N-Phenyl-diethanolamine, reaction products with formaldehyde

Administrative data

Endpoint:

short-term repeated dose toxicity: oral

Type of information:

experimental study

Adequacy of study:

key study

Study period:

17 July 2020 - 23 March 2021

Reliability:

1 (reliable without restriction)

Rationale for reliability incl. deficiencies:

guideline study

Remarks:

Study conducted in accordance with international guidelines and in accordance with GLP. All guideline validity criteria were met.

Data source

Materials and methods

Test guidelineopen allclose all

Principles of method if other than guideline:

An OECD genotoxicity test was integrated into this toxicity study as follows:
- Principle of test: OECD TG474 Mammalian Erythrocyte Micronucleus test in vivo
- Short description of test conditions: Animals are exposed to the test substance by an appropriate route (gavage). Bone marrow is collected, prepared and stained. Each treated and control group must include at least 5 analysable animals per sex.
- Parameters analysed / observed: Preparations are analyzed for the presence of micronuclei, which detects damage induced by the test substance to the chromosomes or the mitotic apparatus of erythroblasts, by analysis of erythrocytes
The results of this test are detailed within Genetic Toxicity (section 7.6)

GLP compliance:

yes (incl. QA statement)

Limit test:

no

Test material

Test animals

Species:

rat

Strain:

Wistar

Details on species / strain selection:

The Wistar Han rat - Crl: WI(Han) - was chosen as the animal model for this study as it is an accepted rodent species for toxicity testing by regulatory agencies. Charles River Den Bosch has general and reproduction/developmental and micronucleus (bone marrow) historical data in this species from the same strain and source. This animal model has been proven to be susceptible to the effects of reproductive toxicants.

Sex:

male/female

Details on test animals or test system and environmental conditions:

TEST ANIMALS
- Source: Charles River Deutschland, Sulzfeld, Germany
- Females (if applicable) nulliparous and non-pregnant: not reported but may be assumed
- Age at study initiation: Males 11-12 weeks old; Females 13-14 weeks old
- Weight at study initiation: Females 191-243g
- Fasting period before study: not reported
- Housing: On arrival and following the pretest (females only) and pre-mating period, animals were group housed (up to 5 animals of the same sex and same dosing group together) in polycarbonate cages (Makrolon, MIV type, height 18 cm).
Positive control males were group housed (up to 5 animals) in polycarbonate cages (Makrolon, MIV type, height 18 cm).
During the mating phase, males and females were cohabitated on a 1:1 basis in Makrolon plastic cages (MIII type, height 18 cm).
During the post-mating phase, males were housed in their home cage (Makrolon plastic cages, MIV type, height 18 cm) with a maximum of 5 males/cage. Females were individually housed in Makrolon plastic cages (MIII type, height 18 cm).
During the lactation phase, females were housed in Makrolon plastic cages (MIII type, height 18 cm). Pups were housed with the dam, except during locomotor activity monitoring of the dams, when the pups were kept warm in their home cage using bottles filled with warm water.
In order to avoid hypothermia of pups, pups were not left without their dam or a bottle filled with warm water for longer than 30-40 minutes.
During locomotor activity monitoring, animals were housed individually in a Hi-temp polycarbonate cage (Ancare corp., USA; dimensions: 48.3 x 26.7 x 20.3 cm) without cage- enrichment, bedding material, food and water.
The cages contained appropriate bedding (Lignocel S 8-15, JRS - J.Rettenmaier & Söhne GmbH + CO. KG, Rosenberg, Germany) and were equipped with water bottles. The room in which the animals were kept was documented in the study records.
Animals were separated during designated procedures/activities.
Each cage was clearly labeled with a color-coded cage card indicating Test Facility Study No., group, animal number(s), and sex.
- Diet (e.g. ad libitum): Pelleted rodent diet (SM R/M-Z from SSNIFF® Spezialdiäten GmbH, Soest, Germany) was provided ad libitum throughout the study, except during designated procedures. During motor activity measurements, animals had no access to food for a maximum of 2 hours.
- Water (e.g. ad libitum): Municipal tap water was freely available to each animal via water bottles. During motor activity measurements, animals had no access to water for a maximum of 2 hours.
- Acclimation period: The animals were allowed to acclimate to the Test Facility toxicology accommodation for 6 days prior to start of the pretest period.

DETAILS OF FOOD AND WATER QUALITY: The feed was analyzed by the supplier for nutritional components and environmental contaminants. Results of the analysis were provided by the supplier and are on file at the Test Facility.
It is considered that there were no known contaminants in the feed that would interfere with the objectives of the study. Periodic analysis of the water was performed, and results of these analyses are on file at the Test Facility.
It is considered that there were no known contaminants in the water that would interfere with the objectives of the study.

ENVIRONMENTAL CONDITIONS
- Temperature (°C): 21˚C
- Humidity (%): 48-74%
- Air changes (per hr): 10 or more, with 100% fresh air (no recirculation)
- Photoperiod (hrs dark / hrs light): 12/12h

IN-LIFE DATES: From: 04 August 2020 To: 07 October 2020

Administration / exposure

Route of administration:

oral: gavage

Details on route of administration:

Oral, by gastric gavage

Vehicle:

DMSO

Details on oral exposure:

PREPARATION OF DOSING SOLUTIONS:

VEHICLE
- Justification for use and choice of vehicle (if other than water): Dimethyl sulfoxide (DMSO). Trial preparations were performed to select the suitable vehicle and to establish a suitable formulation procedure. These trials were not performed as part of this study and these preparations were not used for dosing. Raw data of these trials will be retained by the Test Facility.

FORMULATION PREPARATION
Test item dosing formulations (w/w) were homogenized to visually acceptable levels at appropriate concentrations to meet dose level requirements. The dosing formulations were prepared daily as a solution and dosed within 6 hours after adding the vehicle to the test item.
Test item dosing formulations were kept at room temperature until dosing. If practically possible, the dosing formulations and vehicle were continuously stirred until and during dosing.
Adjustment was made for specific gravity of the vehicle and test item. No correction was made for the purity/composition of the test item

Analytical verification of doses or concentrations:

yes

Details on analytical verification of doses or concentrations:

Within a separate study (test facility No. 20257162), development and validation of an analytical method for the quantitative analysis of Fatty acids, C18 (unsaturated), reaction products with diethylenetriamine in propylene glycol including trial formulation analysis to confirm the accuracy, homogeneity, stability and resuspension was undertaken.

The analytical method was validated for the analysis of Fatty acids, C18 (unsaturated), reaction products with diethylenetriamine in propylene glycol for the following parameters: i) Specificity, ii) Calibration curve, iii) Accuracy and Repeatability, iv) Limit of quantification, v) Stability of analytical system and end solutions.
Stability of stock solutions in methanol was demonstrated in Test Facility Study No. 491557 to be at least 4 days at room temperature. The stability of stock solutions was therefore not determined during this study.

Formulation Analysis: The concentrations analyzed in the formulations at 1 mg/mL and 200 mg/mL were in agreement with target concentrations (i.e. mean accuracies between 90 and 110%). It was observed that dissolving formulation samples in methanol took time.
The formulations were homogeneous (i.e. coefficient of variation ≤ 5%).
Formulations were stable when stored at room temperature under normal laboratory light conditions for at least 24 hours, in a refrigerator (2-8°C) for at least 8 days, and in a freezer (≤ -15°C) for at least 21 days (3 weeks).
Resuspension homogeneity was demonstrated (i.e. coefficient of variation ≤ 5%).

Within the main study, dose formulations samples were collected on Week 1 of treatment (day 1) and week 4 of treatment (day 22). The method development study demonstrated that the test item is stable in the vehicle when prepared and stored under the same conditions at concentrations bracketing those used in the present study. Samples were tested from all groups for concentration, and from groups 2 & 4 (50mg/kg/day and 650mg/kg/day) for homogeneity.

Duplicate sets of samples (approximately 500 mg) for each sampling time point were sent to the analytical laboratory. Concentration results were considered acceptable if mean sample concentration results were within or equal to ±10% for solutions of target concentration. The concentrations analyzed in the formulations of Groups 2, 3 and 4 (50, 150 & 650mg/kg/day, respectively) were in agreement with target concentrations (i.e. mean accuracies between 90% and 110%). No test item was detected in the Group 1 formulations (vehicle control).

Duplicate sets of samples (approximately 500 mg) for each sampling time point were sent to the analytical laboratory. Homogeneity results were considered acceptable if the coefficient of variation (CV) of concentrations was ≤10%. The formulations of Group 2 and Group 4 were homogeneous (i.e. coefficient of variation ≤ 10%).

