Sulfuric acid, C16-C18 (even numbered) alkyl esters, sodium salts and C16-18 (even numbered) alcohols

Groups of 10M+10F Sprague-Dawley rats received daily doses of 0, 100, 500 and 1000 mg/kd Lanette 16 by gavage for 28 days. Full details of this study are reported in Chapter 7.5.1 Repeated dose toxicity: oral.

The testes and ovaries were weighed and these organs plus the prostate, uterus and vagina from all control and top dose animals were subject to histopathological examination.

There were no deaths among the test animals. Food intake, water consumption, body weight, organ weight, and haematological parameters were not affected.

The absolute and relative organ weights of the ovary and testes were determined and were comparable to controls.

Reproductive tissues from the control and top dose animals (1000 mg/kg/day) were examined histopathologically. In females examination of the ovaries, uterus and vagina and in males histopathological examination of the testes and prostate showed no difference between treated and control groups. The NOAEL for effects on the reproductive organs was considered to be 1000 mg/kg/day.

(Reference: Henkel KGaA. 1985a. Lanette 16: 28-Tage-Test mit wiederholter oraler Verabreichung an Ratten.November 1985.Report No. TBD 850499. With pathology report No. 840394)

In a 13 week dietary feeding study in rats 10 male and 10 female rats per dose group (20 M and 20 F as controls) were dosed with Alfol 16 at dose levels of 1.0, 2.5 and 5% in the diet. The 5% dose was increased to 7.5% in week 11 and 10% in weeks 12 and 13.

At termination, all animals were necropsied and tissues from 5 males and 5 females (including gonads) of the high dose group and a similar number of controls were examined histopathologically. Testes and ovary weights were recorded together with other organ weights.

None of the animals displayed overt signs of intoxication due to oral exposure to hexadecanol during the 13 weeks of the experiment. Food consumption and body weights differed significantly for both males and females at various times in the intermediate and high dose levels. The relative testes weights were increased over control levels in all treatment groups reaching signficance in the low and high group according to the study report. The organ weight data were reanalysed by the Weinberg Associates using a Tukey test when significance was attained only at the high dose level. There were no significant changes in ovary weight. Histopathological examination revealed no treatment related changes in the ovaries or testes. The NOAEL for effects on the male reproductive organs can be considered as a dietary concentration of 2.5% (ca 2000 mg/kg/day) the NOAEL for the female reproductive organs is the highest dose level (ca 4000 mg/kg/day). Actual dose levels achieved at respective NOAELs, males 1822 mg/kg/day and females 4567 mg/kg/day.

(Reference: Scientific Associates, Inc. 1966a. Exhibit II. Final report on thirteen-week subacute feeding of Alfol 6 and Alfol 16 to rats.)

1-Octadenol was administered to groups of 12 male and 12 female Wistar rats in the diet for 45 days (males) and ca. 54 days (females) according to the Draft OECD 422 combined repeated dose and reproductive/developmental toxicity screening test.

Mortality and clinical signs were observed daily; body weight was observed weekly; food consumption was observed weekly (except during mating). Haematology and clinical chemistry were examined at day 37 in males only. Full necropsy was performed on all animals. Histopathological examination was carried out on all control and top dose animals plus any obvious lesions observed at necrospy. Organs examined were liver, kidneys, adrenals, brain, heart, spleen, ovaries or testes and epididymes.

Organ weights were recorded for liver, kidneys, thymus (females) liver, kidney, thymus, testes, epididymes (males).

There were no mortalities and no clinical signs reported.

There were no significant changes in body weight or body weight gain in the 3 weeks prior to mating for both sexes or in males after mating.

Food consumption was significantly increased in top dose males (p<0.001) and in mid dose females (p<0.05) at week 3. There were no other differences in food consumption or food conversion efficiency.

There were significant (but non-dose related) differences in free cholesterol (increased) and triglycerides (decreased) at all dose levels. Total cholesterol levels were not significantly increased. Plasma glucose was elevated with statistical significance in the low and mid-dose groups; only males were examined.

There were no statistically significant differences in haematology between treated and control groups (males only examined).

Gross pathology and histopathology were unremarkable.

There was no statistically significant difference in pregnancy rates (confirmed using a Qui2-test) although they were reduced in treated groups (C: 92%, 100 & 500 mg/kg: 75%, 2000 mg/kg/day: 67%). These pregnancy rates were within the normal historical control range according to the authors (actual historical control data not presented).

There were no significant differences in the number of implantations or resorptions between treated and control groups.

There were no significant differences in the number of corpora lutea between treated and control groups.

There was no effect of treatment on litter size and litter weights.

Parental NOAEL for systemic toxicity was 2000 mg/kg/day based on changes in plasma free cholesterol, triglycerides and glucose. These changes were observed at all doses levels but were not dose related and may be due to differences in dietary composition.

There were no statistically significant adverse effects on reproductive parameters and the NOAEL for reproductive and developmental effects can be considered as 2000 mg/kg/day (highest dose level).

(Reference: Hansen, E. 1992b. Combined repeat dose and reproductive/developmental toxicity screening test on 1-octadecanol in rats. : of, National Food Agency, IT 911130.)

The IUCLID dataset of C12-Alkylsulfate (CAS 151-21-3) in the OECD SIDS Initial Assessment Profile on Sodium dodecyl sulfate (SDS) describes the following Klimisch 2 study. Sodium dodecyl sulphate was administered to 10 male Swiss mice per dose group. The male mice were fed diets containing 100 mg/kg bw/d for 6 weeks or 1000 mg/kg bw/d for 2 weeks.

At the highest dose level of 1000 mg/kg bw/d body weights were significantly decreased, while the treatment caused no adverse effects on fertility (i.e. impairment of epididymal spermatozoa). Keeping in mind that the LOAEL for repeated dose toxicity for rats lies between 300 and 600 mg kg/day, the observed reduction in body weight is probably caused by the systemic toxicity of the substance.

In UNEP OECD SIDSInitial Assessment Report: Sodium Dodecyl Sulfate(1997), a NOAEL of 1000 mg/kg and day was derived for this endpoint, using the following parameters: 25 g mice body weight and 2.5 g diet consumed per day.

Reference: Hemsworth BN (1981) Male mouse fertility after ingestion of spermicidal detergents. Soc Occup Med 9, 243 – 244.

UNEP (1997) OECD SIDS Initial Assessment Report: Sodium Dodecyl Sulfate, http://www.chem.unep.ch/irptc/sids/OECDSIDS/151213.htm.