United States
Environmental Protection
Agency
Environmental Monitoring and
Support Laboratory
Cincinnati OH 45268
Research and Development
EPA/600/S4-87/024 Jan. 1988
<>EPA Project Summary
GC-MS Suitability Testing of RCRA
Appendix VIII and Michigan List
Analytes
S. V. Lucas and R. A. Kornfeld
As a first step in a hierarchical scheme
to demonstrate the suitability of present
U.S. Environmental Protection Agency
(EPA) analysis methods and/or develop
new methodology, the gas chromato-
graphic (GC) separation and mass
spectrometric (MS) detection char-
acteristics of 328 toxic and/or hazard-
ous organic materials ware investigated.
The analytes in question are the non-
priority pollutant organic substances in
the RCRA Appendix VIII listing plus
those on the "Michigan List."
Volatile and semivolatile analytes were
tested using the GC-MS conditions
specified in EPA Methods 8240 and
8270, respectively, as modified by the
Contractor Laboratory Program (CLP)
protocol. Standard mixtures of analytes
in organic solvent were analyzed by
septum injection onto the analytical
column without any prior sample
workup procedures.
For analytes that proved suitable for
GC-MS analysis by Methods 8240 and
8270, the relevant characteristics for
GC retention and for MS detection are
reported. For analytes not detected by
GC-MS or omitted a priori from testing,
recommendations for future work are
made.
This Project Summary was developed
by EPA's Environmental Monitoring and
Support Laboratory, Cincinnati, OH, to
announce key findings of the research
project that Is fully documented In a
separate report of the same title (see
Project Report ordering Information at
back).
Introduction
The Resource Conservation and Re-
covery Act (RCRA) specifies over 300
toxic organic compounds in its Appendix
VIII listing which may be used to identify
hazardous wastes. In response to a peti-
tion by the state of Michigan, the U.S.
Environmental Protection Agency (EPA)
has proposed the amendment of RCRA
Appendix VIII by the addition of over 100
other organic compounds. EPA is cur-
rently attempting to validate analytical
methods for as many of these 400 plus
compounds as possible. A hierarchical
approach to these validation efforts is
being pursued.
An example of a hierarchical approach
to the development and validation of
analytical methods for the determination
of organic compounds in wastes is pre-
sented in Figure 1. The final report com-
pletely describes the procedures and
presents fully the results obtained from
implementation of this first phase of the
hierarchical approach. The compounds
were classified as candidates for the
application of either EPA Method 8240 or
Method 8270 to test for volatile or semi-
volatile organic compounds, respectively.
Some compounds were not tested be-
cause they fell into one of the following
categories:
• Priority pollutants — The chromato-
graphic behavior of these compounds
has already been thoroughly char-
acterized.
• Unstable — Compounds known to
degrade rapidly in aqueous sample
matrices.
-------�
• Not amenable to gas chromatography
(GC) — Compounds known to be too
polar and/or too thermally labile to
elute using Method 8240 or Method
8270 conditions.
• Not available — Compounds for
which standards were not available
from the EPA repository or from
commercial sources.
For compounds determined to be amen-
able to the two methods, the following
data were obtained:
• GC Performance — retention
characteristics.
• Mass Spectral (MS) Performance —
response factors, key ions for detec-
tion and quantification using ex-
tracted ion current profiles (EICP).
Figure 1 shows the context in which
the results of this project lead to sub-
sequent method development activities.
Implementation of the hierarchical
method development approach is ex-
pected to contribute to the development
of a suite of analytical methods with a
limited number of analytic procedures for
determining a large proportion of the
more than 400 organic compounds in the
amended RCRA Appendix VIII. Covering
extraction, cleanup, and determinative
steps, this limited number of analytical
procedures would form the core of a
generic approach to the selection of ap-
propriate analytical methods for hazardous
wastes. The proposed system is generic
in the sense that the specifications of
type of analyte, type of matrix, and type of
sensitivity and required specificity would
generate, from the limited suite of com-
ponent analytical procedures, the most
appropriate set of analysis conditions.
This type of generic approach would
permit reduction in the number and
variety of methods required to characterize
wastes and should provide cost benefits
both to the government and to the regu-
latory community. Also, the generic ap-
proach would facilitate periodic updates
of the method, as new information be-
comes available about specific analytes
in specific matrices. Further, areas re-
quiring method modification or method
development could be clearly identified
and easily prioritized for research resource
allocation.