Duration of treatment / exposure:

The test item and vehicle were administered to the appropriate animals for a minimum of 28 days as follows: i) Males were treated for 29 days, up to and including the day before scheduled necropsy. This included a minimum of 14 days prior to mating and during the mating period. ii) Females that delivered were treated for 50-64 days, i.e. 14 days prior to mating (with the objective to cover at least two complete estrous cycles), the variable time to conception, the duration of pregnancy and at least 13 days after delivery, up to and including the day before scheduled necropsy. iii) Females which failed to deliver were treated for 41-44 days.

Frequency of treatment:

once by daily oral gavage 7 days a week

Doses / concentrationsopen allclose all

No. of animals per sex per dose:

10 male, 10 female

Control animals:

yes, concurrent vehicle

Details on study design:

- Dose selection rationale:
The oral route of administration selected because this is a possible route of human exposure during manufacture, handling or use of the test item. The dose levels were selected based on the results of a 10 Day Dose Range Finder with oral administration of N-Phenyl-diethanolamine, reaction products with formaldehyde in rats (see accompanying entry), and in an attempt to produce graded responses to the test item. Dose level spacing was selected in consultation with the Sponsor, and in agreement with OECD 422 testing requirements.

- Rationale for animal assignment (if not random): N/A
- Fasting period before blood sampling for clinical biochemistry: F0 males were fasted overnight with a maximum of 24 hours before blood sampling, but water was available. F0 females were not fasted overnight.
- Rationale for selecting satellite groups: N/A
- Post-exposure recovery period in satellite groups: N/A
- Section schedule rationale (if not random): N/A
- Other: N/A

Examinations

Observations and examinations performed and frequency:

CAGE SIDE OBSERVATIONS: Yes
- Time schedule: Twice daily, morning & end of working day.

DETAILED CLINICAL OBSERVATIONS: Yes
- Time schedule: daily, 30 minutes ± 15 minutes post-dose.

BODY WEIGHT: Yes
- Time schedule for examinations: individually on the first day of treatment (prior to dosing), and weekly thereafter

FOOD CONSUMPTION AND COMPOUND INTAKE (if feeding study):
- Food consumption for each animal determined and mean daily diet consumption calculated as g food/kg body weight/day: Yes
- Compound intake calculated as time-weighted averages from the consumption and body weight gain data: N/A

FOOD EFFICIENCY: No

WATER CONSUMPTION AND COMPOUND INTAKE (if drinking water study): Water consumption was monitored on regular basis throughout the study by visual inspection of the water bottles.

OPHTHALMOSCOPIC EXAMINATION: No

Samples for clinical pathology evaluation were collected as per table No. 01

HAEMATOLOGY: Yes
- Time schedule for collection of blood: Day of necropsy between 7.00 and 10.30 a.m., from the retro-orbital sinus under anesthesia using isoflurane
- Animals fasted: F0 males were fasted overnight with a maximum of 24 hours before blood sampling, but water was available. F0 females were not fasted overnight.
- How many animals: 5/sex/group
- Parameters checked in table [No.02] were examined.

CLINICAL CHEMISTRY: Yes
- Time schedule for collection of blood: Day of necropsy between 7.00 and 10.30 a.m., from the retro-orbital sinus under anesthesia using isoflurane
- Animals fasted: F0 males were fasted overnight with a maximum of 24 hours before blood sampling, but water was available. F0 females were not fasted overnight.
- How many animals: 5/sex/group
- Parameters checked in table [No.03] were examined.

PLASMA/SERUM HORMONES/LIPIDS: Yes - serum for T4 thyroid & TSH thyroid stimulating hormone
- Time of blood sample collection: Day of necropsy between 7.00 and 10.30 a.m., from the retro-orbital sinus under anesthesia using isoflurane
- Animals fasted: F0 males were fasted overnight with a maximum of 24 hours before blood sampling, but water was available. F0 females were not fasted overnight.
- How many animals: All F0 animals. Initial analysis only conducted for male animals.

URINALYSIS: No

NEUROBEHAVIOURAL EXAMINATION: Yes
- Time schedule for examinations: 5 males/dose during Week 4 of treatment and the 5 females/dose during the last week of lactation (i.e. PND 6-13). Tests were performed after dosing, after completion of clinical observations.
- Dose groups that were examined: All dose groups.
- Battery of functions tested: sensory activity (hearing ability, pupillary reflex) / grip strength / motor activity / static righting reflex

IMMUNOLOGY: No

OTHER:

COAGULATION:
- Time schedule for collection of blood: Day of necropsy between 7.00 and 10.30 a.m., from the retro-orbital sinus under anesthesia using isoflurane
- Animals fasted: F0 males were fasted overnight with a maximum of 24 hours before blood sampling, but water was available. F0 females were not fasted overnight.
- How many animals: 5/sex/group
- Parameters checked in table [No.04] were examined.

Sacrifice and pathology:

Terminal procedures, organs weighed, and tissue collection/preservation are outlined in table 05-07.

GROSS PATHOLOGY: Yes for selected animals (see table 08)

HISTOPATHOLOGY: Yes for selected animals (see table 09)

Optional endpoint(s):

Optional endpoints: No

Statistics:

The reviewer considers the analyses used (detailed in table 10) to be appropriate.

Results and discussion

Results of examinations

Clinical signs:

effects observed, treatment-related

Description (incidence and severity):

At 650 mg/kg/day, lethargy and flat posture were recorded for 8 out of 10 males and all females, and for each of these animals these signs occurred on a few days during treatment. Most of these animals also showed hunched posture, rales, piloerection, uncoordinated movements and/or ptosis on a few days during treatment.
At 150 mg/kg/day, flat posture was noted for one male and two females on treatment Days 12 and/or 13 only. One female at 150 mg/kg/day showed hunched posture, labored respiration, rales and/or piloerection during the last three days of treatment.
One female each at 50 and 150 mg/kg/day showed piloerection on two or three consecutive days during the 6th treatment week. As the incidence was similar or even less than encountered in the control group where two females showed piloerection (including hunched posture), these were considered not to be related to treatment with the test item.
Salivation seen after dosing among animals of the 50, 150 and 650 mg/kg/day dose groups with a dose-related trend during the treatment period was considered not toxicologically relevant, taking into account the nature and minor severity of the effect and its time of occurrence (i.e. after dosing). This sign was considered to be a physiological response rather than a sign of systemic toxicity and is a common occurrence in oral gavage studies.
Any other clinical signs noted during the treatment period occurred within the range of background findings to be expected for rats of this age and strain which are housed and treated under the conditions in this study and did not show any apparent dose-related trend. At the incidence observed, these were considered to be unrelated to treatment with the test item.
Clinical observations outlined in full within Appendix 1 (summary) and 2 (individual) in attached study results file.

Mortality:

no mortality observed

Body weight and weight changes:

effects observed, treatment-related

Description (incidence and severity):

Bodyweight (gram) is summarised in table 11. Bodyweight gain is summarised in table 12. At 650 mg/kg/day, mean body weight gain of males was statistically significantly lower throughout the treatment period (mean weight gain at the end of the treatment period was 0.5x of control). Five of these males (Nos. 32, 33, 37, 38 and 39) showed a temporary and minimal weight loss during the first, second and/or third treatment week, ranging between 2 and 6% absolute weight loss over the respective period. Overall weight gain of most of these animals over the treatment period was also slightly lower with 6 to 7% vs 10 to 16% for the other animals within this group. Other male body weight variations at this dose level occurred within the range encountered for control animals.
At 650 mg/kg/day, mean body weight gain of females was lower throughout the lactation period (0.67x of control at the end of lactation; not statistically significant). In particular, Female (No. 79) showed no to minimal weight gain over the lactation period (1% over lactation Days 1 to 13). One other female at this dose level showed weight loss over lactation Days 1 to 7 (up to 13% of lactation Day 1 body weight).Overall, body weights and body weight gain at 50 and 150 mg/kg/day were considered not affected by treatment with the test item.

Food consumption and compound intake (if feeding study):

effects observed, non-treatment-related

Description (incidence and severity):

Food consumption is summarised in table 13, bodyweight consumption corrected for bodyweight is summarised in table 14. At 650 mg/kg/day, a lower food consumption (before and after correction for body weight) was recorded for males during the first three weeks of treatment (up to 0.85x of control). Overall mean food intake after correction for body weight was however similar to the control mean.
For females at 650 mg/kg/day, slightly lower mean food intake was only noted over Days 7 to 13 of lactation. This was ascribed to a reduced food intake of one female (No. 79). It is notable that this female only delivered two pups, and as a result presumably had a lower food consumption requirement. As this observation was isolated to one animal, the overall lowered group mean food intake was therefore considered not to be related to treatment with the test item.
Absolute and relative food consumption at 50 and 150 mg/kg/day was considered not affected by treatment with the test item.

