The Radioprotectant, BIO 300, Protects the Lungs from Total-Body Irradiation Injury in C57L/J Mice

Vijay K Singh; Artur A Serebrenik; Oluseyi O Fatanmi; Stephen Y Wise; Alana D Carpenter; Brianna L Janocha; Michael D Kaytor

doi:10.1667/RADE-22-00142.1

The Radioprotectant, BIO 300, Protects the Lungs from Total-Body Irradiation Injury in C57L/J Mice

Radiat Res. 2023 Mar 1;199(3):294-300. doi: 10.1667/RADE-22-00142.1.

Authors

Vijay K Singh^{1

2}, Artur A Serebrenik³, Oluseyi O Fatanmi^{1

2}, Stephen Y Wise^{1

2}, Alana D Carpenter^{1

2}, Brianna L Janocha^{1

2}, Michael D Kaytor³

Affiliations

¹ Division of Radioprotectants, Department of Pharmacology and Molecular Therapeutics, F. Edward Hébert School of Medicine, Uniformed Services University of the Health Sciences, Bethesda, Maryland.
² Armed Forces Radiobiology Research Institute, Uniformed Services University of the Health Sciences, Bethesda, Maryland.
³ Humanetics Corporation, Minneapolis, Minnesota.

PMID: 36689635
DOI: 10.1667/RADE-22-00142.1

Abstract

Acute exposure to high dose radiation can cause acute radiation syndrome (ARS), a potentially life-threatening illness. Individuals that survive ARS are at risk of developing the delayed effects of acute radiation exposure, with the lungs being particularly susceptible (DEARE-lung). For individuals at risk of radiation exposure, there are no Food and Drug Administration-approved medical countermeasures (MCMs) for prophylactic or post-exposure use that can prevent or mitigate DEARE-lung. BIO 300 is a novel formulation of synthetic genistein that has been extensively studied as a prophylactic MCM for the hematopoietic subsyndrome of ARS (H-ARS). Here, we used a C57L/J mouse model of total-body irradiation (TBI) to investigate whether prophylactic administration of BIO 300 is able to prevent animals from developing DEARE-lung. Oral and parenteral formulations of BIO 300 administered prior to TBI were compared against standard of care, PEGfilgrastim, administered shortly after radiation exposure, and the combination of oral BIO 300 administered prior to TBI and with PEGfilgrastim administered post-exposure. All animals were exposed to 7.75 Gy cobalt-60 gamma-radiation and the primary endpoint was lung histopathology at 180 days post-TBI. Animals treated with BIO 300 had a significant reduction in the incidence of interstitial lung inflammation compared to vehicle groups for both the oral (0% vs. 47%) and parenteral (13% vs. 44%) routes of administration. Similar results were obtained for the incidence and severity of pulmonary fibrosis in animals treated with oral BIO 300 (incidence, 47% vs. 100% and mean severity score, 0.53 vs. 1.3) and parenteral BIO 300 (incidence, 63% vs. 100% and mean severity score, 0.69 vs. 1.7). PEGfilgrastim alone had no significant effect in reducing the incidence of inflammation or fibrosis compared to vehicle. The combination of oral BIO 300 and PEGfilgrastim significantly reduced the incidence of interstitial inflammation (13% vs. 46%) and the severity of pulmonary fibrosis (mean severity score, 0.93 vs. 1.6). Results in the C57L/J mice were compared to those in CD2F1 mice, which are less prone to lung injury following total-body irradiation. Taken together, these studies indicate that BIO 300 is a promising MCM that is able to prophylactically protect against DEARE-lung.

Publication types

Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Acute Radiation Syndrome* / drug therapy
Acute Radiation Syndrome* / pathology
Acute Radiation Syndrome* / prevention & control
Animals
Inflammation / pathology
Lung / radiation effects
Lung Injury* / drug therapy
Lung Injury* / etiology
Lung Injury* / prevention & control
Mice
Mice, Inbred Strains
Pulmonary Fibrosis*
Whole-Body Irradiation / adverse effects