Experimental Approach
The initial set of analytes consisted of
organic compounds included in RCRA
Appendix VIII (Federal Register, October
1, 1984) plus those included in the
Michigan petition (Federal Register,
December, 1984) minus the EPA priority
Analyte
1. HPLC
2. Derivatization
3. Non-chromatographic
1. Add to list
2. Test in
non-MS
methods
1. Add to list
2. Test in
non-MS
methods
Evaluate other options.
1 Heated PTD
2. Direct injection
3. Micro extraction
4. Distillation
5. Non-GC methods
1. Modified extraction
conditions (SPE, other
solvents, etc.)
2. Develop/improve
cleanup procedures
I
Figure 1, Hierarchical approach for analytical method development for organic RCRt
analytes.
pollutants. After eliminating redundancies
in the two lists, the remaining compounds
were classified by their predicted suit-
ability for SW 846 Method 8240 (volatiles),
Method 8270 (semi-volatiles), or for their
predicted inability to be determined by
either method.
Sources for the selected analytes were
identified in the following order of priority:
1) the EPA repositories of reference
compounds and pesticides (EMSL - Las
Vegas and RTP), 2) the EPA repository of
certified solutions (EMSL - Cincinnati),
and 3) commercial suppliers. GC-MS
suitability studies utilized analyte mix-
tures prepared after consideration of
chemical reactivity.
For most of the analytes, individual
analyte concentrations in the volatile
mixtures were 200 /ig/mL, for a few
analytes predicted to exhibit lower re-
sponse factors; concentrations were 400
/jg/mL. Injections of volatile analytes
provided a minimum of 300 ng of analyte
on column. The concentrations of in-
dividual semivolatile analytes in the in-
jection standards were 40 /ug/mL For
analytes not detected on the first attempt
higher concentrations were employed
ranging from 50-400 /ig/mL. Injections
of semivolatile analytes provided a mini
mum of 80 /ug of analyte to the splitless
injection evaporator cavity. The usua
packed GC column, 1 percent SP1000/
Carbopack B (Supelco), was used fo
volatile compounds, and a 30 meter ;
0.25 mm ID fused silica coated with 0.2C
micron immobilized methyl phenyl sili
cone (J&W DB-5) was used for semi
volatile compounds.
Internal standards specified in the CLF
for both volatile and semivolatile analyse:
were used to provide measures for both
GC relative retention indices and MS
detection response factors. Surrogate
standards specified in the CLP were in-
cluded in volatile analyte mixtures bu
not in the semivolatile mixtures. In the
latter case, data interpretation would be
more difficult with little increase in use-
fulness of results. In all cases, the CLF
GC and MS analysis conditions and ME
quality control checks on ion source
tuning were used.
-------�
Results and Discussion
Selection and Procurement of
Analytes to be Tested
After elimination of redundancies, the
combined Appendix VIII and Michigan
analyte sets contain 440 compounds, 112
of which are already thoroughly char-
acterized EPA priority pollutants. Thus,
328 substances qualified for the present
study. Each substance was classified
according to its amenability to analysis by
Method 8240 (volatile analytes), Method
8270 (semivolatile analytes), or by neither
method. Eight of the compounds are
classified as both volatile and semivolatile
since, after failing to elute in the volatile
compound testing, they were carried into
the semivolatile compound testing.
Table 1 lists 58 analytes that are omitted
a priori from GC-MS suitability testing.
Reasons for a priori omission and sug-
gestions for future method development
can be classified as follows:
• Acids — 14 Compounds. Typically,
these acids are carboxylic acids (or
of comparable strength) and require
derivatization to achieve acceptable
GC performance.
• Nonvolatile — 12 compounds. These
analytes are so polar and/or of such
high molecular weight that there is
essentially no possibility of their elu-
tion from a GC column. Typical of
these compounds are macrolytic
antibiotics and dye molecules for
which HPLC, rather than a derivati-
zation-GC approach is ap-
propriate for most cases.
• Hydrolytically or otherwise unstable
— 9 compounds. Since groundwater
and wet soils and sludges are sample
matrices of interest, there is no need
to demonstrate analysis capability
for compounds which decompose
rapidly in these sample types.
• Aldehydes — 6 compounds. Special
GC conditions have been used suc-
cessfully for a number of these
analytes but, generally, the associ-
ated sample workup procedures are
not fully successful in preserving
these reactive analytes prior to their
detection. Hence derivatization fol-
lowed by HPLC with UV detection,
which has been shown to be sensi-
tive and reproducible for formalde-
hyde, is clearly the favored analytical
TaWe 1. Analytes Omitted A Priori From GC-MS Suitability Testing
No.