Food efficiency:

not examined

Water consumption and compound intake (if drinking water study):

not examined

Ophthalmological findings:

not examined

Haematological findings:

effects observed, treatment-related

Description (incidence and severity):

Hematology is summarised in table 15. At 650 mg/kg/day, the following (statistically significant) changes in hematological parameters were recorded: i) Higher white blood cell counts (WBC) in males and females (1.46x and 1.34x of control, respectively); ii) Higher neutrophil counts (NEUT) in males and females (2.13x and 1.33x of control, respectively; not statistically significant for females); iii) Higher lymphocyte counts (LYMPH) in males and females (each 1.34x of control; not statistically significant for females); iv) Lower red blood cell counts (RBC) in males (0.94x of control); v) Higher reticulocyte counts (RETIC) in males (1.33x of control); vi) Lower hemoglobin (HGB) in males (0.94x of control); and vii) Lower mean corpuscular hemoglobin concentration (MCHC) in males (0.97x of control).
At 150 and 650 mg/kg/day, lower mean corpuscular hemoglobin (MCH) was recorded for females (each 0.95x of control), but in absence of correlating changes in red blood cell parameters or histopathological changes, and absence of a clear dose-related trend, this was considered not to be related to treatment with the test item.

Clinical biochemistry findings:

effects observed, treatment-related

Description (incidence and severity):

Clinical biochemistry is summarised in table 16. At 650 mg/kg/day, the following (statistically significant) changes in clinical biochemistry parameters were recorded: i) Higher total bilirubin (TBIL) in males (1.59x of control); ii) Higher urea in males (1.38x of control); iii) Higher bile acid (BILEAC) in males (2.22x of control, not statistically significant); iv) Lower total bilirubin (TBIL) in females (0.76x of control, not statistically significant).
At 50 and 150 mg/kg/day, clinical biochemistry parameters were considered not affected by treatment with the test item.

Endocrine findings:

no effects observed

Description (incidence and severity):

Serum levels of T4 in F0 males were considered unaffected by treatment with the test item up to 650 mg/kg/day.

Urinalysis findings:

not examined

Behaviour (functional findings):

effects observed, non-treatment-related

Description (incidence and severity):

Functional observations are summarised in table 17. At 650 mg/kg/day, mean ambulation counts of males appeared higher (1.28x of control, not statistically significant). This was ascribed to higher activity of two out of five males (Nos. 31 and 33).
For females at 50 and 650 mg/kg/day, mean total movements and ambulations appeared lower than control means (not statistically significant). However, control means for both parameters exceeded the historical control range while means of these parameters at 50 and
650 mg/kg/day were well within this range. In addition, the expected decreasing trend in motor activity over the duration of the test period (habituation profile) of control females was less apparent, in particular for total movements. It could not be ascertained what factors may have attributed to this. Motor activity habituation profile of control males followed the expected pattern. In absence of a dose-related trend, these variations over the dose groups were considered not to be related to treatment with the test item.
At 50 and 150 mg/kg/day, motor activity was considered not to be affected by treatment with the test item. All male groups (including the 650 mg/kg/day group) showed a similar motor activity habituation profile with a decreasing trend in activity over the duration of the test period.
Hearing ability, pupillary reflex, static righting reflex were normal in all examined animals up to 650 mg/kg/day. Grip strength was considered not affected by treatment with the test item.

Immunological findings:

not examined

Organ weight findings including organ / body weight ratios:

effects observed, treatment-related

Description (incidence and severity):

Absolute organ weights are summarised in table 18. Relative organ weights are summarised in table 19. Test item-related higher liver and spleen weights (absolute and relative to body weights) were noted in the 650 mg/kg/day group males. A statistically significant higher liver weight (absolute and relative to body weight) was recorded for males at 650 mg/kg/day. A statistically significant higher spleen weight (absolute and relative to body weight) was recorded for males at 650 mg/kg/day. Some organ weight differences in males were statistically significant when compared to the control group (relative brain and kidney weight at 650 mg/kg/day), which were considered to be the result of a test item-related effect on final body weight. The relatively high kidney weight of one male at 650 mg/kg/day (No. 32) was not associated with kidney lesions that discerned this animal from other animals within this dose group and that would support this higher kidney weight. This higher kidney weight was therefore considered unrelated to treatment with the test item.
There were no other test item-related organ weight changes, including in females.

Gross pathological findings:

effects observed, treatment-related

Description (incidence and severity):

Gross pathology (macroscopic findings) are summarised in table 21. Test item-related macroscopic findings were present in the stomach of males and females treated at 650 mg/kg/day. These findings consisted of: i) Crateriform retractions (black and hard) in the forestomach in 9/10 males and 4/10 females and thickened limiting ridge in 10/10 males and 4/10 females. The microscopic correlate was ulcerative inflammation of the forestomach with transmural necrosis. ii) Reddish focus/foci in the glandular stomach in 5/10 males. The microscopic correlate was mucosal hemorrhage.
The remainder of the recorded macroscopic findings were within the range of background gross observations encountered in rats of this age and strain.

Neuropathological findings:

not examined

Histopathological findings: non-neoplastic:

effects observed, treatment-related

Description (incidence and severity):

Histopathological (microscopic) findings are summarised in tables 22 & 23. Test item-related microscopic findings after treatment with the test item were noted in the stomach and spleen of males and females and in kidneys and liver of males. Stomach-forestomach: Ulcerative inflammation (up to massive degree) and transmural necrosis (slight or marked degree) was observed in the forestomach of males and females at 650 mg/kg/day. The ulcers were large and were accompanied by inflammation (mostly in the submucosa and/or at the serosal side) and large necrotic areas throughout all layers of the forestomach (transmural).

Stomach-glandular stomach: In the glandular stomach of two males and a single female at 650 mg/kg/day, an ulcer or erosion (slight degree) was observed and submucosal inflammation was noted to be slightly above background (minimal inflammation is considered background). In a few males (a single male at 50 mg/kg/day and three males at 650 mg/kg/day) hemorrhages were observed which correlated at 650 mg/kg/day with reddish focus/foci in the glandular stomach.

Spleen: A dose-dependent increase in incidence and severity in extramedullary hematopoiesis was observed in males starting at 50 mg/kg/day, up to slight degree. Pigmentation was increased in severity in males and females treated at 650 mg/kg/day, up to slight degree. Liver: A dose-dependent increased incidence of minimal hepatocellular centrilobular hypertrophy was observed in males starting at 150 mg/kg/day.

Kidney: A combination of tubular findings was observed in kidneys of males treated at 150 and 650 mg/kg/day consisting of increased incidence and severity of tubular basophilia up to marked degree, presence of granular casts up to slight degree and degeneration of tubular epithelial cells up to moderate degree.
There were no other test item-related histologic changes. The remainder of the recorded microscopic findings were within the range of background pathology encountered in rats of this age and strain.

Other effects:

effects observed, non-treatment-related

Description (incidence and severity):

Coagulation: At 150 and 650 mg/kg/day, lower activated partial thromboplastin time (APTT) was recorded for males (0.80x and 0.78x of control, respectively).
The statistically significantly lower prothrombin time (PT) of males at 50 and 150 mg/kg/day occurred in the absence of a dose-related trend and was therefore considered not related to treatment with the test item. Coagulation is summarised in table 20.

Effect levels

Target system / organ toxicity

Any other information on results incl. tables

Table 11: Summary bodyweights (gram) 

BODY WEIGHTS MALES	(GRAM) SUMMARY
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING
DAY 1	MEAN	312	330 *	325	318
WEEK 1	ST.DEV	14.6	11.5	17.4	8.1
	N	10	10	10	10
DAY 8	MEAN	338	341	340	321 *
WEEK 2	ST.DEV	11.6	8.6	18.7	12.3
	N	10	10	10	10
MATING PERIOD
DAY 1	MEAN	359	364	361	339 *
WEEK 1	ST.DEV	12.8	12.5	21.6	17.0
	N	10	10	10	10
DAY 8	MEAN	369	373	373	344 *
WEEK 2	ST.DEV	11.7	15.0	25.9	19.0
	N	10	10	10	10
DAY 15	MEAN	381	383	383	354 **
WEEK 3	ST.DEV	12.9	15.5	27.4	15.6
	N	10	10	10	10

 

BODY WEIGHTS FEMALES	(GRAM) SUMMARY
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING
DAY 1	MEAN	220	217	216	225
WEEK 1	ST.DEV	9.6	13.6	12.4	13.4
	N	10	10	10	10
DAY 8	MEAN	221	216	220	227
WEEK 2	ST.DEV	8.3	14.6	10.1	12.5
	N	10	10	10	10
MATING PERIOD
DAY 1	MEAN	227	225	227	231
WEEK 1	ST.DEV	10.4	13.2	8.0	12.9
	N	10	10	10	10
DAY 8 WEEK 2	MEAN	247 --- 1	0 x	0 x
	ST.DEV
	N
DAY 15 WEEK 3	MEAN		--- --- 0 x	--- --- 0 x
	ST.DEV
DAY 22 WEEK 4	MEAN		--- --- 0 x	--- --- 0 x
	ST.DEV
	N

