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§799.3300 Unsubstituted phenylenediamines.
(a) Identification of test substance. (1) The unsubstituted
phenylenediamines (pda's), para-phenylenediamine (p-pda, CAS No.
106-50-3), or its sulfate salt (p-pda.H (2) p-Pda, m-pda, and o-pda of at least 98 percent
purity shall be used as the test substances. Either the hydrochloride or sulfate
salt of m-pda shall be used as the test substances. Either the
hydrochloride or sulfate salt of m-pda shall be used as a test substance
in the oncogenicity test in paragraph (c)(2) of this section if the free base
proves to be unstable under the conditions of this study. Either the
hydrochloride or sulfate salt of o-pda, p-pda, or m-pda
shall be used as a test substance in the 90-day subchronic neurotoxicity studies
in paragraph (c)(3)(B) of this section if the free base proves to be unstable
under the conditions of these studies. The salt(s) shall be of at least 98
percent purity.
(b) Persons required to submit study plans, conduct tests, and submit
data. (1) All persons who manufacture (including import or by-product
manufacture) or process m-pda or m-pda.H (2) All persons who manufacture (including import or by-product manufacture)
or process p-pda, or p-pda.H (3) All persons who manufacture (including import or by-product manufacture)
or process o-pda, or intend to manufacture or process o-pda after
the effective date of this rule to the end of the reimbursement period shall
submit letters of intent to test, submit study plans, conduct tests, and submit
data, or submit exemption applications as specified in paragraphs (c)(3), (d),
and (e) of this section, subpart A of this part, and parts 790 and 792 of this
chapter for single-phase rulemaking.
(c) Health effects testing -- (1) Mutagenicity testing -- (i)
Required testing. (A) The sex-linked recessive lethal (SLRL) assay shall
be conducted, by injection, in Drosophila melanogaster with m-pda
in accordance with § 798.5275 of this chapter.
(B) If the SLRL assay conducted pursuant to paragraph (c)(1)(i)(A) of this
section is positive, either the mouse visible specific locus test (MVSL) or the
mouse biochemical specific locus test (MBSL) shall be conducted for m-pda
by gavage in accordance with §§798.5200 or 798.5195 of this chapter, if after
public program review, EPA issues a FEDERAL REGISTER notice or sends a certified
letter to the test sponsor(s) specifying that testing shall be initiated. The
test sponsor shall notify EPA of its choice in writing in its first interim
report.
(C) The mouse bone marrow cytogenetics: micronucleus (MBMC) assay shall be
conducted on m-pda in accordance with § 798.5395
of this chapter.
(D) If the MBMC assay conducted pursuant to paragraph (c)(1)(i)(C) of this
section is positive, the dominant lethal assay (DL) in mice shall be conducted
on m-pda pursuant to § 798.5450 of this chapter.
(E) If the DL conducted pursuant to paragraph (c)(1)(i)(D) of this section is
positive, heritable translocation (HT) testing in the mouse on m-pda
shall be conducted pursuant to § 798.5460 of this
chapter, if after a public program review, EPA issues a FEDERAL REGISTER notice
or sends a certified letter to the test sponsor(s) specifying that testing shall
be initiated.
(ii) Reporting requirements. (A) The tests shall be completed and the
final reports for the MBMC assay shall be submitted to the EPA no later than
January 16, 1991. The final report for the SLRL in Drosophila
melanogaster shall be submitted no later than April 15, 1991.
(B) If required, the DL test shall be completed and the final report shall be
received by EPA no later than 24 months after the effective date of this final
rule.
(C) If required, the MVSL or the MBSL shall be completed and the final report
shall be received by EPA no later than 51 months after EPA issues a FEDERAL
REGISTER Notice or sends a certified letter to the test sponsor(s) identified
under paragraph (c)(1)(i)(B) of this section specifying that testing shall be
initiated.
(D) If required, the HT test shall be completed and the final report shall be
submitted to EPA not later than 36 months after the date on which EPA notifies
the test sponsor under paragraph (c)(1)(i)(E) of this section to begin testing.
(E) Interim reports for the SLRL assay and MBMC are required at 6-month
intervals beginning 6 months after the effective date of this section. If the DL
is triggered, interim reports are required at 6 month intervals beginning with
the date of initiation of the study.
(F) Interim reports for the HT and either the MBSL or MVSL are required at
6-month intervals beginning 6 months after the date of notification by EPA that
testing shall be initiated, and ending when the final report is submitted.
(2) Oncogenicity -- (i) Required testing. A 2-year dermal
oncogenicity bioassay shall be conducted with m-pda if, after public
program review, EPA issues a FEDERAL REGISTER notice specifying that the testing
shall be initiated.
(ii) [Reserved]
(iii) Reporting requirements. (A) The final results and final report
for the oncogenicity bioassay shall be submitted to EPA no later than 53 months
after EPA issues a FEDERAL REGISTER notice or sends a certified letter to the
test sponsor under paragraph (c)(2)(i) of this section specifying that the
testing shall be initiated.
(B) Interim reports for the oncogenicity study are required at 6-month
intervals beginning 6 months after the date of notification by EPA that testing
shall be initiated and ending when the final report is submitted.
