No studies were done on the
lethality of humans in relation to HCCPD. It was however tested on animals and is postulated to have effects on brain and
adrenal glands. In the brain, HCCPD or a metabolite thereof can react with
lipids. In order to see degenerative brain effects in for example rats, the animals are exposed to a high dose of HCCPD concentration by inhalation. When dealing with low exposure levels, HCCPD reactivity makes the chance of reactive species in the blood at high concentrations very low. However, at higher doses the probability of transporting reactive material across the
blood-brain barrier is higher. Short-term inhalation of HCCPD is
lethal to mice, rats, rabbits and guinea pigs. The
lethality of the animals can be affected by the concentration and duration of HCCPD exposure. From all the animals tested, guinea pigs showed to be the most resistant to the compound toxicity. Almost all biological systems are shown to be vulnerable to the toxicity of HCCPD, except the
hematological and
musculoskeletal systems.
Oral effects Single doses of HCCPD were found to be moderately toxic to animals if ingested orally. However, as the compound was not entirely pure (93.3%) while performing studies, some of the toxic effects could be attributed to the impurities, especially at high doses. Data of oral effects on other species that mice and rats are limited. Single high doses of HCCPD resulted in increased effort to breathe in rats and rabbits alike. The lung tissues of these animals were
hyperemic and
edematous after a given dose. Extensive lung
hemorrhage appeared after a single non lethal dose after 21 days. Lower doses in rats caused no observable tissue changes in the lungs. High doses created degenerative changes to the heart as well. Again, low doses resulted in no observable change in heart tissue. Also, these rats and rabbits experienced
diarrhea after single oral dosages of HCCPD, and showed acute necrotic
lesions in the
forestomach. In repeated exposure experiments on rats and mice
inflammation and
epithelial hyperplasia of the
forestomach were observed. The dose had a direct relationship to the severity of these effects. This and the location suggests that these effects result from direct contact of the tissue with HCCPD. Body weight was heavily affected after oral ingestion of HCCPD by rats, more severely for males than females.
Dermal effects Increasing dermal doses showed a shorter survival time for the animals. Lung effects of rabbits were examined in dermal animal studies, showing
congested blood and fluid by exposure of HCCPD (93,3% pure, so again a possibility of contaminant interference). Other effects regarding organs with dermal dose were degenerative changes in the heart,
necrosis of the liver and
kidney tubules and degenerative changes of the adrenal glands. The form in which HCCPD appears in the environment, so in its pure form or in solution, showed a striking effect on the
epidermis of rabbits, guinea pigs and monkeys. Damage to the skin could be seen, namely discolored and inflamed skin. When the animals did not die by these lesions, they healed over time by itself.
Inhalation effects HCCPD is highly toxic to animals when inhaling its vapours. No human studies regarding lethality were done, but there has been an incident involving a waste water treatment centre where humans were exposed, from which most relevant human information is taken.
Human inhalation effects There is data for human exposure to HCCPD for numerous organ systems. Waste water treatment plant and water cleanup crew workers were exposed after industrial release of the compound into the environment. The initial concentration of the compound in air was unknown but was later determined to be ranging between 0.27 and 0.97
ppm. Workers noticed a strange odor on the plant and even a blue haze after a heavy rain. When some of them sought medical attention, it was determined the plant was contaminated with HCCPD, and numerous tests were performed to document these circumstances. Approximately one fifth of waste water treatment workers reported having nausea and abdominal cramps after exposure for a period between 3 and 15 days. They also reported respiratory complaints like sore throats, coughing and breathing difficulty. However, tests on lung function and chest
X-rays did not show any abnormalities. Workers exposed to HCCPD for a longer time reported respiratory irritation,
nasal irritation and
sinus congestion, most likely because of direct contact of these tissues with HCCPD from the air, and not as a
systemic effect through the lungs. In addition, elevated levels of
lactic dehydrogenase was found in 11 out of 41 workers from the wastewater treatment. These levels was not nearly as high for workers from the water cleanup crew, but the
aspartate aminotransferase levels were elevated for 12 out of 97 of these workers. These
enzymes might indicate damage to heart, as well as to the liver. No evidence of heart function impairment was found in both worker groups though. The elevated levels in patients diminished after a period of 3 weeks.
Animal inhalation effects For prolonged exposure, significant differences occur between lab animal species. Where all mice died in the first week in a 13-week study, being exposed to 2 ppm HCCPD for 5 days a week, 6 hours a day, rats however survived until the third week. For a very low exposure of 0.04 ppm, 3 out of 20 mice died and none of the rats died. Chronic exposure of HCCPD at very low concentrations produced a yellow-brown pigment in the lung, tracheal and nasal epithelium in rats and mice. The pigmentation did not disappear after the exposure stopped. For acute high exposures (1 hour, 42 ppm) all animals died, after showing difficulty breathing and gasping for air. Their lung tissues showed hemorrhagic
lesions,
inflammation,
edema and
necrosis in the
bronchi. However recovery of the animals that survived was apparent 2 weeks after the treatment.
Cardiac and
gastrointestinal function seemed not be impaired after exposure of HCCPD in rats, mice and monkeys. Moderate
hepatic tissue degeneration was observed for acute inhalation. The same tissue degeneration was observed for longer experiments with lower concentrations. == History ==