FEMALES F0-GENERATION

		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
POST COITUM
DAY 0	MEAN	232	227	223	231
	ST.DEV.	10.8	16.8	7.0	12.9
	N	9	9	9	9
DAY 4	MEAN	244	238	239	243
	ST.DEV.	8.1	17.2	7.7	12.4
	N	9	9	9	9
DAY 7	MEAN	249	245	247	250
	ST.DEV.	8.5	17.7	8.4	11.1
	N	9	9	9	9
DAY 11	MEAN	263	258	263	264
	ST.DEV.	6.2	21.3	10.1	12.5
	N	9	9	9	9
DAY 14	MEAN	273	270	274	272
	ST.DEV.	8.5	19.7	13.1	13.6
	N	9	9	9	9
DAY 17	MEAN	298	293	297	294
	ST.DEV.	7.5	20.5	15.7	19.3
	N	9	9	9	9
DAY 20	MEAN	337	329	337	328
	ST.DEV.	8.3	21.5	24.3	31.0
	N	9	9	9	9
LACTATION
DAY 1	MEAN	262	254	263	266
	ST.DEV.	8.0	21.3	14.7	12.1
	N	7	10	10	9
DAY 4	MEAN	277	267	276	272
	ST.DEV.	5.3	21.3	14.0	12.8
	N	9	10	10	9
DAY 7	MEAN	278	275	285	274
	ST.DEV.	14.8	19.5	15.0	13.5
	N	8	10	10	8
DAY 13	MEAN	302	295	297	293
	ST.DEV.	7.8	26.6	20.0	16.3
	N	9	10	10	9

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

x Explanations for excluded data are listed in the tables of the individual values (see attached additional study reporting)

Note to clinical signs tables: For males, “Repro period” represents the mating phase. For females, “Repro period” represents the mating, post‑coitum and lactation phase.

 

Table 12: Bodyweight gain (%) summary

BODY WEIGHT GAIN (%) SUMMARY MALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING DAY 1	MEAN	0	0	0	0
WEEK 1	ST.DEV	0.0	0.0	0.0	0.0
	N	10	10	10	10
DAY 8	MEAN	8	3 **	5 **	1 **
WEEK 2	ST.DEV	2.7	2.0	1.5	2.6
	N	10	10	10	10
MATING PERIOD DAY 1	MEAN	15	10 **	11 **	6 **
WEEK 1	ST.DEV	2.7	2.2	1.2	4.0
	N	10	10	10	10
DAY 8	MEAN	18	13 **	15	8 **
WEEK 2	ST.DEV	3.4	3.2	2.3	5.0
	N	10	10	10	10
DAY 15	MEAN	22	16 **	18 *	11 **
WEEK 3	ST.DEV	4.1	3.3	2.7	3.6
	N	10	10	10	10
BODY WEIGHT GAIN (%)SUMMARY FEMALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING DAY 1	MEAN	0	0	0	0
WEEK 1	ST.DEV	0.0	0.0	0.0	0.0
	N	10	10	10	10
DAY 8	MEAN	1	0	2	1
WEEK 2	ST.DEV	3.3	1.5	3.6	2.5
	N	10	10	10	10
MATING PERIOD DAY 1	MEAN	4	4	5	3
WEEK 1	ST.DEV	3.4	2.9	4.1	3.4
	N	10	10	10	10
DAY 8 WEEK 2	MEAN ST.DEV N	13 --- 1	--- --- 0 x	--- --- 0 x
DAY 15 WEEK 3	MEAN ST.DEV N		--- --- 0 x	--- --- 0 x
DAY 22 WEEK 4	MEAN ST.DEV N		--- --- 0 x	--- --- 0 x
BODY WEIGHT GAIN (%)SUMMARY FEMALES F0-GENERATION
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
POST COITUM DAY 0	MEAN	0	0	0	0
	ST.DEV.	0.0	0.0	0.0	0.0
	N	9	9	9	9
DAY 4	MEAN	5	5	7	5
	ST.DEV.	2.8	1.6	1.9	1.9
	N	9	9	9	9
DAY 7	MEAN	7	8	11 **	8
	ST.DEV.	3.2	1.5	2.7	1.7
	N	9	9	9	9
DAY 11	MEAN	14	13	18 *	14
	ST.DEV.	3.9	2.7	2.9	2.5
	N	9	9	9	9
DAY 14	MEAN	18	19	23 **	18
	ST.DEV.	2.9	2.4	4.0	3.2
	N	9	9	9	9
DAY 17	MEAN	28	29	33	27
	ST.DEV.	5.2	2.9	5.3	5.1
	N	9	9	9	9
DAY 20	MEAN	45	45	51	42
	ST.DEV.	7.5	5.1	8.3	9.5
	N	9	9	9	9
LACTATION DAY 1	MEAN	0	0	0	0
	ST.DEV.	0.0	0.0	0.0	0.0
	N	7	10	10	9
DAY 4	MEAN	5	5	5	2
	ST.DEV.	2.9	5.4	2.9	3.7
	N	7	10	10	9
DAY 7	MEAN	5	9	8	3
	ST.DEV.	6.7	6.4	3.4	7.5
	N	6	10	10	8
DAY 13	MEAN	15	16	13	10
	ST.DEV.	5.1	7.6	5.7	5.2
	N	7	10	10	9

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

x Explanations for excluded data are listed in the tables of the individual values (see attached additional study reporting)

Note to clinical signs tables: For males, “Repro period” represents the mating phase. For females, “Repro period” represents the mating, post‑coitum and lactation phase

 

Table 13: Absolute Food consumption (g/animal/day) summary

FOOD CONSUMPTION (G/ANIMAL/DAY) SUMMARY  MALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING DAYS 1-8	MEAN	25	25	25	22
WEEKS 1-2	ST.DEV	0.2	0.5	0.5	0.6
	N (CAGE)	2	2	2	2
DAYS 8-15	MEAN	24	24	24	22
WEEKS 2-3	ST.DEV	0.0	0.0	1.4	1.5
	N (CAGE)	2	2	2	2
MEAN OF MEANS OVER PRE MATI...	MEAN	24	24	25	22
MATING PERIOD DAYS 1-8	MEAN	26	27	26	22
WEEKS 1-2	ST.DEV	1.5	1.9	1.9	1.1
	N (CAGE)	2	2	2	2
DAYS 8-15	MEAN	26	25	26	25
WEEKS 2-3	ST.DEV	0.1	0.7	1.0	0.5
	N (CAGE)	2	2	2	2
MEAN OF MEANS OVER MATING P...	MEAN	26	26	26	24
FOOD CONSUMPTION (G/ANIMAL/DAY) SUMMARY FEMALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
PRE MATING DAYS 1-8	MEAN	17	17	18	17
WEEKS 1-2	ST.DEV	0.6	0.1	0.2	2.3
	N (CAGE)	2	2	2	2
DAYS 8-15	MEAN	17	16	17	17
WEEKS 2-3	ST.DEV	0.2	0.4	0.1	1.2
	N (CAGE)	2	2	2	2
MEAN OF MEANS OVER PRE MATI...	MEAN	17	17	17	17
FOOD CONSUMPTION (G/ANIMAL/DAY) SUMMARY FEMALES F0-GENERATION
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
POST COITUM DAYS 0-4	MEAN	18	18	20	19
	ST.DEV.	1.4	3.1	2.0	1.9
	N	9	9	9	9
DAYS 4-7	MEAN	21	21	22	21
	ST.DEV.	1.5	2.8	2.3	1.5
	N	9	9	9	9
DAYS 7-11	MEAN	22	22	24	22
	ST.DEV.	1.6	3.4	2.9	1.9
	N	9	9	9	9
DAYS 11-14	MEAN	23	22	24	23
	ST.DEV.	2.2	2.5	2.7	1.1
	N	9	9	9	9
DAYS 14-17	MEAN	23	22	24	23
	ST.DEV.	1.9	2.9	2.4	2.4
	N	9	9	9	9
DAYS 17-20	MEAN	24	24	25	25
	ST.DEV.	1.5	2.7	2.9	1.7
	N	9	9	9	9
MEAN OF MEANS		22	22	23	22
LACTATION DAYS 1-4	MEAN	32	30	32	32
	ST.DEV.	3.2	4.4	5.2	9.4
	N	9	10	10	9
DAYS 4-7	MEAN	47	42	43	40
	ST.DEV.	9.1	5.4	4.5	9.6
	N	9	10	10	8
DAYS 7-13	MEAN	54	55	53	47
	ST.DEV.	6.5	7.4	6.3	9.6
	N	9	10	10	9
MEAN OF MEANS		44	42	43	40