(3) Neurotoxicity -- (i) Required testing. (A) Acute
neurotoxicity testing in the neurotoxicity functional observational battery
(FOB) in accordance with § 798.6050 of this chapter, and
the motor activity test (MAT) in accordance with
§ 798.6200 of this chapter, shall be conducted for
o-, m-, and p-pda. The test chemicals shall be administered
in a single oral dose. Clinical observations shall be made at a minimum of 1, 4,
24, and 48 hours and at 7 days after dosing.
(B) If neurotoxic effects are observed at 24 hours, or longer, during the
testing conducted pursuant to paragraph (c)(3)(i)(A) of this section, then
90-day subchronic neurotoxic FOB and MAT tests shall be conducted in accordance
with §§ 798.6050 and 798.6200 of this chapter,
respectively, for each isomer showing such effects. At the end of these tests,
the animals shall be sacrificed and the nervous tissue preserved and examined as
described in the neuropathology test standard, § 798.6400
of this chapter.
(ii) Reporting requirements. (A) The acute neurotoxicity tests shall
be completed and the final report submitted to EPA no later than September 15,
1990. If triggered, the final report of the subchronic neurotoxicity testing and
the neuropathological examination shall be submitted to EPA on the following
schedules. If one isomer is triggered, the reporting deadline is July 15, 1990.
If two isomers are triggered, the reporting deadline is January 15, 1992. If
three isomers are triggered, the reporting deadline is July 15, 1992.
(B) [Reserved]
(d) Chemical fate testing -- (1) Indirect photolysis testing --
(i) Required testing. Indirect photolysis studies shall be conducted with
p-, m-, and o-pda to determine the half-life in water of
each of the three unsubstituted pda's in accordance with
§ 795.70 of this chapter.
(ii) Reporting requirements. (A) The final report shall be submitted
to EPA no later than 8 months after the effective date of the final rule.
(B) The final report shall include a calculation of the predicted
environmental concentration (PEC), 100×PEC, and 1,000×PEC for each isomer. PEC
shall be calculated by using results from the indirect photolysis studies and
solving the following equations for the appropriate isomer: o-pda: PECo =
0.3629 + 1.0468 log t 1/2; m-pda: PECm = 0.6830 + 1.9702 log t 1/2;
p-pda: PECp = 0.0085 + 0.0024 log t 1/2, where PEC is the predicted
concentration in ppb and t 1/2 is the half-life for oxidation (i.e., indirect
photolysis) expressed in minutes. PEC, 100×PEC, and 1,000×PEC shall be used in
the decision logic described in paragraph (e) of this section.
(2) [Reserved]
(e) Environmental effects testing -- (1) Acute toxicity testing
-- (i) Required testing. (A) Flow-through fish acute toxicity tests in
the rainbow trout (Salmo gairdneri) shall be conducted with o-,
m-, and p-pda in accordance with § 797.1400
of this chapter.
(B) Acute flow-through studies on the freshwater invertebrate Gammarus
shall be conducted with o-, m-, and p-pda in accordance
with § 795.120 of this chapter.
(C) If the concentration affecting 50 percent of the population (LC (ii) Reporting requirements. The final reports for acute toxicity
testing shall be submitted as follows:
(A) Testing on the rainbow trout shall be completed and submitted to EPA 9
months after the effective date of the final rule for o-pda and
p-pda. Testing for m-pda shall be completed and submitted by
January 15, 1991.
(B) The acute toxicity testing in freshwater Gammarus shall be
completed and submitted no later than January 15, 1991.
(2) Chronic toxicity testing -- (i) Required testing. (A) A
fish partial life-cycle flow-through test shall be conducted in the more
sensitive fish species, either Pimephales promelas or Salmo
gairdneri, with each isomer, o-, m-, and p-pda,
demonstrating an LC (B) An invertebrate life-cycle flow-through toxicity test shall be conducted
in Daphnia magna for o- and p-pda in accordance with
§ 797.1330 of this chapter.
(ii) Reporting requirements. (A) The fish partial life-cycle
flow-through test shall be completed and final results shall be submitted to EPA
no later than December 1, 1992.
(B) The invertebrate life-cycle flow-through toxicity test shall be completed
and the final report submitted to EPA no later than January 15, 1993.
(C) Progress reports shall be submitted at 6 month intervals after the
effective date of the final rule.
(f) Effective dates. (1) The effective date of this final rule is
January 16, 1990, except for paragraphs (c)(1)(i)(B), (c)(1)(ii)(A),
(c)(1)(ii)(C), (c)(1)(ii)(F), (c)(3)(ii)(A), (e)(1)(ii), (e)(2)(ii)(A), and
(e)(2)(ii)(B) of this section. The effective date for paragraphs (c)(1)(i)(B),
(c)(1)(ii)(C), and (c)(1)(ii)(F) of this section is May 21, 1990. The effective
date for paragraphs (c)(1)(ii)(A), (c)(3)(ii)(A), and (e)(1)(ii), of this
section is May 21, 1991. The effective date for paragraph (e)(2)(ii)(A) is June
12, 1992. The effective date for paragraph (e)(2)(ii)(B) is May 28, 1993.
(2) The guidelines and other test methods cited in this rule are referenced
as they exist on the effective date of the final rule.
[54 FR 49294, Nov. 30, 1989, as amended at 55 FR 12644, Apr. 5, 1990;
56 FR 23231, May 21, 1991; 57 FR 24961, June 12, 1992; 58 FR 30992, May 28,
1993; 58 FR 34205, June 23, 1993]
