[Federal Register: April 8, 2005 (Volume 70, Number 67)]
[Notices]
[Page 17997-18001]
From the Federal Register Online via GPO Access [wais.access.gpo.gov]
[DOCID:fr08ap05-55]
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ENVIRONMENTAL PROTECTION AGENCY
[OPP-2005-0017; FRL-7704-2]
Kasugamycin; Notice of Filing a Pesticide Petition to Establish a
Tolerance for a Certain Pesticide Chemical in or on Food
AGENCY: Environmental Protection Agency (EPA).
ACTION: Notice.
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SUMMARY: This notice announces the initial filing of a pesticide
petition proposing the establishment of regulations for residues of a
certain pesticide chemical in or on various food commodities.
DATES: Comments, identified by docket identification (ID) number OPP-
2005-0017, must be received on or before May 9, 2005.
ADDRESSES: Comments may be submitted electronically, by mail, or
through hand delivery/courier. Follow the detailed instructions as
provided in Unit I. of the SUPPLEMENTARY INFORMATION.
FOR FURTHER INFORMATION CONTACT: Mary Waller, Registration Division
(7505C), Office of Pesticide Programs, Environmental Protection Agency,
1200 Pennsylvania Ave., NW., Washington, DC 20460-0001; telephone
number: (703) 308-9354; e-mail address: waller.mary@epa.gov.
SUPPLEMENTARY INFORMATION:
I. General Information
A. Does this Action Apply to Me?
You may be potentially affected by this action if you an
agricultural producer, food manufacturer, or pesticide manufacturer.
Potentially affected entities may include, but are not limited to:
Crop production (NAICS 111)
Animal production (NAICS 112)
Food manufacturing (NAICS 311)
Pesticide manufacturing (NAICS 32532)
This listing is not intended to be exhaustive, but rather provides
a guide for readers regarding entities likely to be affected by this
action. Other types of entities not listed in this unit could also be
affected. The North American Industrial Classification System (NAICS)
codes have been provided to assist you and others in determining
whether this action might apply to certain entities. If you have any
questions regarding the applicability of this action to a particular
entity, consult the person listed under FOR FURTHER INFORMATION
CONTACT.
[[Page 17998]]
B. How Can I Get Copies of this Document and Other Related Information?
1. Docket. EPA has established an official public docket for this
action under docket ID number OPP-2005-0017. The official public docket
consists of the documents specifically referenced in this action, any
public comments received, and other information related to this action.
Although a part of the official docket, the public docket does not
include Confidential Business Information (CBI) or other information
whose disclosure is restricted by statute. The official public docket
is the collection of materials that is available for public viewing at
the Public Information and Records Integrity Branch (PIRIB), Rm. 119,
Crystal Mall 2, 1801 S. Bell St., Arlington, VA. This docket
facility is open from 8:30 a.m. to 4 p.m., Monday through Friday,
excluding legal holidays. The docket telephone number is (703) 305-
5805.
2. Electronic access. You may access this Federal Register document
electronically through the EPA Internet under the ``Federal Register''
listings at http://www.epa.gov/fedrgstr/.
An electronic version of the public docket is available through
EPA's electronic public docket and comment system, EPA Dockets. You may
use EPA Dockets at http://www.epa.gov/edocket/ to submit or view
public comments, access the index listing of the contents of the
official public docket, and to access those documents in the public
docket that are available electronically. Although not all docket
materials may be available electronically, you may still access any of
the publicly available docket materials through the docket facility
identified in Unit I.B.1. Once in the system, select ``search,'' then
key in the appropriate docket ID number.
Certain types of information will not be placed in the EPA Dockets.
Information claimed as CBI and other information whose disclosure is
restricted by statute, which is not included in the official public
docket, will not be available for public viewing in EPA's electronic
public docket. EPA's policy is that copyrighted material will not be
placed in EPA's electronic public docket but will be available only in
printed, paper form in the official public docket. To the extent
feasible, publicly available docket materials will be made available in
EPA's electronic public docket. When a document is selected from the
index list in EPA Dockets, the system will identify whether the
document is available for viewing in EPA's electronic public docket.
Although not all docket materials may be available electronically, you
may still access any of the publicly available docket materials through
the docket facility identified in Unit I.B.1. EPA intends to work
towards providing electronic access to all of the publicly available
docket materials through EPA's electronic public docket.