1
2
3
4
5
6
7
a
9
10
11
12
13
14
15
16
17
18
19
20
21
22
23
24
25
26
27
28
29
30
31
32
33
34
35
36
37
38
39
40
41
42
43
44
45
46
47
48
49
50
51
52
53
54
55
56
57
58
Substance
Acetaldehydefb)
Acetyl chloride
Actinomycin D
Aflatoxins(b)
Aniline hydrochloride
0-Anisidine hydrochloride
Azaserine
Benzal chloride
Benzenearsonic acid
Benzidine sulfate
Benzotrichloride
Chlorambucil
Chloroacetaldehyde(b)
Coal tars
Creosote
Crotonaldehyde(b)
Cycasin
2.4-D
Daunomycin
Dimethylcarbamoyl chloride
Diphenylamine(c)
5,5-Diphenylhydantoin monosodium salt
2,4-Dithiobuiret
Endothal
Epinephrine
Ethylene bis-dithiocarbamates
Fluoroacetic acid, sodium salt
Formaldehyde(bl
Formic acid
Glycidaldehyde (b)
Hydrazine
Ketene
Lasiocarpine
Malachite green
Melphalan
Methyl chlorocarbonate
Mitomycin C
Monocrotaline
Nitrogen mustard N-oxide
N-Nitrososarcosine
Paraldehyde{b)
Peroxyacetic acid
Phenesterin
Phenyl dichloroarsine
Polybrominated biphenyls(b)
Polychlorinated biphenylsfb)
Reserpme
Semicarbazide
Silvex
Streptozotocin
2.4.5-T
2.3.7.8-TCDD(bJ
Thiosemicarbazide
Thiourea
Thiram(d)
Tnchloromethanesulfenyl chloride
Trypan blue
Ziram
ListfaJ
a
8
M
8
M
M
8
8
8
M
8
8
8
8
8
8
8
8
8
8
8
M
a
8
8
8
8
8
8
8
8
M
8
M
8
8
8
M
a
8
8
M
M
8
M
8
8
M
8
8
8
8
8
8
a
8
8
M
CAS No.
75-07-0
75-36-5
50-76-0
98-05-5
142-04-1
134-29-2
1 15-02-6
98-87-3
98-05-5
531-86-2
98-07-7
305-03-3
107-20-0
20830-81-3
8001-58-9
123-73-9
14901-08-7
94-75-7
20830-81-3
79-44-7
62-74-8
630-93-3
541-53-7
129-67-9
51-43-4
142-59-6
62-74-8
50-00-0
64-18-6
765-34-4
302-01-2
463-51-4
303-34-4
569-64-2
148-82-3
79-22-1
50-07-7
315-22-0
302-70-5
13256-22-9
123-63-7
79-21-0
3546-10-9
696-28-6
59536-65-1
1336-36-3
50-55-5
57-56-7
93-72-1
18883-66-4
93-76-5
1746-01-6
79-19-6
62-56-6
137-26-8
594-42-3
72-57-1
137-30-4
la) 8 = Appendix VIII; M = Michigan List.
(b) Partially or fully demonstrated method for selected matrices already exists.
(c) Diphenylamine has been well characterized by GC-MS since the priority pollutant
N-nitrodiphenyl-amine has been thoroughly demonstrated to quantitatively decompose to
diphenylamine upon GC injection.
(d) This family of analytes have been successfully determined in aqueous media by GC-
Hall/Sulfur analysis of carbon disulfide decomposition product.
-------�
approach for these compounds. Thus,
there was no need to include them
in GC method testing.
Redundancies — 5 compounds.
Typically, these compounds are salts
of a free base also listed as an
analyte. Diphenylamine was con-
sidered redundant with the priority
pollutant, N-nitrosodiphenylamine
since the latter is known to decom-
pose quantitatively to the former in
GC injectors.
Inappropriate for inclusion in the
present scope for miscellaneous
reasons — 12 substances. Some
analytes were considered inappro-
priate because they can hardly be
considered organic analytes. Ex-
amples of this category include
hydrazine, thiosemicarbizide, semi-
carbizide, thiourea and dithiobiuret.
Others are currently, or expected to
be addressed by other specialized
methods. Examples of this category
include tetrachlorodibenzodioxin and
polychlorinated and polybrominated
biphenyls. Two substances, coal tars
and creosote, are too heterogeneous
for inclusion in Method 8270.
Epinephrine had to be omitted since
it could not be dissolved at suffici-
ently high concentration in any rea-
sonable GC injection solvent.
Some 32 analytes could not be obtained
in time to be included in this work and
are listed in Table 2. One of these, chloral,
is available as the hydrate which was
included in the volatile analyte testing.
Thus, the summary listings show 31
analytes as "unavailable."
