Disodium 4,4'-bis[6-anilino-[4-[bis(2-hydroxyethyl)amino]-1,3,5-triazin-2-yl]amino]stilbene-2,2'-disulphonate

A teratology study was conducted using the test chemical was conducted to analyze the effects on the maternal and fetal health. In this study, four groups each of 25 mated female New Zealand white rabbits per group were treated once per day via oral gavage either with 0.5% carboxymethylcellulose (vehicle) alone (one control group) or with test chemical each at dose levels of 100, 400 and 800 mg/kg bw/day in a dosing volume of 10 ml/kg bw/day. Dosing was initiated on day 5 of gestation and continued to and included day 29 of gestation.  At the dose level of 800 mg/kg bw/day, excessive mortality and maternal toxicity were observed (8/25 found dead, 1/25 euthanized) with clinical signs of convulsions, decreased defecation, soft stool, discolored feces and reddish fluid in refuse pan and with significant decreases in body weight gain and food consumption. Abortion occurred in 7/25 animals. Necropsy findings included discoloration of the liver, edematous and/or discolored stomach, red discolored and/or edematous intestines, and bloody and/or mucoid contents in the intestines. As a result this group was terminated prior to completion of study. At the dose level of 400 mg/kg bw/day, 1/25 dams died from mechanical injury from gavage. Slight increases in reduced, soft or discolored feces were noted. Abortion occurred in 1/25 and early delivery in 2/25 which was considered to be treatment-related. No changes in body weight, body weight gain or food consumption were noted. At necropsy the dam that aborted showed an edematous stomach and liquid, bloody contents in the intestines. There were no further substance-related findings at necropsy. No effects on the following uterine parameters were observed: number of corpora lutea, implantation, live fetuses, resorption, uterine weight and adjusted body weight gain. Fetal body weights were significantly lower when compared to controls which was considered to be secondary to the maternal toxicity and not an indicator of developmental toxicity. At visceral examination of fetuses, the litter incidence of hemorrhagic iris at 400 mg/kg bw/day was slightly above the historical range while the incidences of gallbladder agenesis, hypoplasia of the gallbladder and a zygous lobe of lung absent were slightly increased but well within historical control range. Since all the above findings were within or only slightly above the historical control range, the findings were considered to be spontaneous in nature and unrelated to test substance. Also, no significant treatment-related effects were noted at external and skeletal examinations. At the dose level of 100 mg/kg bw/day there was no mortality observed; abortion occurred in 1/25 animal having mechanical injuries consistent with gavage errors; no changes in body weight, body weight gain or food consumption; no findings at necropsy; no effects on uterine parameters and fetal examinations. Control group: 2/25 animals died from mechanical injury from gavage. Based on all the available observations and results, it was concluded that NOAEL as per the maternal toxicity and fetal parameters was found to be 100 mg/kg bw/day.

The chemical was given by oral gavage to 30 presumed pregnant rats per dose level at 0 (vehicle control), 100, 400 and 1000 mg/kg bw/day from day 6 to 19 of gestation. All animals survived to planned death. There was no compound-related effect on body weight, body weight gain or food intake. The numbers of corpora lutea, implantations, live foetuses and resorptions, foetal weight, and sex ratio were similar between the groups. Pre- and post-implantation losses were similar between the groups, as was gravid uterine weight. The numbers of pregnant animals were 30, 29, 28 and 28 and 0, 100, 400 and 1000 mg/kg, respectively. No abortions were observed. The total numbers of foetuses were 383, 357, 363 and 348 at 0, 100, 400 and 1000 mg/kg, respectively. No dead foetuses were observed. One foetus at 1000 mg/kg showed omphalocele and a second foetus from a different litter lacked tail and anal atresia. Because only one foetus was affected in each case, the findings were considered to be spontaneous in nature. Visceral findings were unremarkable. Skeletal abnormalities were limited to an increased incidence of vertebral malformations at 1000 mg/kg (7.1% of litters) compared to the control (0% of the litters); increased incidences of misaligned sternebra at 100 (10.3% of litters) and 1000 mg/kg (10.7% of litters) compared to control (3.3% of litters); and increased incidences of rudimentary ribs at 100 (75.9% of litters) and 1000 mg/kg (78.6% of litters) compared to control (63.3% of litters). The incidence of vertebral malformation at 1000 mg/kg was very slightly above the historical control range (0 to 7%) and was not statistically different from the control group. The incidences of misaligned sternebra at 100 and 1000 mg/kg were within the historical control data (0 to 27% of litters). The incidences of rudimentary ribs at 100 and 1000 mg/kg were above the historical control data (0 to 70%) but at no dose level statistically different from the control group. No clear dose dependency was observed for this effect since the incidence of rudimentary ribs at 400 mg/kg (57.1% of litters) was lower compared to the control group (63.3% of litters). The study-derived NOAEL for maternal and developmental toxicity was 1000 mg/kg bw/day. The study was performed according to GLP.