For public commenters, it is important to note that EPA's policy is
that public comments, whether submitted electronically or in paper,
will be made available for public viewing in EPA's electronic public
docket as EPA receives them and without change, unless the comment
contains copyrighted material, CBI, or other information whose
disclosure is restricted by statute. When EPA identifies a comment
containing copyrighted material, EPA will provide a reference to that
material in the version of the comment that is placed in EPA's
electronic public docket. The entire printed comment, including the
copyrighted material, will be available in the public docket.
Public comments submitted on computer disks that are mailed or
delivered to the docket will be transferred to EPA's electronic public
docket. Public comments that are mailed or delivered to the docket will
be scanned and placed in EPA's electronic public docket. Where
practical, physical objects will be photographed, and the photograph
will be placed in EPA's electronic public docket along with a brief
description written by the docket staff.
C. How and to Whom Do I Submit Comments?
You may submit comments electronically, by mail, or through hand
delivery/courier. To ensure proper receipt by EPA, identify the
appropriate docket ID number in the subject line on the first page of
your comment. Please ensure that your comments are submitted within the
specified comment period. Comments received after the close of the
comment period will be marked ``late.'' EPA is not required to consider
these late comments. If you wish to submit CBI or information that is
otherwise protected by statute, please follow the instructions in Unit
I.D. Do not use EPA Dockets or e-mail to submit CBI or information
protected by statute.
1. Electronically. If you submit an electronic comment as
prescribed in this unit, EPA recommends that you include your name,
mailing address, and an e-mail address or other contact information in
the body of your comment. Also include this contact information on the
outside of any disk or CD ROM you submit, and in any cover letter
accompanying the disk or CD ROM. This ensures that you can be
identified as the submitter of the comment and allows EPA to contact
you in case EPA cannot read your comment due to technical difficulties
or needs further information on the substance of your comment. EPA's
policy is that EPA will not edit your comment, and any identifying or
contact information provided in the body of a comment will be included
as part of the comment that is placed in the official public docket,
and made available in EPA's electronic public docket. If EPA cannot
read your comment due to technical difficulties and cannot contact you
for clarification, EPA may not be able to consider your comment.
i. EPA Dockets. Your use of EPA's electronic public docket to
submit comments to EPA electronically is EPA's preferred method for
receiving comments. Go directly to EPA Dockets at http://www.epa.gov/edocket/
, and follow the online instructions for submitting comments.
Once in the system, select ``search,'' and then key in docket ID number
OPP-2005-0017. The system is an ``anonymous access'' system, which
means EPA will not know your identity, e-mail address, or other contact
information unless you provide it in the body of your comment.
ii. E-mail. Comments may be sent by e-mail to opp-docket@epa.gov,
Attention: Docket ID Number OPP-2005-0017. In contrast to EPA's
electronic public docket, EPA's e-mail system is not an ``anonymous
access'' system. If you send an e-mail comment directly to the docket
without going through EPA's electronic public docket, EPA's e-mail
system automatically captures your e-mail address. E-mail addresses
that are automatically captured by EPA's e-mail system are included as
part of the comment that is placed in the official public docket, and
made available in EPA's electronic public docket.
iii. Disk or CD ROM. You may submit comments on a disk or CD ROM
that you mail to the mailing address identified in Unit I.C.2. These
electronic submissions will be accepted in WordPerfect or ASCII file
format. Avoid the use of special characters and any form of encryption.
2. By mail. Send your comments to: Public Information and Records
Integrity Branch (PIRIB) (7502C), Office of Pesticide Programs (OPP),
Environmental Protection Agency, 1200 Pennsylvania Ave., NW.,
Washington, DC 20460-0001, Attention: Docket ID Number OPP-2005-0017.
3. By hand delivery or courier. Deliver your comments to: Public
Information
[[Page 17999]]
and Records Integrity Branch (PIRIB), Office of Pesticide Programs
(OPP), Environmental Protection Agency, Rm. 119, Crystal Mall
2, 1801 S. Bell St., Arlington, VA, Attention: Docket ID
Number OPP-2005-0017. Such deliveries are only accepted during the
docket's normal hours of operation as identified in Unit I.B.1.