Results of Volatile Analyte Testing
Table 3 lists 54 volatile analytes tested
with Method 8240 GC conditions. The
status of each analyte is indicated: satis-
factorily detected (S); detected with a
response factor versus benzene-D6 below
Table 2. Volatile and Semivolatile Analytes Not Obtainable in Time for Inclusion
No. Substance
List(a)
CAS No.
1
2
3
4
5
6
7
8
9
10
11
12
13
14
15
16
17
18
19
20
21
22
23
24
25
26
27
28
29
30
31
32
1 -Amino-2-methylanthraquinone
5-(Aminomethyl)-3-isoxazolol
Azinophos-ethyl
Benz(c)acridine
7,8-Benzfluoranthene
4-(Butylnitrosoamino)- 1 -butanol
Chloral(b)
Chloronaphazine
1 -<2-Chlorophenyl)thiourea
Citrus Red No. 2
1 ,2:5.6-Dibenzacridine
3.4:5.6-Dibenzocarbazole
Dibenzofa. i)pyrene(c)
Dibenzo(a.h)pyrene
Diethylarsine
1 ,2-Diethylhydrazine
Diisopropyl fluorophosphate
3.3-Dimethyl- 1 -(p-chlorophenyl)triazene
O, O-Dimethyl-S-methyl phosphorodithioate
Furathiazole
Hexaethyl tetraphosphate
4.4'-Methylenebis(2-methylaniline)
2-Methyl- 1 -nitroanthraquinone
Nifurthiazol
Niridazole
Nithiazide
N-Nitrosomethylvinylamine
N-Nitrosonornicotine
Phosacetim
4,4'- Thiodianiline
Trisfl -azridinyl)phosphine sulfide
Uracil mustard
M
8
M
8
8
M
8
8
8
8
8
8
8
8
8
8
8
M
8
M
8
M
M
M
M
M
8
8
M
M
8
8
82-28-0
2763-96-4
2642-71-9
225-51-4
205-82-3
3817-11-6
75-87-6
494-03-1
5344-82-1
6358-53-8
226-36-8
194-59-2
189-55-9
129-67-9
692-42-2
1615-80-1
55-91-4
7203-90-9
3288-58-2
531-82-8
757-58-4
838-88-0
129-15-7
3570-75-0
61-57-4
139-94-6
4549-40-0
16543-55-8
4104-14-7
139-65-1
66-75-1
(a) 8 = Appendix VIII; M = Michigan list.
(b) Chloral hydrate was substituted for chloral.
(c) Judged cost prohibitive for this program.
0.02 (LR), or not detected (ND). Thirty
three analytes were satisfactorily detecte
and six were detected with low responsi
factors. The very low response factor
will probably result in unacceptably higl
minimum detection limit (MDL) value:
for Method 8240.
Table 3 also lists 15 volatile analyte:
that were not detected under Metho<
8240 conditions. All of these analyte!
were analyzed at least twice, with thi
repeat analysis usually at 2- to 5-fok
higher levels than the original 300 nc
level. Three of these 15 analytes, hexa
chloropropene, tetranitromethane, am
thiophenol, were thought to have faile<
to elute due to boiling points and/o
polarities that were too high for th<
SP1000/Carbopack B column, and thesi
compounds were retested using th<
Method 8270 (semivolatile analyte
conditions.
Non-detection of the hydrazines anc
aziridines (6 analytes) was probably due
to extreme GC peak tailing on tru
SP1000/Carbopack B column. Five o
these nitrogen bases were also testec
with the semivolatile analytes. The sixth
N(2-hydroxyethyl)ethyleneimine, was not
tested due to its extreme polarity.
In the injector, 2-Butanone peroxide
apparently quantitatively decomposed tc
2-butanone. Methyl mercaptan apparently
coelutes with methanol on the SP1000/
Carbopack B column and would be sub-
stantially lost at the jet separator due tc
the presence of the methanol vapor dis-
placement of the helium carrier. The
remaining four undetected volatile com-
pounds, two haloethers, methyl iso-
cyanate, and 2-methyllactonitrile, were
not repeated in the semivolatile set since
they were both too volatile to be recovered
in a Kuderna-Danish (KD) distillation of
extraction solvent and were also known
to be chemically and/or hydrolytically
labile.
Results of Semivolatile
Analyte Testing
Table 4 lists the 185 semivolatile
analytes and the eight volatile analytes to
be retested with Method 8270 conditions.
