Section 1 - CHEMICAL PRODUCT AND COMPANY IDENTIFICATION

PRODUCT NAME

YTTRIUM(III) 2-ETHYLHEXANOATE

NFPA

PRODUCT USE

Reagent. Drier

SYNONYMS

C24-H48-O6.Y, (C8-H16-O2)3.Y, "yttrium iso-octanoate"

Section 2 - HAZARDS IDENTIFICATION

CANADIAN WHMIS SYMBOLS

EMERGENCY OVERVIEW

RISK

POTENTIAL HEALTH EFFECTS

ACUTE HEALTH EFFECTS

SWALLOWED

  The material has NOT been classified as "harmful by ingestion". This is because of the lack of corroborating animal or human evidence. The material may still be damaging to the health of the individual, following ingestion, especially where pre-existing organ (e.g. liver, kidney) damage is evident. Present definitions of harmful or toxic substances are generally based on doses producing mortality (death) rather than those producing morbidity (disease, ill-health). Gastrointestinal tract discomfort may produce nausea and vomiting. In an occupational setting however, unintentional ingestion is not thought to be cause for concern.  

EYE

  Although the material is not thought to be an irritant, direct contact with the eye may cause transient discomfort characterized by tearing or conjunctival redness (as with windburn). Slight abrasive damage may also result. The material may produce foreign body irritation in certain individuals.  

SKIN

  The material is not thought to produce adverse health effects or skin irritation following contact (as classified using animal models). Nevertheless, good hygiene practice requires that exposure be kept to a minimum and that suitable gloves be used in an occupational setting.  Entry into the blood-stream, through, for example, cuts, abrasions or lesions, may produce systemic injury with harmful effects. Examine the skin prior to the use of the material and ensure that any external damage is suitably protected.  

INHALED

  There is some evidence to suggest that the material can cause respiratory irritation in some persons. The body's response to such irritation can cause further lung damage.  Persons with impaired respiratory function, airway diseases and conditions such as emphysema or chronic bronchitis, may incur further disability if excessive concentrations of particulate are inhaled.  Exposure to vapors of some rare earth salts can cause sensitivity to heat, itching, and increased sensitivity of smell and taste. Other effects include inflamed airways and lung,  emphysema, regional narrowing of terminal airways and cell changes. Rarely, excess blood flow has occurred following a delay. Lung cancers can also occur.  

CHRONIC HEALTH EFFECTS

  Limited evidence suggests that repeated or long-term occupational exposure may produce cumulative health effects involving organs or biochemical systems.  Based on experience with animal studies, there is a possibility that exposure to the material may result in toxic effects to the development of the fetus, at levels which do not cause significant toxic effects to the mother.  Long term exposure to high dust concentrations may cause changes in lung function i.e. pneumoconiosis; caused by particles less than 0.5 micron penetrating and remaining in the lung. Prime symptom is breathlessness; lung shadows show on X-ray.  Yttrium is a rare earth metal - heavy type (yttrium family). There has been no reports of poisoning in workers, although the metal can cause chest X-ray abnormalities due to its high density. It can cause scarring of the lungs, anemia and changes in blood cell distribution, due to inhalation of their dusts.  2-Ethylhexanoic acid (2-EHA) its esters and its salts are of concern to human health because of their potential to induce carcinogenicity, liver toxicity and developmental/reproductive toxicity. 2-EHA is of low acute oral and dermal toxicity, is a mild skin irritant and a severe eye irritant. It is not mutagenic in Ames test, but is capable of inducing chromosome aberration and sister chromatid exchanges in vitro, liver toxicity and liver tumours after repeated dose treatment, In addition, 2-EHA acid has been associated with reproductive and developmental toxicity in experimental animals.  2-EHA is quickly resorbed orally, dermally and following inhalation and almost fully excreted mainly  in urine. As in the case of fatty acids, degradation mainly takes place by means of peroxisomal  beta-oxidation.  Various studies on reproduction toxicity have produced indications of an embryotoxic effect of 2-EHA. After oral administration, NOAEL values for maternal toxicity and foetotoxic effects of 2-EHA were determined in rabbits at 25 and >250 mg/kg body weight/day and in rats at 250 and 100 mg/kg body weight/day. The foetotoxic findings in rats were based on a reduced skeleton ossification at the next higher dose (250 mg/kg body weight/day). No teratogenic effects were observed in this study. In comparison with the structural isomer valproic acid, a known human teratogen, 2-EHA does have similar reprotoxic effects at maternal toxic doses in animal experiments but a far lower potency  Following sub-chronic oral administration of 2-EHA, critical effects like liver changes (higher relative liver weight, histological changes in hepatocytes) were observed in rats and mice and histological renal tubule results were observed in mice. Furthermore, statistically significant, higher cholesterol values were found in all treated male rats (61, 303 and 917 mg/kg body weight/day) and in male and female mice in the middle and high dose groups (885-3139 mg/kg body weight/day). In rats the maximum dose with no adverse effect (NOAEL) was 61 mg/kg body weight/day  In bacterial test systems, mutagenicity studies produced negative findings. In test systems  with mammalian cells, by contrast, the findings were weakly positive. Cytogenetic and SCE studies involving CHO cells were positive, one SCE test in human lymphocytes was questionably positive and one experiment concerning tritium-thymidine incorporation into the DNA of mouse lymphocytes was negative. Furthermore, An unpublished micronucleus study on the bone marrow of CD-1 mice was conducted in compliance with OECD Guideline 474. No significant increase in the micronuclei was observed at doses of 400, 800 or 1,600 mg/kg body weight (Inveresk Research International Ltd, 1994). Furthermore, in vitro and in vivo genotoxicity data (micronucleus test, dominant lethal test) are available for 2-  ethylhexanol which is rapidly and quantitatively converted into 2-EHA in metabolism studies. This data do not indicate any genotoxic potential which means that such an effect of 2-EHA is not likely either. As 2-EHA can induce both DNA synthesis and inhibition of intercellular communication in hepatic cells, a tumour-promoting potential in rodents, comparable to that of other peroxisome proliferators, cannot be ruled out. The carcinogenic effect of peroxisome proliferators in rodents (e.g. of di(2-  ethylhexyl)phthalate, DEHP) is not deemed to be relevant for humans.  Calcium/zinc and barium/zinc salts of 2-EHA are used as thermo-stabilisers for PVC, together with co-stabilisers like polyols or epoxy compounds, in order to capture the hydrochloride cleaved during the thermal loading of PVC; in addition various salts are used in other food and beverage containers as plasticisers. The migration of 2-EHA from the sealing compounds in the metal lids. has been demonstrated in food contamination. The potential for human exposure to 2-EHA therefore is significant.