D. How Should I Submit CBI to the Agency?
Do not submit information that you consider to be CBI
electronically through EPA's electronic public docket or by e-mail. You
may claim information that you submit to EPA as CBI by marking any part
or all of that information as CBI (if you submit CBI on disk or CD ROM,
mark the outside of the disk or CD ROM as CBI and then identify
electronically within the disk or CD ROM the specific information that
is CBI). Information so marked will not be disclosed except in
accordance with procedures set forth in 40 CFR part 2.
In addition to one complete version of the comment that includes
any information claimed as CBI, a copy of the comment that does not
contain the information claimed as CBI must be submitted for inclusion
in the public docket and EPA's electronic public docket. If you submit
the copy that does not contain CBI on disk or CD ROM, mark the outside
of the disk or CD ROM clearly that it does not contain CBI. Information
not marked as CBI will be included in the public docket and EPA's
electronic public docket without prior notice. If you have any
questions about CBI or the procedures for claiming CBI, please consult
the person listed under FOR FURTHER INFORMATION CONTACT.
E. What Should I Consider as I Prepare My Comments for EPA?
You may find the following suggestions helpful for preparing your
comments:
1. Explain your views as clearly as possible.
2. Describe any assumptions that you used.
3. Provide copies of any technical information and/or data you used
that support your views.
4. If you estimate potential burden or costs, explain how you
arrived at the estimate that you provide.
5. Provide specific examples to illustrate your concerns.
6. Make sure to submit your comments by the deadline in this
notice.
7. To ensure proper receipt by EPA, be sure to identify the docket
ID number assigned to this action in the subject line on the first page
of your response. You may also provide the name, date, and Federal
Register citation.
II. What Action is the Agency Taking?
EPA has received a pesticide petition, as follows, proposing the
establishment and/or amendment of regulations for residues of a certain
pesticide chemical in or on various food commodities under section 408
of the Federal Food, Drug, and Cosmetic Act (FFDCA), 21 U.S.C. 346a.
EPA has determined that this pesticide petition contains data or
information regarding the elements set forth in FFDCA section
408(d)(2); however, EPA has not fully evaluated the sufficiency of the
submitted data at this time or whether the data support granting of the
pesticide petition. Additional data may be needed before EPA rules on
the petition.
List of Subjects
Environmental protection, Agricultural commodities, Feed additives,
Food additives, Pesticides and pests, Reporting and recordkeeping
requirements.
Dated: March 28, 2005.
Lois Rossi,
Director, Registration Division, Office of Pesticide Programs.
Summary of Petition
The petitioner summary of the pesticide petition (PP) is printed
below as required by FFDCA section 408(d)(3). The summary of the
petition was prepared by the petitioner and represents the view of the
petitioner. The petition summary announces the availability of a
description of the analytical methods available to EPA for the
detection and measurement of the pesticide chemical residues or an
explanation of why no such method is needed.
Arvesta Corporation as agent for Hokko Chemical Industry Co., Ltd.
PP 3E6579
EPA has received pesticide petition 3E6579 from Arvesta
Corporation, 100 First St., Suite 1700, San Francisco, CA 94105 as
agent for Hokko Chemical Industry Co. Ltd. 4-20, Nihonbashi Hongokucho
4 Chome, Chuo-Ku, Tokyo 103-8341, Japan, proposing, pursuant to section
408(d) of the Federal Food, Drug, and Cosmetic Act (FFDCA), 21 U.S.C.
346a(d), to amend 40 CFR part 180 by establishing tolerances for
residues of kasugamycin, 1L-1,3,4/2,5,6-1-deoxy-2,3,4,5,6-pentahydroxy-
cyclohexyl-2-amino-2,3,4,6-tetradeoxy-4-([alpha]-iminoglycino)-[alpha]-
D-arabino-hexopyranoside, in or on the raw agricultural commodity
fruiting vegetables (Crop Group 8) at 0.04 parts per million (ppm),
tomato juice at 0.06 ppm, tomato puree at 0.06 ppm, and tomato paste at
0.25 ppm. EPA has determined that the petition contains data or
information regarding the elements set forth in FFDCA section
408(d)(2). However, EPA has not fully evaluated the sufficiency of the
submitted data at this time or whether the data supports granting of
the petition. Additional data may be needed before EPA rules on the
petition.