The status of each analyte is indicated;
satisfactorily detected (S), expected to be
satisfactory for GC-MS determination
based on other information (ES), detected
with a response factor less than 0.02
versus phenanthrene-D10 (LR), or not
detected (ND). One hundred and twenty
eight analytes were detected with satis-
factory response factors and nine analytes
were detected with low response factors.
-------�
Table 3. GC-MS Suitability Testing Results for Volatile Analytes
No.
1
2
3
4
5
6
7
a
9
10
11
12
13
14
15
16
17
18
19
20
21
22
23
24
25
26
27
28
29
30
31
32
33
34
35
36
37
38
39
40
41
42
43
44
45
46
47
48
49
50
51
52
53
54
Substance
Acetonitrile
Ally/ alcohol
Allyl chloride
Benzyl chloride
Bis-(2-chloroethyl) sulfide
Bis(chloromethyl) ether
Bromoacetone
2-Butanone peroxide
2-Butanone
Carbon disulfide
Chloral hydrate
2-Chloroethanol
Chloromethyl methyl ether
Chloroprene
3 - Chloropropionitrile
1 . 2 -Dibromo -3 -chloropropane
Dibromomethane
1 ,4-Dichloro-2-butene
Dichlorodifluoromethane
1 . 3 -Dichloro-2-propan ol
1 ,2,3.4-Diepoxybutane
1 , 1 -Dimethylhydrazine
1 ,2-Dimethylhydrazine
1 ,4-Dioxane
Epichlorohydrm
Ethylene dibromide
Ethylene oxide
Ethylenimine
Ethyl methacrylate
Hexachloropropene
N-(2-Hydroxyethyl)ethyleneimine
2-Hydroxypropionitrile
Isobutyl alcohol
Malononitrile
Methacrylonitrile
2-Methylaziridine
Methylhydrazine
Methyl iodide
Methyl isocyanate
2-Methyl/actonitnle
Methyl mercaptan
Methyl methacrylate
Pentachloroethane
2-Picoline
Propargyl alcohol
(i-Propiolactone
Propionitrile
N-Propylamine
Pyndine
Styrene
1, 1 , 1 ,2-Tetrachloroethane
Tetranitromethane
Thiophenol
1 ,2.3- Trichloropropane
List(a)
8
8
8 M
8
8 M
8
8
8
8
8
8
M
a
8 M
8
8
8
8
8
8
8
8
8
8
8
8
a
8
8
8
M
M
8
8
8
8
8
8
8
8
8
8
8
8
8
M
8
8
8
M
8
8
8
8
RCRA
CAS No. Number
75-05-8
107-18-6
107-05-1
100-44-7
505-60-2
542-88-1
598-31-2
1338-23-4
78-93-3
75-15-0
75-87-6
107-07-3
107-30-2
126-99-8
542-76-7
96-12-8
74-95-3
764-41-0
75-71-8
96-23-1
1464-53-5
57-14-7
540-73-8
123-91-1
106-89-8
106-93-4
75-21-8
151-56-4
97-63-2
1888-71-7
1072-52-2
78-97-7
78-83-1
109-77-3
126-98-7
75-55-8
60-34-4
74-88-4
624-83-9
75-86-5
74-93-1
80-62-6
76-01-7
109-06-8
107-19-7
57-57-8
107-12-0
107-10-8
110-86-1
100-42-5
630-20-6
509-14-8
108-98-5
96-18-4
U003
POOS
U317
P028
P158
P017
U160
U034
P133
U046
U276
P027
U074
U085
U098
U099
U108
U115
P054
U118
U243
U289
U149
U152
P067
P068
U138
P064
P069
U162
U191
P102
U302
P101
U194
U196
U323
P112
P104
Status
Code(b)
S
S
S
S
LR
ND
S
ND
S
S
LR
LR
ND
S
S
S
S
S
S
S
ND
ND
S
S
S
S
ND
S
ND
ND
LR
S
S
S
ND
ND
S
ND
ND
ND
S
S
S
LR
S
S
LR
S
S
S
ND
ND
S
(a) 8 - Appendix VIII: M - Michigan list.
(b) LR- low response factor
S: suitable for GC-MS analysis
ND not detected in GC-MS data.
All of these latter nine analytes are highly
polar and are expected to be sensitive to
thermal decomposition in the injection
port.
Table 4 contains 11 analytes with the
status "ES." All 11 of these analytes are
suitably analyzed in Work Assignment 2-
08 which extracts analytes from spiked
aqueous standards, concentrated and
analyzed by fused silica capillary GC-FID.
Thus, although MS data was not obtained
in the WA 2-08 work, their non-detection
in the present work is anomalous. Except
for the two organophosphates, these "ES"
analytes in Table 4 are strongly basic
molecules; a possible explanation for their
non-detection is that the GC column used
was somewhat acidic, precluding satis-
factory elution.