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

x Explanations for excluded data are listed in the tables of the individual values (see attached additional study reporting)

Note to clinical signs tables: For males, “Repro period” represents the mating phase. For females, “Repro period” represents the mating, post‑coitum and lactation phase

 

Table 14: Relative Food consumption (g/animal/day) summary

RELATIVE FOOD CONSUMPTION (G/KG BODY WEIGHT/DAY)SUMMARY MALES
				GROUP 1 CONTROL		GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
PRE MATING DAYS 1-8		MEAN		73		72		74		68
WEEKS 1-2		ST.DEV		0.3		2.5		0.4		0.7
		N (CAGE)		2		2		2		2
DAYS 8-15		MEAN		71		71		72		70
WEEKS 2-3		ST.DEV		0.2		0.9		2.5		3.2
		N (CAGE)		2		2		2		2
MEAN OF MEANS OVER PRE MATI...		MEAN		72		72		73		69
MATING PERIOD DAYS 1-8		MEAN		70		73		71		65
WEEKS 1-2		ST.DEV		4.7		6.9		1.7		1.1
		N (CAGE)		2		2		2		2
DAYS 8-15		MEAN		67		65		69		69
WEEKS 2-3		ST.DEV		1.3		0.6		0.7		0.5
		N (CAGE)		2		2		2		2
MEAN OF MEANS OVER MATING PERIOD		MEAN		69		69		70		67
RELATIVE FOOD CONSUMPTION (G/KG BODY WEIGHT/DAY) FEMALES
				GROUP 1 CONTROL		GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
PRE MATING DAYS 1-8		MEAN		77		77		80		73
WEEKS 1-2		ST.DEV		3.1		0.9		0.0		9.1
		N (CAGE)		2		2		2		2
DAYS 8-15		MEAN		75		76		78		75
WEEKS 2-3		ST.DEV		1.3		2.1		1.2		4.2
		N (CAGE)		2		2		2		2
MEAN OF MEANS OVER PRE-MATING PERIOD		MEAN		76		77		79		74
RELATIVE FOOD CONSUMPTION (G/KG BODY WEIGHT/DAY) F0-GENERATION
			GROUP 1 CONTROL		GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
POST COITUM DAYS 0-4	MEAN		74		77		83		77
	ST.DEV.		7.0		9.1		6.9		7.4
	N		9		9		9		9
DAYS 4-7	MEAN		84		85		89		86
	ST.DEV.		6.8		8.1		7.3		6.3
	N		9		9		9		9
DAYS 7-11	MEAN		83		84		89		85
	ST.DEV.		7.1		9.2		8.2		6.7
	N		9		9		9		9
DAYS 11-14	MEAN		83		82		89		86
	ST.DEV.		8.8		7.4		7.5		4.8
	N		9		9		9		9
DAYS 14-17	MEAN		77		76		81		78
	ST.DEV.		6.7		5.6		5.3		7.2
	N		9		9		9		9
DAYS 17-20	MEAN		73		73		76		77
	ST.DEV.		3.7		6.6		5.5		5.7
	N		9		9		9		9
MEAN OF MEANS			79		80		84		81
RELATIVE FOOD CONSUMPTION (G/KG BODY WEIGHT/DAY) LACTATION
DAYS 1-4	MEAN		115		111		116		116
	ST.DEV.		12.4		12.4		15.6		35.5
	N		9		10		10		9
DAYS 4-7	MEAN		164		152		150		144
	ST.DEV.		38.8		15.6		13.2		38.7
	N		8		10		10		7
DAYS 7-13	MEAN		179		187		180		161
	ST.DEV.		20.6		17.0		16.5		27.9
	N		9		10		10		9
MEAN OF MEANS			153		150		149		140

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

x Explanations for excluded data are listed in the tables of the individual values (see attached additional study reporting)

Note to clinical signs tables: For males, “Repro period” represents the mating phase. For females, “Repro period” represents the mating, post‑coitum and lactation phase

 

Table 15: Summary of hematology values: F0 Generation

MALES: day 30 relative to start

Sex: Male		Reporting Hematology
		WBC (10^9/L) [G]	NEUT (10^9/L) [G]	LYMPH (10^9/L) [G1]	MONO (10^9/L) [G]	EOS (10^9/L) [G]	BASO (10^9/L) [G]	LUC (10^9/L) [G1]	RBC (10^12/L) [G]	RETIC (10^9/L) [G]	RDWG (%) [G]	HGB (g/L) [G]	HCT (L/L) [G]
0	Mean	6.302	0.946	5.148	0.100	0.068	0.014	0.030	8.780	231.88	13.10	155.0	0.4572
mg/kg/day	SD	0.511	0.264	0.290	0.040	0.013	0.005	0.010	0.278	21.44	0.23	3.0	0.0101
Group 1	N	5	5	5	5	5	5	5	5	5	5	5	5
50	Mean	6.482	0.820	5.468	0.090	0.056	0.010	0.032	8.836	202.46	12.94	156.0	0.4580
mg/kg/day	SD	1.672	0.137	1.709	0.032	0.009	0.000	0.027	0.281	32.66	0.72	3.7	0.0087
Group 2	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.03	0.87	1.06	0.90	0.82	0.71	1.07	1.01	0.87	0.99	1.01	1.00
150	Mean	7.796	1.342	6.230	0.092	0.086	0.012	0.028	8.652	246.02	13.06	151.8	0.4504
mg/kg/day	SD	1.224	0.390	1.487	0.026	0.030	0.004	0.008	0.372	26.96	0.27	5.9	0.0197
Group 3	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.24	1.42	1.21	0.92	1.26	0.86	0.93	0.99	1.06	1.00	0.98	0.99
650	Mean	9.230 *	2.014 *	6.904	0.142	0.104	0.020	0.048	8.266 *	307.64 **	13.14	146.4 *	0.4450
mg/kg/day	SD	2.107	0.870	1.215	0.048	0.067	0.007	0.011	0.303	48.43	0.87	5.2	0.0184
Group 4	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.46	2.13	1.34	1.42	1.53	1.43	1.60	0.94	1.33	1.00	0.94	0.97

 

Sex: Male		Reporting Hematology
		MCV (fL) [G]	MCH (pg) [G]	MCHC (g/L) [G]	PLT (10^9/L) [G1]
0	Mean	52.10	17.68	338.8	725.8
mg/kg/day	SD	1.70	0.44	3.0	90.5
Group 1	N	5	5	5	5
50	Mean	51.86	17.64	340.8	754.4
mg/kg/day	SD	1.17	0.59	4.9	68.4
Group 2	N	5	5	5	5
	tCtrl	1.00	1.00	1.01	1.04
150	Mean	52.08	17.54	336.8	757.0
mg/kg/day	SD	0.98	0.15	4.1	27.6
Group 3	N	5	5	5	5
	tCtrl	1.00	0.99	0.99	1.04
650	Mean	53.84	17.76	329.4 **	869.4
mg/kg/day	SD	1.11	0.45	3.8	121.1
Group 4	N	5	5	5	5
	tCtrl	1.03	1.00	0.97	1.20

[G] - Anova & Dunnett: * = p ≤ 0.05

[G1] - Kruskal-Wallis & Dunn

 

FEMALES: Day 51 relative to start date

Sex: Female		Reporting Hematology
		WBC (10^9/L) [G]	NEUT (10^9/L) [G]	LYMPH (10^9/L) [G]	MONO (10^9/L) [G]	EOS (10^9/L) [G]	BASO (10^9/L) [G]	LUC (10^9/L) [G]	RBC (10^12/L) [G]	RETIC (10^9/L) [G]	RDWG (%) [G]	HGB (g/L) [G]	HCT(L/L) [G1]
0	Mean	5.062	1.598	3.278	0.092	0.072	0.008	0.020	6.824	261.04	13.02	140.2	0.4076
mg/kg/day	SD	0.749	0.317	0.518	0.025	0.026	0.004	0.000	0.117	47.87	0.44	3.2	0.0228
Group 1	N	5	5	5	5	5	5	5	5	5	5	5	5
50	Mean	5.536	1.662	3.594	0.124	0.130	0.004	0.020	6.936	238.30	12.90	136.2	0.3978
mg/kg/day	SD	0.901	0.264	0.810	0.040	0.053	0.005	0.022	0.289	37.34	1.02	1.8	0.0090
Group 2	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.09	1.04	1.10	1.35	1.81	0.50	1.00	1.02	0.91	0.99	0.97	0.98
150	Mean	4.770	1.262	3.314	0.096	0.072	0.004	0.024	6.958	210.54	12.72	135.6	0.4012
mg/kg/day	SD	0.780	0.457	0.579	0.027	0.029	0.005	0.026	0.245	59.83	1.02	3.6	0.0080
Group 3	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	0.94	0.79	1.01	1.04	1.00	0.50	1.20	1.02	0.81	0.98	0.97	0.98
650	Mean	6.804 *	2.118	4.382	0.154	0.106	0.012	0.028	7.012	248.92	13.56	136.2	0.3986
mg/kg/day	SD	1.393	0.958	0.636	0.072	0.069	0.004	0.015	0.356	53.85	1.06	1.5	0.0082
Group 4	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.34	1.33	1.34	1.67	1.47	1.50	1.40	1.03	0.95	1.04	0.97	0.98