A. Residue Chemistry
1. Plant metabolism. The nature of residues of kasugamycin in
tomato was investigated using \14\C radiolabeled kasugamycin. Parent
kasugamycin was the primary component in both fruit and foliage. The
main metabolite in fruit, present at a maximum level of 0.01 ppm, was
identified as kasugamycinic acid, resulting from the conversion of the
iminomethyl function to a carboxylic acid. Additional investigation of
extracts from foliage indicated the presence of:
i. 2-N-acetyl kasugamycin, formed by acylation of the primary
amine.
ii. Kasuganobiosamine, formed by loss of the carboxylic acid
function of kasugamycinic acid.
iii. Conjugates of kasugamycin and kasugamycinic acid.
However, of the minor metabolites found in the foliage, only the
conjugates were observed in tomato fruit.
2. Analytical method. A practical analytical method for detecting
and measuring levels of kasugamycin has been developed and validated in
all appropriate agricultural commodities. This analytical method is
suitable for monitoring of food with residues at the levels proposed
for the tolerances. The limit of quantitation (LOQ) for this method is
0.04 ppm. An independent laboratory validation of the residue
analytical method was successful.
3. Magnitude of residues. The number of field residue trials
required for an import tolerance is based on the percent of total
consumed crop commodity attributed to imports from countries where the
product is or is intended to be registered for use on the crop. The
number of trials may be reduced if a crop group tolerance is requested.
Using this consideration, EPA determined that the residue field program
should consist of three trials on bell pepper, three trials on non-bell
pepper, and eight trials on tomato. Field residue trials in support of
this import tolerance were conducted at sites representative of
locations in which the product will be used on the intended crops with
applications at the
[[Page 18000]]
maximum use rate for each crop. As a result of the field trials, the
tolerance proposed for the fresh fruiting vegetables is 0.04 ppm. A
tomato processing study was not conducted. However, using the
detectable levels of kasugamycin residues in the tomato fruits, the
expected levels of residues in tomato juice, tomato puree, and tomato
paste were calculated using the maximum theoretical concentration
factors from the harmonized test guideline OPPTS 860.1520 of 1.4, 1.4,
and 5.5, respectively. As a result of these calculations, the following
tolerances are proposed for tomato processing commodities: 0.06 ppm
(tomato juice), 0.06 ppm (tomato puree), and 0.25 ppm (tomato paste).
B. Toxicological Profile
A full battery of toxicology testing including studies of acute,
subchronic, chronic, oncogenicity, developmental, reproductive, and
genotoxicity effects is available for kasugamycin. The acute oral
toxicity, the only acute testing required for import tolerances, is
low. Subchronic and chronic studies exhibit no-observed-effects-level
(NOEL) values from a low 5 milligram/kilogram/day (mg/kg/day) (2-year
chronic toxicity in dogs) to 135 mg/kg/day (13-week feeding study with
mice). Kasugamycin is not oncogenic and weight-of-evidence indicates it
is not genotoxic. There are no concerns of developmental or
reproductive effects. The lowest chronic NOEL of 3 mg/kg/day is taken
from the rabbit maternal toxicity in the developmental study.
1. Acute toxicity. The acute oral toxicity for kasugamycin (the
only study required for import tolerances establishment) is very low.
The acute oral Lethal Dose to 50% (LD50) is greater than
5,000 mg/kg, which will gives kasugamycin a Toxicity Category IV.
2. Genotoxicty. Kasugamycin was negative in the following assays:
Bacterial reverse mutation, Chinese hamster ovary (CHO), chromosomal
aberration (in vitro), mammalian erythrocyte micronucleus, unscheduled
DNA synthesis, in vitro mammalian cell gene mutation. Overall, it is
unlikely that kasugamycin presents a genetic hazard.
3. Reproductive and developmental toxicity. Developmental effects
of kasugamycin were studied in rats and rabbits and multi-generational
effects on reproduction were studied in rats.
i. Rat developmental. In the developmental toxicity study conducted
with rats the maternal NOEL is 40 mg/kg/day based on reduced body
weight gain and food consumption. There were no developmental effects
and the developmental NOEL is 1,000 mg/kg/day the highest dose tested.
ii. Rabbit developmental. In the developmental toxicity study
conducted with rabbits the maternal NOEL is 3 mg/kg/day based on
reduced body weight gain and food consumption, two abortions and one
total litter loss. There were no developmental effects and the
developmental NOEL is 10 mg/kg/day the highest dose tested.
iii. Reproduction. In the rat reproduction study the parental NOEL
is 10 mg/kg/day based on decrease body weight. The reproductive NOEL is
50 mg/kg/day (based on increase length of time required for mating).
