United States           Office of Pesticides and Toxic Substances
                  Environmental Protection     Office of Pesticide Programs (TS-766C)
                  Agency              Washington, DC 20460
                                                           540/FS-89-021
&EPA     Pesticide
                 Fact Sheet
                 Name of Chemical:
                 Reason for Issuance:  Registration  Standard
                 Date Issued:        December 20,  1988
                 Fact Sheet Number:  189
  1.  DESCRIPTION OF CHEMICAL
                     2-chloro-4f6-bis(isopropylamino)-s-triazine
                     Propazine
                     Milogard,ョ  Gesamil,ョ Milo-Pro, Pramitol,  Prozinex
    Generic Name
    Common Name
    Trade Name
    OPP Chemical  Code:  080808
    Chemical Abstracts Service (CAS) Number:   139-40-2
    Year of Initial Registration:  1974
    Pesticide Type:  Herbicide
    Chemical Family:  S-Triazine
    U.S. and Foreign Producers:  Ciba-Geigy,  Drexel,  Makhteshim-Agan,
        Griffin Corp., l.pi.ci.

2.   USE PATTERNS  AND FORMULATIONS

    Application Sites:  Propazine is registered  for use on the
        terrestrial food crop sorghum and for noncrop areas.

    Percent of Pesticide Applied:  99+% of propazine  is used on
        sorghum.

    Types and Methods of Application:  Propazine is used as a
        selective preemergent herbicide to control broadleaf and
        grass weeds.  Propazine is applied as a  spray, at the
        time of planting, prior to planting or immediately follow-
        ing planting by ground or aerial equipment.

    Application Rates:  Propazine is applied  generally from 1 to
        2 pounds  active ingredient per acre;  however, as much as
        3.2 pounds active ingredient per acre may be  used on
        certain fine textured or highly organic  soils for sorghum
        and from  1.6 to 13.3 pounds per acre  for non-crop areas.

    Types of Formulations:  Wettable powders  (90 to 26.67% active
        ingredient); flowable concentrates (44.5 to 18.7% active
        ingredient); soluble concentrates (43% active ingredient)

    Usual Carrier:  Water.  Agitation in the  spray tank is necessary
        to keep the chemical in suspension.

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3.  SCIENCE FINDINGS

    Summary Science Statement:   Propazine has low acute oral
        toxicity and is classified in Toxicity Category III*.
        Propazine is not considered to be teratogenic in rats.
        Propazine did not induce tumors in mice but an increased
        incidence of mammary gland tumors was observed in female
        rats.   Based on the rat study, the Agency has classified
        propazine at a Group C  oncogen (potential human carcinogen)
        but has concluded that  quantitative risk assessment  is
        not warranted because tumors in the rat study occurred  in
        only one sex, were mostly benign and were significantly
        increased only at the highest dose tested.

        Propazine can be characterized as slightly toxic to  cold-
        water  fish and practically nontoxic to waterfowl.   It will
        not pose a hazard to endangered plant or wildlife species.
        Propazine does have the potential to contaminate groundwater

    Chemical Characteristics:

        Physical State:  Solid
        Color:   Colorless, white
        Odor:   Odorless
        Melting Point:  212-214 ーC
        Density:  1.16 +_ 0.002  g/cm3 at 20 ーC
        Solubility:   8.6 ppm; water 20-22 ーC
        Vapor  Pressure:  2.9 x  10~8 mmHg at 20 ーC
        Stability:  Minimum of  3 years at room temperature

    Toxicology  Characteristics:

        Acute  Toxicity:

            Acute Oral-由at: >  5 g/kg (Toxicity Category IV)

            Acute Dermal由abbit:  > 2 g/kg (Toxicity Category III)

            Acute Inhalation由at:  > 2.1 mg/L/4 hr  (Toxicity
                Category III)

            Primary Eye Irritation由abbit:  No corneal opacity  at
                24 hours (Toxicity Category III)

            Primary Skin Irritation由abbit:   Score of 3.9/8.0
                with erythema,  eschar, and edema with improvement
                within 72 hours (Toxicity Category III)

        Subchronic Toxicological Results:   No acceptable studies
            are available.   However, because an acceptable chronic
            rat study is available and a nonrodent  chronic study
            is  required, subchronic studies are not required.
      Refer  to  40  CFR  156.10  for  a  discussion
      of  the toxicity  categories.