Also listed in Table 4, are the 45
analytes for which non-detection in the
GC-MS data cannot be classified as
anomalous. Generally, these analytes are
highly polar, or labile to decomposition
before or during chromatography. Four
of these 45 analytes are aromatic dia-
mines, 1,2- and 1,3-phenylenediamine,
2,4-diaminoanisole, and 1,5-naphthalen-
diamine. These four analytes probably
can be analyzed by fused silica GC if
special precautions are taken to ensure
good performance for basic materials.
Ethylene thiourea (ETU) has been shown
in previous work at Battelle to be amen-
able to GC analysis using special condi-
tions. For another six analytes (acrylamide,
cycloheximide, 2-fluoroacetamide, niclo-
samide, oxydemeton-methyl, and thioace-
tamide) polarity, volatility and lability
considerations apparently do not account
for the non-detection, and, therefore, a
more thorough attempt to develop GC-
based methods might be successful. For
the remaining 34 analytes, the causes of
non-detection can be classified as one or
more of the following: exceptionally high
polarity, thermal or chemical lability, or
insufficient volatility. Recommendations
for further method development for these
analytes focus on HPLC techniques,
especially ion chromatography or post
column derivatization methods.
Conclusions and
Recommendations
After the elimination of redundancies,
the Appendix VIII and Michigan list com-
pounds include 440 organic compounds.
The classification of these compounds
and results of testing them for suitability
for inclusion in present volatile and
semivolatile analysis methods are sum-
marized as follows:
-------�
Analytes Considered
Tested for GC-MS Suitability 239*
Omitted Priority Pollutant 1 1 2
Omitted A Priori 58
Not obtainable 31
Total considered 440
Volatile Analyte Testing
Suitably Detected 33
Detected with Low
Response Factor 6
Nnt DptprtpH 1 ^
IWl LXOIOV*IOU 1 *J
Sub Total 33 + 21 = 54*
Semivolatile Analyte Testing
Suitably Detected 1 28
Expected to be
Suitable 1 1
Detected with Low
Response Factor 9
Not Detected 45
Sub Total 139 + 54 =193*
Total Suitable 1 72
Total Not Suitable 75
Total Tested 247*
* Eight of the analytes that failed volatile
testing were carried into the semi-
volatile testing. Two of these eight
analytes were suitably detected in
semivolatile testing.
For the 39 volatile and 1 37 semivolatile
compounds which were detected by GC-
MS analyses, key GC performance and
mass spectral data were obtained.
The general recommendation arising
from the data and results generated in
the studies presented in this report is to
continue implementation of the hier-
archical research strategy. The following
specific recommendations are made:
• The 39 volatile compounds detected
using the GC conditions of Method
8240 should be included in an evalu-
ation of the Method 5030 PTD
sample introduction.
• Extractability studies of the 137
semivolatile compounds detected
using the GC conditions of Method
8270 should be conducted.
• The 1 1 compounds which were
anomalously not detected should
receive more detailed examination.
• Twelve additional analytes that were
not detected should also receive
further direct GC investigation.
Table 4. GC-MS Suitability Testing Results for Semivolatile Analytes
RCRA