 

Sex: Female		Reporting Hematology
		MCV (fL) [G]	MCH (pg) [G]	MCHC (g/L) [G]	PLT (10^9/L) [G]
0	Mean	59.74	20.54	344.6	703.2
mg/kg/day	SD	3.39	0.42	13.5	72.5
Group 1	N	5	5	5	5
50	Mean	57.40	19.66	342.6	725.2
mg/kg/day	SD	2.11	0.70	5.7	75.1
Group 2	N	5	5	5	5
	tCtrl	0.96	0.96	0.99	1.03
150	Mean	57.72	19.50 *	337.8	717.0
mg/kg/day	SD	2.03	0.47	4.9	128.4
Group 3	N	5	5	5	5
	tCtrl	0.97	0.95	0.98	1.02
650	Mean	56.90	19.44 *	341.6	737.8
mg/kg/day	SD	2.36	0.84	4.6	108.5
Group 4	N	5	5	5	5
	tCtrl	0.95	0.95	0.99	1.05

 

[G] - Anova & Dunnett: * = p ≤ 0.05

[G1] - Kruskal-Wallis & Dunn

 

Table 16: Summary of clinical chemistry values: F0 Generation

MALES: day 30 relative to start

Sex: Male		Reporting Biochemistry
		ALT (U/L) [G]	AST (U/L) [G]	ALP (U/L) [G]	TPROT (g/L) [G]	ALB (g/L) [G]	BILEAC (umol/L) [G1]	TBIL (umol/L) [G]	UREA (mmol/L) [G]	CREAT (umol/L) [G]	GLUC (mmol/L) [G]	CHOL (mmol/L) [G1]	NA (mmol/L) [G]
0	Mean	53.7	87.8	94.9	61.64	37.80	21.52	2.36	5.83	27.7	8.704	2.118	143.4
mg/kg/day	SD	6.5	10.5	14.1	1.63	1.05	17.56	0.33	0.74	3.6	0.621	0.249	0.5
Group 1	N	5	5	5	5	5	5	5	5	5	5	5	5
50	Mean	47.2	81.1	106.2	62.06	38.22	10.98	2.30	6.08	26.5	8.460	1.860	143.4
mg/kg/day	SD	5.7	3.3	25.4	1.69	0.82	4.21	0.22	0.98	2.6	1.376	0.154	0.5
Group 2	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	0.88	0.92	1.12	1.01	1.01	0.51	0.97	1.04	0.96	0.97	0.88	1.00
150	Mean	58.8	89.3	100.7	60.60	37.36	37.91	2.92	7.09	26.6	9.936	1.924	142.2
mg/kg/day	SD	15.3	12.8	4.6	2.43	1.35	22.33	0.40	1.20	2.9	2.316	0.494	1.1
Group 3	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.09	1.02	1.06	0.98	0.99	1.76	1.24	1.22	0.96	1.14	0.91	0.99
650	Mean	61.5	86.1	83.3	60.58	37.72	47.67	3.76 **	8.06 *	28.4	9.516	2.448	142.0
mg/kg/day	SD	10.9	7.4	13.8	1.36	1.19	22.84	0.51	1.27	3.5	1.792	0.541	1.6
Group 4	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.15	0.98	0.88	0.98	1.00	2.22	1.59	1.38	1.03	1.09	1.16	0.99

 

Sex: Male		Reporting Biochemistry				Reporting S
		K (mmol/L) [G]	CL (mmol/L) [G]	CA (mmol/L) [G]	PHOS (mmol/L) [G]	T4 (ng/mL) [G]
0	Mean	3.91	106.2	2.608	1.958	38.60
mg/kg/day	SD	0.31	1.3	0.072	0.135	6.99
Group 1	N	5	5	5	5	10
50	Mean	4.04	105.8	2.646	1.840	39.68
mg/kg/day	SD	0.12	0.8	0.076	0.222	5.79
Group 2	N	5	5	5	5	10
	tCtrl	1.03	1.00	1.01	0.94	1.03
150	Mean	3.83	105.0	2.584	1.872	44.89
mg/kg/day	SD	0.14	2.0	0.103	0.120	11.30
Group 3	N	5	5	5	5	10
	tCtrl	0.98	0.99	0.99	0.96	1.16
650	Mean	4.19	105.4	2.588	1.852	34.52
mg/kg/day	SD	0.15	1.3	0.095	0.194	4.50
Group 4	N	5	5	5	5	10
	tCtrl	1.07	0.99	0.99	0.95	0.89

[G] - Anova & Dunnett: * = p ≤ 0.05

[G1] - Kruskal-Wallis & Dunn

FEMALES: Day 51 relative to start date

Sex: Female		Reporting Biochemistry
		ALT (U/L) [G]	AST (U/L) [G]	ALP (U/L) [G]	TPROT (g/L) [G]	ALB (g/L) [G]	BILEAC (umol/L) [G]	TBIL (umol/L) [G]	UREA (mmol/L) [G]	CREAT (umol/L) [G]	GLUC (mmol/L) [G]	CHOL (mmol/L) [G]	NA (mmol/L) [G]
0	Mean	129.9	95.7	253.3	56.74	34.96	11.35	2.30	9.72	22.4	7.384	2.134	141.0
mg/kg/day	SD	15.6	5.7	93.1	1.27	1.08	3.20	0.89	0.65	2.7	1.628	0.310	1.2
Group 1	N	5	5	5	5	5	5	5	5	5	5	5	5
50	Mean	138.0	98.5	197.9	54.60	33.74	11.96	2.52	9.69	21.0	8.904	2.160	140.2
mg/kg/day	SD	25.7	7.8	90.2	2.04	0.76	4.30	0.77	0.17	2.2	0.876	0.249	1.3
Group 2	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	1.06	1.03	0.78	0.96	0.97	1.05	1.10	1.00	0.94	1.21	1.01	0.99
150	Mean	122.4	97.2	231.3	55.10	33.98	8.16	2.14	9.72	24.8	8.160	1.866	140.8
mg/kg/day	SD	20.8	11.3	107.9	2.90	1.98	2.61	0.46	0.93	4.1	1.484	0.418	1.3
Group 3	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	0.94	1.02	0.91	0.97	0.97	0.72	0.93	1.00	1.11	1.11	0.87	1.00
650	Mean	120.9	96.2	234.0	55.60	33.80	11.06	1.74	9.13	21.1	8.692	2.230	141.2
mg/kg/day	SD	21.2	14.6	120.3	2.71	1.48	2.02	0.44	0.81	3.9	0.741	0.197	1.1
Group 4	N	5	5	5	5	5	5	5	5	5	5	5	5
	tCtrl	0.93	1.00	0.92	0.98	0.97	0.97	0.76	0.94	0.94	1.18	1.04	1.00

 

Sex: Female		Reporting Biochemistry
		K (mmol/L) [G]	CL (mmol/L) [G]	CA (mmol/L) [G]	PHOS (mmol/L) [G1]
0	Mean	4.54	105.8	2.442	1.270
mg/kg/day	SD	0.19	1.3	0.054	0.491
Group 1	N	5	5	5	5
50	Mean	4.91	106.0	2.450	1.080
mg/kg/day	SD	0.51	2.1	0.060	0.305
Group 2	N	5	5	5	5
	tCtrl	1.08	1.00	1.00	0.85
150	Mean	4.85	106.4	2.456	1.534
mg/kg/day	SD	0.31	1.5	0.076	0.309
Group 3	N	5	5	5	5
	tCtrl	1.07	1.01	1.01	1.21
650	Mean	4.72	105.8	2.504	1.496
mg/kg/day	SD	0.54	0.4	0.053	0.138
Group 4	N	5	5	5	5
	tCtrl	1.04	1.00	1.03	1.18

[G] - Anova & Dunnett: * = p ≤ 0.05

[G1] - Kruskal-Wallis & Dunn

 