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    Chronic Feeding Results:  In a chronic feeding study in
        rats, the NOEL was 100 ppm.  A chronic feeding study
        in nonrodents is required.

    Oncogenic Testing Results:  Propazine was not oncogenic in
        a mouse study.  In a rat study, however, it did produce
        an increased incidence of mammory gland tumors in female
        rats at the highest dosage level tested (1,000 ppm).

    Developmental and Reproductive Study Results:  Propazine did
        not induce terata in a rat developmental toxicity study.
        The reproductive NOEL was 100 ppm.  An additional
        developmental study in a second species is required.

    Major Route of Exposure:  Dermal (mixers, loaders and
        applicators)

Physiological Characteristics:

    Absorption Characteristics:  Propazine is absorbed through
        plant roots.

    Translocation:  Propazine is absorbed by plant roots and is
        translocated upwardly in the plant to the leaves.  It
       .accumulates in the growing parts and leaves of plants.

    Mechanism of Action: Inhibition of cell division and photo-
        synthesis

Environmental Characteristics:  Propazine is persistent,
    moderately mobile and stable to hydrolysis, photolysis and
    microbial degradation, demonstrating a potential to con-
    taminate groundwater.  It has been detected in groundwater
    samples in 8 states with maximum concentrations of 20 ppb
    in surface water and 300 ppb in groundwater.  Available
    data are insufficient to fully assess the environmental
    fate and transport of propazine.

Ecological Characteristics:  Propazine is slightly toxic to
    coldwater fish with a toxicity value (LC5Q) of 16.5 ppm
    for rainbow trout.  It is practically nontoxic to waterfowl
    with a toxicity value (LCsg) of 32000 ppm for Mallards.
    Based on use, estimated concentrations and the available
    toxicity data, there is no threat to endangered wildlife or
    plant species.

Tolerance Assessment: Tolerances are established for negli-
    gible residues of propazine in or on sweet sorghum, its
    grain, fodder and forage at 0.25 ppm (40 CFR 180.243).
    The provisional acceptable daily intake (PADI) for
    propazine is 0.02 mg/kg/day, based on a 2-year rat feed-
    ing study in which the systemic NOEL was set at 100 ppm

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        (5 mg/kg).  The safety factor used was 300 based on an
        uncertainty factor of 100 to account for inter- and intra-
        species differences with an additional factor of 3 to
        account for the incompleteness of the chronic data base.
        The theoretical maximum residue contribution (TMRC) for
        the U.S. population average is 0.0003 mg/kg/day, equivalent
        to 1.7 percent of the PADI.

4.  SUMMARY OF REGULATORY POSITION AND RATIONALE.  As the result
        of a Data Call-in Notice, issued in April 1988, for a
        groundwater monitoring study, all propazine registrations
        have been either cancelled or suspended.  Therefore, the
        Agency has determined, at this time, that it is not
        necessary to formulate specific regulatory positions
        regarding prdpazine.  If a registrant commits to generate
        the required data and complies with the requirements of
        FIFRA, the Agency will then address specific regulatory
        positions for this chemical.

5.  SUMMARY OF MAJOR DATA GAPS

        Product Chemistry
        Toxicology
            Dermal Sensitization
            21-Day Dermal
            Chronic Toxicity (Nonrodent)
            Teratogenicity (Rabbit)
            General Metabolism
        Residue Chemistry
        Environmental Fate
        Ecological Effects

6.  EPA CONTACT

        Robert J. Taylor, Product Manager (25)
        Office of Pesticide Programs
        Registration Division (TS-767C)
        Environmental Protection Agency
        401 M Street, SW.
        Washington, DC  20460
        Telephone:  (703) 557-1800
DISCLAIMER;  The information presented in this Pesticide Fact Sheet
is for informational purposes only and may not be used to fulfill
data requirements for pesticide registration and reregistration.

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