User Manual
Conditions to avoid
freezing
Incompatible materials
no d
ata available
Hazardous decomposition
produ
cts
No decomposition products expected under normal conditions of use.
SECTION 11: TOXICOLOGICAL INFORMATION
E
xposure routes
Ingestion, Inhalation, Eye contact, Skin contact
Immediate Effects
Eye
Moderate eye irritation.
Skin
H
armful if absorbed through skin.
Ingestion
H
armful if swallowed.
Inhalation
H
armful if inhaled.
Information on toxicological effects
Acute oral toxicity
LD50
(male/female combined rat) > 2,000 mg/kg
Acute inhalation toxicity
LC50
(male/female combined rat) > 1.2 mg/l
Exposure time: 4 h
Determined in the form of liquid aerosol.
Highest attainable concentration.
(actual)
LC50
(male/female combined rat) > 4.8 mg/l
Exposure time: 1 h
Determined in the form of liquid aerosol.
Extrapolated from the 4 hr LC50.
(actual)
Acute dermal toxicity
LD50
(male/female combined rat) > 4,000 mg/kg
Skin irritation
N
o skin irritation (rabbit)
Eye irritation
N
o eye irritation (rabbit)
Sensitisation
N
on-sensitizing. (guinea pig)
Assessment repeated dose toxicity
The toxic effects of beta-Cyfluthrin are related to transient hyperactivity typical for pyrethroid
neur
otoxicity.
Imidacloprid did not cause specific target organ toxicity in experimental animal studies.
Assessment Mutagenicity
beta-Cyfluthrin was not mutagenic or genotoxic in a battery of in vitro and in vivo tests.
Imid
acloprid was not mutagenic or genotoxic based on the overall weight of evidence in a battery of in
vitro and in vivo tests.
Assessment Carcinogenicity
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Revision Date: 05/01/2017