No. Substance List(a) CAS No. Number
1
2
3
4
5
6
7
8
9
10
11
12
13
14
15
16
17
18
19
20
21
22
23
Ojf
24
25
26
27
28
29
30
31
32
33
34
35
36
37
38
39
40
41
42
43
44
45
46
47
48
49
50
51
52
53
54
55
56
57
58
59
60
61
62
63
64
65
66
Acetophenone
2-Acetylaminofluorene
1 -Acetyl-2-thiourea
Acrylamide
Aldicarb
2-Aminoanthraquinone
Aminoazobenzene
4-Aminobiphenyl
3-Amino-9-ethylcarbazole
Amitrole
Anilazine
Aniline
o-Anisidine
Aramite
Aura mine
Azinphos-methyl
Barban
Benomyl
p-Benzoquinone
Bromoxynil
Brucine
Captafol
Captan
Carbaryl
Carbofuran
Carbophenothion
Chlorfen vinphos
4-Chloroaniline
Chlorobenzilate
5-Chloro-2-methylaniline
3-(Chloromethyl)pyridine hydrochloride
4-Chloro- 1 ,3-phenylenediamine
4-Chloro- 1 ,2-phenylenediamine
Coumaphos
p-Cresidine
Crotoxyphos
Cupferron
Cycloheximide
2-Cyclohexyl-4.6-dinitrophenol
Cyclophosphamide
Demeton
Dial/ate
2,4-Diaminoanisole sulfate
2.4-Diaminotoluene
Diazinon
1, 2:7,8 -Dibenzacridine
1, 2:4,5 -Dibenzopyrene
Dichlone
2,6-Dichlorophenol
Dichlorovos
Dicrotophos
Diethylstilbestrol
Diethyl sulfate
Dihydrosafrole
Dimethoate
3.3'-Dimethoxybenzidine
1 , 4 -Dimethylaminoazobenzene
7, 1 2-Dimethylbenzfa)anthracene
3, 3 '-Dimeth ylbenzidine
1, 1 -Dimethylhydrazine
1 ,2-Dimethylhydrazine
aa-Dimethylphenethylamine
1 . 2 -Dinitrobenzene
1 ,3-Dinitrobenzene
1,4-Dinitrobenzene
Dinocap
8
8
8
a
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
a
8
8
8
8
8
8
8
8
8
8
8
M
M
M
M
M
M
M
M
M
M
M
M
M
mjj
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
98-86-2
53-96-3
591-08-2
79-06-1
116-06-3
117-79-3
60-09-3
92-67-1
132-32-1
61-82-5
101-05-3
62-53-3
90-04-0
140-57-8
492-80-8
86-50-0
101-27-9
17804-35-2
106-51-4
1689-84-5
OK~7 C~7 "3
JO/-O/-3
2425-06-1
133-06-2
CO OK O
OO-2D-Z
1563-66-2
786-19-6
470-90-6
106-47-8
510-15-6
95-79-4
6959-48-4
5131-60-2
95-83-0
56-72-4
120-71-8
7700-17-6
135-20-6
66-81-9
131-89-5
50-18-0
8065-48-3
2303-16-4
39156-41-7
95-80-7
333-41-5
224-42-0
192-65-4
117-80-6
87-65-0
62-73-7
141-66-2
56-53-1
64-67-5
56312-13-1
60-51-5
1 19-90-4
60-11-7
57-97-6
119-93-7
57-14-7
540-73-8
122-09-8
99-65-0
528-29-0
100-25-4
39300-45-3
U004
U005
P002
U264
U257
U274
U253
U011
U333
U260
U326
U014
P151
U280
U271
U197
U272
nf\i O
PO18
U285
U266
1 IO7Q
uz/y
U127
U148
P143
U038
U329
U319
U305
U306
P130
U262
U238
U290
P134
P034
U058
P155
U062
U307
U327
U313
U299
P144
P146
U086
U325
U090
U091
U093
U094
U095
U098
U099
P046
U284
Status
Code(b)
S
S
LR
ND
ND
S
S
S
ES
ND
S
ES
S
S
ND
S
LR
ND
S
S
A/n
Nu
S
S
S
S
S
S
S
S
S
ES
ES
S
S
S
ND
ND
LR
ND
S
S
ND
S
ES
S
S
S
S
S
S
S
LR
ND
S
LR
S
S
S
ND
ND
S
S
S
S
S
-------�
• For 33 non-detected analytes, HPLC Table 4. (continued)
(including ion chromatography or 67 Dinoseb
post-column derivatization) should 68 Dioxathion
be investigated. 69 5.5-Diphenylhydantoin
• No recommendations can be made 70 1 ,2-Diphenylhydrazine
at this time for 7 analytes not de- 71 Disulfoton
tected in this study. 72 EPN
73 Ethion
74 Ethyl carbamate
75 Ethylenimine
76 Ethylene thiourea
77 Ethyl methanesulfonate
78 Famphur
79 Fensulfothion
80 Fenthion
81 Fluchloralin
82 2-Fluoroacetamide
83 Hexachlorophene
84 Hexachloropropene
85 Hexamethyl phosphoramide
86 Hydroquinone
87 Isodrin
88 Isonicotinic acid hydrazide
89 Isosafrole
90 Kepone
91 Leptophos
92 Malathion
93 Maleic anhydride