4. Subchronic toxicity. Subchronic toxicity studies have been
conducted with kasugamycin in the rat, mouse, and dog.
i. Rats. Kasugamycin technical was tested in rats in a 13-week
feeding study. Observations were altered blood biochemistry, elevated
absolute and relative cecum weights, and increased relative kidney
weights. Both males and females at the high dose increased their water
consumption compared to controls. In addition, males in the 6,000 ppm
group had an increase in eosinophilic bodies in the proximal tubule
cells of the kidney and the females had an increase in foam cell
aggregation in the lungs. Foam cells generally contained lipid droplets
and may be derived from macrophage. The NOEL is 300 ppm (17.53 mg/kg/
day in males and 22.33 mg/kg/day in females)
ii. Mice. A 13-week feeding study in mice was conducted. Effects
included ulceration and inflammation of the anus, altered
hematological, and clinical chemistry. Females in the 10,000 ppm group
had a diffuse basophilia and hyperplasia of the epithelium of the
proximal tubule of the kidney. Dilatation of the seminiferous tubules
of males was observed in the high-dose group and sometimes associated
with degeneration of the seminiferous epithelium. The NOEL is 1,000 ppm
(135.4 mg/kg/day in males and 170.9 mg/kg/day in females).
iii. Dog. A 13-week oral toxicity study was conducted in beagle
dogs. Effects included decreased food consumption and body weight gain,
discolored feces, tongue lesions, swollen mouth, and excessive
salivation. The NOEL is 300 ppm (10.59 mg/kg/day in males and 11.44 mg/
kg/day in females).
5. Chronic toxicity. Kasugamycin has been tested in chronic studies
with dogs, rats, and mice.
i. Rats. In a 24-month combined chronic/oncogenicity study in rats
findings were increased cecum weights and kidney weights, increased
brown pigment deposition in the kidney proximal tubules and an
increased incidence of foam cell aggregation in the lungs. No
significant increase in neoplastic lesions. The NOEL is 300 ppm (10.59
mg/kg/day in males and 11.44 mg/kg/day in females).
ii. Mice. Kasugamycin was administered in diet to mice for 78
weeks. Observations were lower absolute and relative spleen weights for
males at 1,500 ppm. The NOEL is 300 ppm (34.94 mg/kg/day in males and
42.49 mg/kg/day in females)
iii. Dog. Kasugamycin was administered for 52 weeks to dogs. The
administration of 3,000 ppm kasugamycin was associated with minimally
higher urea nitrogen and creatinine, lower urine volume, and higher
urine specific gravity. The NOEL is 1,000 ppm.
iv. Carcinogenicity. Kasugamycin did not produce carcinogenicity in
adequately designed chronic studies with rats or mice. Arvesta
Corporation anticipates that the cancer classification of kasugamycin
will be ``E'' (no evidence of carcinogenicity for humans).
6. Animal metabolism. Following administration to the rodent, the
majority of kasugamycin is excreted into the feces, a small amount was
eliminated in the urine, and less than 0.1% of the radioactivity was
retained in the carcass. Kasugamycin is not excreted in the bile and
enterohepatic circulation of kasugamycin does not occur. There were no
apparent sex related differences.
7. Metabolite toxicology. No metabolites of significant expected
toxicity were identified in the animal metabolism study.
8. Endocrine disruption. Data from the subchronic studies indicate
that there is no expected endocrine disruption effects.
C. Aggregate Exposure
1. Dietary exposure. Acute and chronic dietary analyses were
conducted to estimate exposure to potential kasugamycin residues in or
on the following crops: Fruiting vegetables using CARES software
developed by CropLife and DietRisk\TM\ TSG's software. Kasugamycin is
not used in the United States so there is no need for water exposure
analysis. In calculating the exposure the following assumptions were
made: Tolerance level of residues, and 100% imported crops treated with
kasugamycin.
