Acute radiation syndrome (ARS) occurs when hematopoietic or gastrointestinal cells are damaged by radiation exposure causing DNA damage to the bone marrow and gastrointestinal epithelial stem cell populations. In these highly proliferative cell types, DNA damage inhibits stem cell repopulation. In humans and animals, this inability to regenerate stem cells is lethal. Within this manuscript, several compounds, Amifostine, Captopril, Ciprofloxacin, PrC-210, 5-AED (5-androstene-3β,17β-diol), and 5-AET (5-androstene-3β,7β,17B-triol), are assessed for their ability to protect against ARS in an in vitro and/or in vivo setting. ARS was accomplished by irradiating mouse bone marrow cells or rat intestinal epithelial (IEC-6) cells in vitro with 4-8 Gy and in vivo by exposing Mus musculus to 7.3 Gy of whole-body irradiation. The primary endpoints of this study include cellular viability, DNA damage via γ-H2AX, colony formation, and overall survival at 30-days post-irradiation. In addition to evaluating the radioprotective performance of each compound, this study establishes a distinct set of in vitro assays to predict the overall efficacy of potential radioprotectors in an in vivo model of ARS. Furthermore, these results highlight the need for FDA-approved medical intervention to protect against ARS.
Identification of Potential Prophylactic Medical Countermeasures Against Acute Radiation Syndrome (ARS).
识别针对急性放射综合征(ARS)的潜在预防性医疗对策
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作者:Liermann-Wooldrik Kia T, Chatterjee Arpita, Kosmacek Elizabeth A, Myers Molly S, Adebisi Oluwaseun, Monga-Wells Louise, Mei Liu, Takacs Michelle P, Dussault Patrick H, Draney Daniel R, Powers Robert, Checco James W, Guda Chittibabu, Helikar Tomáš, Berkowitz David B, Bayles Kenneth W, Epstein Alan H, Cary Lynnette, Murry Daryl J, Oberley-Deegan Rebecca E
| 期刊: | International Journal of Molecular Sciences | 影响因子: | 4.900 |
| 时间: | 2025 | 起止号: | 2025 Apr 25; 26(9):4055 |
| doi: | 10.3390/ijms26094055 | ||
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