Asuka Takumi scite author profile

To assess the influences of blood sampling volumes or sites on toxicological and toxicokinetic (TK) evaluations, 4-week duration animal studies and a single-dose TK study of imipramine were conducted. In the toxicological evaluation, six-week-old Sprague-Dawley rats were divided into no blood and blood sampling groups. Fifty microliters (microsampling) or 100 μL (larger sampling) of blood/time point was collected from the jugular vein (50 μL of data was reported previously as Yokoyama et al., 2020) or the tail vein 6 to 7 times on days 1/2 and in week 4. Although no parameters were affected by the 100 μL sample from the tail vein, the 100 μL jugular vein sampling decreased the red blood cell parameters in females, possibly due to hemorrhage at the sampling site. Regarding the TK assessment, 50 μL of blood/site/time point was collected at 6 time points from the tail and jugular vein of the same male rats after single oral administration of 10 or 100 mg/kg imipramine, which was selected as a representative drug with high distribution volume. Although there were no differences in the AUC 0-24hr and C max values between the sites, the plasma concentrations at the early time points were significantly lower from the tail vein than the jugular vein. From our studies, 50 μL of jugular and tail vein microsampling did not affect the toxicity parameters or AUC/C max . However, appropriate toxicity considerations and/or selection of the blood sampling site may be important in the case of larger sampling volumes or blood concentration assessment.

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Mutagenicity and genotoxicity studies of aspartame

Otabe

Ohta

Takumi

et al. 2019

Regulatory Toxicology and Pharmacology

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Two studies were conducted to further assess its mutagenic and genotoxic potential. In a bacterial reverse mutation pre-incubation study, Salmonella typhimurium strains TA100, TA1535, TA98, and TA1537 and Escherichia coli WP2 uvrA were treated with aspartame at concentrations of up to 5000 μg/plate with or without metabolic activation and showed no mutagenic potential. Similarly, in vivo micronucleus testing of aspartame following gavage administration (500-2000 mg/kg body weight) to Crlj:CD1(ICR) strain SPF male mice showed no increase in the proportion of micronucleated polychromatic erythrocytes in bone marrow cells collected and evaluated 24 or 48 h post administration. Overall, aspartame had no potential for mutagenic or genotoxic activity.

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Genotoxicity and repeated-dose toxicity evaluation of dried Wolffia globosa Mankai

et al. 2020

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Highlights Wolffia globosa Mankai can serve as a plant substitute for animal protein. Genotoxicity and subchronic toxicity studies (GLP) of dry Mankai were conducted. Dry Mankai was judged as having no potential to induce gene mutations in Ames test. Dry Mankai did not induce chromosomal aberration in in vitro micronucleus test. The NOAEL of Dry Mankai in 90-day dietary toxicity study was 20 % (w/w).

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Asuka Takumi

Lack of toxicological influences by microsampling (50 µL) from jugular vein of rats in a collaborative 28-day study

Effects of serial cervical or tail blood sampling on toxicity and toxicokinetic evaluation in rats

Mutagenicity and genotoxicity studies of aspartame

Genotoxicity and repeated-dose toxicity evaluation of dried Wolffia globosa Mankai

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