Table 17: Functional Observations & Motor Activity Summary

FUNCTIONAL OBSERVATIONS SUMMARY MALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
END OF TREATMENT HEARING	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
PUPIL L	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
PUPIL R	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
STATIC R	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
GRIP FORE	MEAN	1249	1149	1201	1112
GRAM	ST.DEV	287	258	115	91
	N	5	5	5	5
GRIP HIND	MEAN	560	534	537	492
GRAM	ST.DEV	108	64	68	89
	N	5	5	5	5
FUNCTIONAL OBSERVATIONS SUMMARY FEMALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
END OF TREATMENT HEARING	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
PUPIL L	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
PUPIL R	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
STATIC R	MEDIAN	0	0	0	0
SCORE 0/1	N	5	5	5	5
GRIP FORE	MEAN	959	787	889	895
GRAM	ST.DEV	181	93	219	171
	N	5	5	5	5
GRIP HIND	MEAN	330	312	317	341
GRAM	ST.DEV	49	61	54	57
	N	5	5	5	5

 

MOTOR ACTIVITY SUMMARY MALES
Total Movements	GROUP 1 CONTROL	50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
MEAN	3185	3370	2753	3155
N	5	5	5	5
STDEV	850	594	492	1153
* indicates a p-value <0.05, ** indicates a p-value <0.01 MEAN and STDEV values are calculated per group, from each animal's total Total Movements over all intervals
MOTOR ACTIVITY SUMMARY MALES
Ambulations	GROUP 1 CONTROL	50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4650MG/KG/DAY
MEAN	570	617	469	731
N	5	5	5	5
STDEV	158	158	141	450
* indicates a p-value <0.05, ** indicates a p-value <0.01 MEAN and STDEV values are calculated per group, from each animal's total Ambulations over all intervals
MOTOR ACTIVITY SUMMARY FEMALES
Total Movements	GROUP 1 CONTROL	50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
MEAN	5712	4124	4755	3559
N	5	5	5	5
STDEV	1708	979	1492	1435
* indicates a p-value <0.05, ** indicates a p-value <0.01 MEAN and STDEV values are calculated per group, from each animal's total Total Movements over all intervals
MOTOR ACTIVITY SUMMARY FEMALES
Ambulations	GROUP 1 CONTROL	50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4650MG/KG/DAY
MEAN	1459	969	1307	817
N	5	5	5	5
STDEV	408	302	618	330
* indicates a p-value <0.05, ** indicates a p-value <0.01 MEAN and STDEV values are calculated per group, from each animal's total Ambulations over all intervals

 

 

Table 18: Absolute Organ Weights (gram) Summary

ORGAN WEIGHTS (GRAM) SUMMARY MALES
		GROUP 1 CONTROL		GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
END OF TREATMENT BODY W.	MEAN	356		359		357		330 **
(GRAM)	ST.DEV	13		14		26		17
	N	10		10		10		10
BRAIN	MEAN	2.07		2.06		2.07		2.11
(GRAM)	ST.DEV	0.07		0.04		0.09		0.09
	N	5		5		5		5
HEART	MEAN	0.976		0.962		0.922		0.926
(GRAM)	ST.DEV	0.033		0.066		0.083		0.026
	N	5		5		5		5
LIVER	MEAN	8.38		8.37		8.41		9.46 *
(GRAM)	ST.DEV	0.36		0.84		0.56		0.47
	N	5		5		5		5
THYROIDS	MEAN	0.0171		0.0165		0.0175		0.0164
(GRAM)	ST.DEV	0.0021		0.0030		0.0041		0.0038
	N	10		10		10		10
THYMUS	MEAN	0.315		0.334		0.339		0.275
(GRAM)	ST.DEV	0.095		0.044		0.068		0.061
	N	5		5		5		5
KIDNEYS	MEAN	2.52		2.53		2.42		2.84
(GRAM)	ST.DEV	0.07		0.15		0.14		0.39
	N	5		5		5		5
ADRENALS	MEAN	0.055		0.059		0.059		0.063
(GRAM)	ST.DEV	0.012		0.007		0.005		0.007
	N	5		5		5		5
SPLEEN	MEAN	0.558		0.554		0.600		0.650 *
(GRAM)	ST.DEV	0.055		0.073		0.036		0.024
	N	5		5		5		5
TESTES	MEAN	3.47		3.54		3.60		3.40
(GRAM)	ST.DEV	0.21		0.44		0.32		0.20
	N	10		10		10		10
PROSTATE GLAND	MEAN	0.847		0.955		0.885		0.826
(GRAM)	ST.DEV	0.129		0.176		0.104		0.062
	N	10		10		10		10
EPIDIDYMIDES	MEAN	1.066		1.101		1.117		1.045
(GRAM)	ST.DEV	0.072		0.111		0.114		0.074
	N	10		10		10		10
SEMINAL VESICLES	MEAN	1.339		1.426		1.320		1.366
(GRAM)	ST.DEV	0.273		0.273		0.149		0.130
	N	10		10		10		10
ORGAN WEIGHTS (GRAM) SUMMARY FEMALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
END OF TREATMENT BODY W.	MEAN	294	286		293		320
(GRAM)	ST.DEV	23	24		17		107
	N	10	10		10		10
BRAIN	MEAN	1.92	1.92		1.96		1.92
(GRAM)	ST.DEV	0.07	0.05		0.07		0.02
	N	5	5		5		5
HEART	MEAN	0.868	0.839		0.825		0.822
(GRAM)	ST.DEV	0.040	0.113		0.043		0.065
	N	5	5		5		5
LIVER	MEAN	12.81	11.33		11.91		12.74
(GRAM)	ST.DEV	0.75	1.61		1.04		1.18
	N	5	5		5		5
THYROIDS	MEAN	0.0161	0.0162		0.0159		0.0156
(GRAM)	ST.DEV	0.0021	0.0031		0.0028		0.0026
	N	10	10		10		10
THYMUS	MEAN	0.210	0.198		0.214		0.218
(GRAM)	ST.DEV	0.037	0.021		0.057		0.042
	N	5	5		5		5
KIDNEYS	MEAN	2.12	1.94		2.01		2.13
(GRAM)	ST.DEV	0.09	0.16		0.14		0.18
	N	5	5		5		5
ADRENALS	MEAN	0.071	0.067		0.082		0.080
(GRAM)	ST.DEV	0.014	0.013		0.002		0.010
	N	5	5		5		5
SPLEEN	MEAN	0.523	0.455		0.502		0.529
(GRAM)	ST.DEV	0.021	0.072		0.066		0.072
	N	5	5		5		5
OVARIES	MEAN	0.118	0.105		0.119		0.104
(GRAM)	ST.DEV	0.015	0.012		0.022		0.011
	N	5	5		5		5
UTERUS	MEAN	0.368	0.333		0.395		0.443
(GRAM)	ST.DEV	0.045	0.024		0.079		0.218
	N	5	5		5		5

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

 

