Toxicology of polymer pharmaceutical excipients in Sprague-Dawley rats and Beagle dogs
10.3969/j.issn.1671-7856.2025.06.006
- VernacularTitle:高分子药用辅料对SD大鼠和Beagle犬毒理研究
- Author:
Jinlong DAI
1
;
Xialing LEI
1
;
Yuankeng HUANG
1
;
Jianmin GUO
1
;
Zhisen CHEN
1
;
Wei YANG
1
Author Information
1. 广州湾区生物医药研究院,广东莱恩医药研究院有限公司,广东省药物非临床评价与研究重点实验室,国家中药现代化工程技术研究中心中药非临床评价分中心,从化区动物病理与医学检验检测工程技术研究中心,广州 510990
- Publication Type:Journal Article
- Keywords:
polymer pharmaceutical excipient;
toxicological research;
SD rats;
Beagle dogs
- From:
Chinese Journal of Comparative Medicine
2025;35(6):50-64
- CountryChina
- Language:Chinese
-
Abstract:
Objective To investigate the effects of the polymer pharmaceutical excipient methoxy poly-ethylene glycol poly-lactic acid(mPEG-PLA)in Sprague-Dawley(SD)rats and Beagle dogs and its toxicological reactions,to provide a reference for its safe clinical use.Methods SD rats and Beagle dogs(male∶female ratios,1∶1)were divided randomly into control group and low,medium,and high dose mPEG-PLA groups(70,210,700 mg/kg).Animals received intravenous mPEG-PLA once a day for 90 days,followed by a 28-day recovery period.Indicators including clinical observations,food intake,body weight,hematology,blood biochemistry,immune function,and pathological examination were recorded.Results Compared with the control group,(1)food intake was decreased(P<0.01)and body weight was increased(P<0.05 or P<0.01)after 90 days of continuous administration,with similar changes in the medium and high dose groups in both rats and dogs.In addition,MONO/MONO%,RBC,MCH,MCHC,HCT,HGB,PLT,TP,ALB,GLB,and Fbg were all decreased(P<0.05 or P<0.01)and coagulation indexes(e.g.,APTT)were increased(P<0.05 or P<0.01).Organ weights and the organ-to-body/brain weight ratios of the liver and spleen were increased(P<0.05 or P<0.01),and histopathology indicated numerous foam-like macrophages in the hepatic sinuses,red spleen pulp,and lymph node medulla.DBIL and TBIL also increased in rats in the high dose group(P<0.05 or P<0.01),while the dogs experienced skin swelling or scabs,abdominal swelling,vomiting,decreased activity,high albuminuria,and ascites,and the renal glomerular cells showed vacuoles.(2)After 28 days of recovery,rats and dogs in the medium and high dose groups showed a few foam-like macrophages in the hepatic sinuses,red spleen pulp,and lymph node medulla,as well as decreased of food intake in dogs.The MCHC,PLT,and TP decreased in dogs in the high dose group(P<0.05),and the liver and spleen weights and organ coefficients in rats increased(P<0.05 or P<0.01),while the MONO%decreased in male rats in the medium dose group(P<0.05).Conclusions Administration of mPEG-PLA 210 and 700 mg/kg for 90 days caused blood mononuclear cells to enter and aggregate in the liver,spleen,lymph nodes,and other tissues in SD rats and Beagle dogs,leading to secondary tissue structural damage.Protein and fibrinogen synthesis and bilirubin metabolism in the liver decreased,leading to abnormal coagulation function,and decreased intravascular colloid osmotic pressure resulted in edema and bleeding.The result suggest that the liver,spleen,kidney,and lymph nodes are target organs for mPEG-PLA toxicity,with dose-dependent and reversible effects and species differences,but no significant sex differences.Clinical monitoring of related organ functions is needed to avoid secondary damage.