2. Food--i. The acute dietary margin of exposure (MOE) estimates
for kasugamycin residues in food at 99.9\th\ percentile of females age
13-49 is higher
[[Page 18001]]
than 12,000 based on a NOEL of 3 mg/kg/day from the developmental
toxicity study. The acute dietary exposure to kasugamycin for this
group is less than 1% of the reference dose (RfD) which was defined as
the NOEL from the developmental study in rabbits including an
uncertainty factor of 100 (NOEL = 3 mg/kg/day, RfD = 0.03 mg/kg/day).
ii. Chronic dietary exposure to kasugamycin residues of females age
13-49 was less than 0.1% of the chronic RfD. The RfD was defined as the
NOEL from the developmental study in rabbits including an uncertainty
factor of 100 (NOEL = 3 mg/kg/day, RfD = 0.03 mg/kg/day).
These values are based on tolerance level residues and 100%
imported crops treated with kasugamycin. These can be considered
conservative values.
D. Cumulative Effects
Section 408(b)(2)(D)(v) of FFDCA requires that the Agency must
consider ``available information'' concerning the cumulative effects of
a particular pesticide's residues and ``other substances that have a
common mechanism of toxicity.'' Available information in this context
includes not only toxicity, chemistry, and exposure data, but also
scientific policies and methodologies for understanding common
mechanism of toxicity and conducting cumulative risk assessments. For
most pesticides, although the Agency has some information in its files
that may turn out to be helpful in eventually determining whether a
pesticide shares a common mechanism of toxicity with any other
substances, EPA does not at this time have methodologies to resolve the
complex scientific issues concerning common mechanism of toxicity in a
meaningful way for most registered pesticides. However, the mode of
action of kasugamycin differs substantially from those of other
aminoglycoside antibiotics. Because kasugamycin acts at a different
point in protein syntheses than that affected by other aminoglycoside
antibiotics, cross-resistance between kasugamycin and other similar
antibiotics is extremely unlikely. In addition, kasugamycin is active
only against phytopathogenic fungi and bacteria. Because kasugamycin is
not effective against common human or animal pathogens, it has never
been employed as a human or veterinary-use antibiotic. For the same
reason, there is essentially no possibility that use of kasugamycin as
a plant protection agent can give rise to antibiotic resistance in
human or animal pathogens.
E. Safety Determination
1. U.S. population. Using the conservative assumptions of tolerance
level residues and 100% of imported crops treated with kasugamycin,
based on the completeness and reliability of the toxicity data, it is
concluded that dietary exposure to proposed uses of kasugamycin will
utilize less than 0.1% of the chronic RfD and less than 1% of the acute
RfD for the females of childbearing age population group, the most
sensitive group, and is likely to be much less, as more realistic data
and models are developed. The MOE from the dietary exposure for the
same group is higher than 12,000 and is likely to be higher, as more
realistic data and models are developed. The Agency has no cause for
concern if total acute residue contribution is less than 100% of the
acute RfD, because the RfD represents the level at or below which daily
exposure over a lifetime will not pose appreciable risk to human
health. Therefore, there is a reasonable certainty that no harm will
occur to the U.S. population from dietary exposure to residues of
kasugamycin.
2. Infants and children. The toxicological database for evaluating
pre- and post-natal toxicity for kasugamycin is complete with respect
to current data requirements. There are no special pre- and post-natal
toxicity for infants and children, based on the results of the rat and
rabbit developmental toxicity studies or the 2-generation reproductive
toxicity study in rats. In all cases there were no developmental and
offspring toxicity effects at the maternal toxicity level. Using the
conservative assumption described in Unit E.1., based on the
completeness and reliability of the toxicity data, it is concluded that
the exposure to the proposed uses of kasugamycin on imported crops will
utilize at most 1.0% of the acute or chronic RfD. Therefore, there is a
reasonable certainty that no harm will occur to infants and children
from exposure to residues of kasugamycin.
F. International Tolerances
CODEX Maximum Residue Limits (MRLs) have not been established for
kasugamycin in either tomato or peppers, and a joint meeting on
pesticide residues (JMPR) review of kasugamycin residue data is not
scheduled. Spain has established an MRL for kasugamycin in tomato, at
0.05 ppm. There are no existing MRLs for kasugamycin in pepper.
[FR Doc. 05-6848 Filed 4-7-05; 8:45 am]
BILLING CODE 6560-50-S