induced bystander signals

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