Table 19: Relative Organ Weights (%) Summary

ORGAN/BODY WEIGHT RATIOS (%) SUMMARY MALES
		GROUP 1 CONTROL		GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
END OF TREATMENT BODY W.	MEAN	356		359		357		330 **
(GRAM)	ST.DEV	13		14		26		17
	N	10		10		10		10
BRAIN	MEAN	0.57		0.58		0.60		0.62 **
(%)	ST.DEV	0.02		0.01		0.01		0.03
	N	5		5		5		5
HEART	MEAN	0.271		0.270		0.267		0.273
(%)	ST.DEV	0.011		0.011		0.023		0.018
	N	5		5		5		5
LIVER	MEAN	2.32		2.35		2.43		2.79 **
(%)	ST.DEV	0.10		0.17		0.06		0.08
	N	5		5		5		5
THYROIDS	MEAN	0.0048		0.0046		0.0049		0.0050
(%)	ST.DEV	0.0005		0.0008		0.0008		0.0012
	N	10		10		10		10
THYMUS	MEAN	0.087		0.094		0.098		0.081
(%)	ST.DEV	0.025		0.011		0.016		0.016
	N	5		5		5		5
KIDNEYS	MEAN	0.70		0.71		0.70		0.84 *
(%)	ST.DEV	0.03		0.04		0.03		0.15
	N	5		5		5		5
ADRENALS	MEAN	0.015		0.016		0.017		0.019
(%)	ST.DEV	0.003		0.002		0.001		0.003
	N	5		5		5		5
SPLEEN	MEAN	0.155		0.156		0.174		0.192 **
(%)	ST.DEV	0.014		0.019		0.018		0.010
	N	5		5		5		5
TESTES	MEAN	0.98		0.99		1.01		1.03
(%)	ST.DEV	0.08		0.13		0.05		0.07
	N	10		10		10		10
PROSTATE GLAND	MEAN	0.238		0.267		0.250		0.250
(%)	ST.DEV	0.037		0.055		0.039		0.016
	N	10		10		10		10
EPIDIDYMIDES	MEAN	0.300		0.307		0.313		0.317
(%)	ST.DEV	0.020		0.034		0.020		0.025
	N	10		10		10		10
SEMINAL VESICLES	MEAN	0.376		0.398		0.371		0.416
(%)	ST.DEV	0.074		0.078		0.049		0.055
	N	10		10		10		10
ORGAN/BODY WEIGHT RATIOS (%)SUMMARY FEMALES
		GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY		GROUP 3 150 MG/KG/DAY		GROUP 4 650 MG/KG/DAY
END OF TREATMENT BODY W.	MEAN	294	286		293		320
(GRAM)	ST.DEV	23	24		17		107
	N	10	10		10		10
BRAIN	MEAN	0.64	0.71		0.68		0.66
(%)	ST.DEV	0.03	0.06		0.03		0.04
	N	5	5		5		5
HEART	MEAN	0.292	0.306		0.285		0.284
(%)	ST.DEV	0.012	0.029		0.015		0.020
	N	5	5		5		5
LIVER	MEAN	4.31	4.13		4.11		4.39
(%)	ST.DEV	0.24	0.36		0.18		0.30
	N	5	5		5		5
THYROIDS	MEAN	0.0055	0.0057		0.0054		0.0052
(%)	ST.DEV	0.0010	0.0010		0.0011		0.0015
	N	10	10		10		10
THYMUS	MEAN	0.071	0.073		0.074		0.076
(%)	ST.DEV	0.014	0.010		0.019		0.017
	N	5	5		5		5
KIDNEYS	MEAN	0.71	0.71		0.69		0.73
(%)	ST.DEV	0.03	0.05		0.05		0.04
	N	5	5		5		5
ADRENALS	MEAN	0.024	0.025		0.028		0.027
(%)	ST.DEV	0.005	0.003		0.002		0.003
	N	5	5		5		5
SPLEEN	MEAN	0.176	0.166		0.174		0.182
(%)	ST.DEV	0.006	0.018		0.021		0.020
	N	5	5		5		5
OVARIES	MEAN	0.040	0.038		0.041		0.036
(%)	ST.DEV	0.005	0.006		0.006		0.003
	N	5	5		5		5
UTERUS	MEAN	0.124	0.122		0.137		0.154
(%)	ST.DEV	0.017	0.009		0.030		0.076
	N	5	5		5		5

*/** Dunnett-test based on pooled variance significant at 5% (*) or 1% (**) level

 

 

Table 20: Coagulation Values (F0 generation) Summary

MALES: day 30 relative to start

Sex: Male		Reporting Coagulation
		PT   (sec)   [G]	APTT   (sec)   [G]
0 mg/kg/dayGroup 1	Mean SD N	16.63 0.55 3	20.08 3.02 4
50	Mean	15.42 *	16.56
mg/kg/day	SD	0.39	1.97
Group 2	N	5	5
	tCtrl	0.93	0.82
150	Mean	15.44 *	16.06 *
mg/kg/day	SD	0.47	1.60
Group 3	N	5	5
	tCtrl	0.93	0.80
650	Mean	15.74	15.60 *
mg/kg/day	SD	0.72	1.63
Group 4	N	5	5
	tCtrl	0.95	0.78

[G] - Anova & Dunnett: * = p ≤ 0.05

 

FEMALES: Day 51 relative to start date

Sex: Female		Reporting Coagulation
		PT   (sec)   [G]	APTT   (sec)   [G]
0 mg/kg/dayGroup 1	Mean SD N	15.52 0.70 5	15.64 0.97 5
50	Mean	16.28	15.34
mg/kg/day	SD	0.40	0.74
Group 2	N	5	5
	tCtrl	1.05	0.98
150	Mean	15.94	14.82
mg/kg/day	SD	0.62	1.89
Group 3	N	5	5
	tCtrl	1.03	0.95
650	Mean	16.15	15.28
mg/kg/day	SD	1.10	2.96
Group 4	N	4	4
	tCtrl	1.04	0.98

[G] - Anova & Dunnett: * = p ≤ 0.05

 

Table 21: Gross Pathology Summary

MACROSCOPIC FINDINGS SUMMARY MALES
	GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
END OF TREATMENT Animals examined	10	10	10	10
Animals without findings	8	9	9	0
Animals affected	2	1	1	10
Stomach Several crateriform retractions	0	0	0	9
Focus/foci	0	0	0	5
Thickened	0	0	0	10
Irregular surface	0	0	0	1
Liver
Right medial lobe constricted.	1	0	0	0
Accessory liver	0	0	1	0
Grown together with:	0	0	0	1
Kidneys
Pelvic dilation	1	0	0	0
Testes
Reduced in size	0	1	0	0
Epididymides
Reduced in size	0	1	0	0
Skin
Scab formation	0	0	0	3
MACROSCOPIC FINDINGS SUMMARY FEMALES
	GROUP 1 CONTROL	GROUP 2 50 MG/KG/DAY	GROUP 3 150 MG/KG/DAY	GROUP 4 650 MG/KG/DAY
END OF TREATMENT Animals examined	10	10	10	10
Animals without findings	8	8	9	3
Animals affected	2	2	1	7
Stomach Several crateriform retractions	0	0	0	2
Crateriform retraction	0	0	0	2
Thickened	0	0	0	4
Liver
Reduced in size	1	0	0	0
Grown together with:	0	0	0	1
Discolouration	1	0	0	0
Uterus
Nodule(s)	1	0	0	0
Clitoral glands Focus/foci	0	1	0	0
Thyroid gland Discolouration	0	0	1	0
Mandibular lymph n
Discolouration	0	0	0	1
Skin
Alopecia	0	0	0	1
Scab formation	1	1	0	0

# / ## Fisher's Exact test significant at 5% (#) or 1% (##) level

 

Table 22: Summary Test Item-Related Microscopic Stomach and Spleen Findings – Scheduled Euthanasia Animals

	Males				Females
Dose level (mg/kg/day / ppm):	0	50	150	650	0	50	150	650
STOMACH a	5	5	5	10	5	5	5	7
Ulcerative inflammation, forestomach
Moderate	-	-	-	1	-	-	-	-
Marked	-	-	-	3	-	-	-	-
Massive	-	-	-	4	-	-	-	4
Necrosis, transmural, forestomach
Slight	-	-	-	1	-	-	-	-
Marked	-	-	-	7	-	-	-	4
Ulcer/Erosion, glandular stomach
Slight	-	-	-	2	-	-	-	1
Inflammation, glandular stomach
Minimal	-	2	-	3	-	-	-	-
Slight	-	-	-	2	-	-	-	1
Hemorrhage, glandular stomach
Minimal	-	1	-	2	-	-	-	-
Slight	-	-	-	1	-	-	-	-
SPLEEN a	5	5	5	5	5	5	5	5
Extramedullary hematopoiesis
Minimal	1	3	2	1	3	2	2	2
Slight	-	1	2	4	2	-	1	-
Moderate	-	-	-	-	-	-	-	1
Pigmentation
Minimal	4	3	4	2	4	4	2	-
Slight	-	-	-	3	1	1	3	5

 

Table 23: Summary Test Item-Related Microscopic Findings – Scheduled Euthanasia Animals (Males)

	Males
Dose level (mg/kg/day / ppm):	0	50	150	650
LIVER a	5	5	5	5
Hepatocellular hypertrophy
Minimal	-	-	2	4
KIDNEYS a	5	5	5	5
Basophilia, tubular
Minimal	1	4	4	-
Slight	-	-	1	2
Moderate	-	-	-	1
Marked	-	-	-	2
Cast, granular
Minimal	-	-	-	2
Slight	-	-	-	1
Degeneration, tubular
Minimal	-	-	1	-
Slight	-	-	-	2
Moderate	-	-	-	1

^a  =  Number of tissues examined from each group.

 

Table 24: Correlations of Selected Observations

Necropsy	Organ Weight	Hematology	Histopathology
Forestomach: Crateriform retractions and Thickened limiting ridge	n.a.	WBC↑ Neutrophils↑ Lymphocytes↑	Ulcerative inflammation and Transmural necrosis
Glandular stomach: Red foci	n.a.	-	Hemorrhages (males)
Liver: No macroscopic findings	↑ (males)	-	Hepatocellular hypertrophy (males)
Spleen: No macroscopic findings	↑ (males)	RBC↓, HGB↓, MCHC↓ (males) Reticulocytes↑ (males)	Increased extramedullary hematopoiesis
Kidney: No macroscopic findings	-	Urea ↑	Increased basophilia, granular casts and tubular degeneration

-  =  no findings / no correlate; n.a.= not applicable