94 Maleic hydrazide
95 Mestranol
96 Methapyrilene
97 Methomyl
98 p,p'-Methoxychlor
99 2-Methylaziridine
100 3-Methylcholanthrene
101 4.4 '-Methylenebisf2-chloroaniline)
102 4,4'-Methylenebis(N,N-dimethylaniline)
103 Methylhydrazine
104 Methyl methanesulfonate
105 N-Methyl-N-nitro-N-nitrosoguanidine
106 Methyl parathion
107 2-Methylphenol
108 3-Methylphenol
109 4-Methylphenol
1 10 Methylthiouracil
1 1 1 Mevinphos
1 12 Mexacarbate
1 13 Mir ex
114 Monocrotophos
1 15 Naled
116 1 ,5-Naphthalenediamine
117 1 ,4-Naphthoquinone
118 1 -Naphthylamine
1 19 2-Naphthylamine
120 1 -Naphthyl-2-thiourea
121 Niclosamide
122 Nicotine
123 5-Nitroacenaphthene
124 4-Nitroaniline
125 5-Nitro-o-anisidine
126 4-Nitrobiphenyl
127 Nitrofen
128 Nitrogen mustard
129 Nitroglycerine
130 5-Nitro-o-toluidine
131 4-Nitroquinoline-l-oxide
132 N-Nitrosodibutylamine
133 N-Nitrosodiethanolamine
134 N-Nitrosodiethylamine
135 p-Nitrosodiphenylamine
8
a
a
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
a
8
8
8
8
8
8
8
8
8
8
8
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
88-85-7
78-34-2
57-41-0
122-66-7
298-04-4
2104-64-5
563-12-2
51-79-6
151-56-4
96-45-7
62-50-0
52-85-7
115-90-2
55-38-9
33245-39-5
640-19-7
70-30-4
1888-71-7
680-31-9
123-31-9
465-73-6
54-85-3
120-58-1
143-50-0
21609-90-5
121-75-5
108-31-6
123-33-1
72-33-3
91-80-5
16752-77-5
72-43-5
75-55-8
56-49-5
101-14-4
101-61-1
60-34-4
70-25-7
298-00-0
95-48-7
108-39-4
106-44-5
56-04-2
7786-34-7
315-18-4
2385-85-5
6923-22-4
300-76-5
2243-62-1
130-15-4
134-32-7
91-59-8
86-88-4
50-65-7
54-11-5
602-87-9
100-01-6
99-59-2
92-93-3
1836-75-5
51-75-2
55-63-0
99-55-8
56-57-5
924-16-3
1116-54-7
55-18-5
156-10-5
P153
U109
P141
P154
U238
P054
U119
P097
P156
U330
P057
U132
U243
U312
P060
U141
P140
U324
U147
U301
U155
P066
P067
U157
U158
U255
P068
U163
U164
P131
P128
U297
P147
U309
U298
U166
U167
U168
P072
U321
P075
U250
U263
U275
U288
P132
P081
U181
U173
U287
S
S
S
ND
S
S
S
S
ND
ND
S
S
S
S
S
ND
S
S
S
S
S
ND
S
S
S
S
S
ND
S
S
ND
S
ND
S
LK
£S
ND
S
ND
S
S
S
S
ND
S
S
S
S
S
ND
S
S
ES
ND
ND
S
S
S
S
S
S
ND
ND
S
S
S
ND
S
ES
-------�
Table 4. (continued)
136
137
138
139
140
141
142
143
144
145
146
147
148
149
150
151
152
153
154
155
156
157
158
159
160
161
162
163
164
165
166
167
168
169
170
171
172
173
174
175
176
177
178
179
180
181
182
183
184
185
186
187
188
189
190
191
192
193
N-Nitroso-N-ethylurea
N-Nitrosomethylethylamine
N-Nitroso-N-methylurea
N-Nitroso-N-methylurethane
N-Nitrosomorpholine
N-Nitrosoplperidine
N-Nitrosopyrrolidine
Octamethylpyrophosphoramide
Oxydemeton-methyl
4,4'-Oxydianiline
Parathion ethyl
Pentachlorobenzene
Pentachloronitrobenzene
Phenacetin
Phenazopyridine hydrochloride
Phenobarbital
1 ,2-Phenylenediamine
1 ,3-Phenylenediamine
1 ,4-Phenylenediamine
N-Phenylthiourea
Phorate
Phosalone
Phosmet
Phosphamidon
Phthalic anhydride
Piperonyl suit 'oxide
Pronamide
1,3-Propane sultone
Propylthiouracil
Resorcinol
Rotenone
Saccharin
Safrole
Strychnine
Sulfallate
Terbufos
1,2.4,5- Tetrachlorobenzene
2, 3,4,6- Tetrachlorophenol
Tetrachlorvinphos
Tetraethyl dithiopyrophosphate
Tetraethyl pyrophosphate
Tetranitromethane
Thioacetamide
Thiofanox
Thionazine
Thiophenol
Toluene diisocyanate
o-Toluidine
Trichlorform
2,4,5- Trichlorophenol
0,0,0- Triethyl phosphorothioate
Trifluralin
2,4,5- Trimethylaniline
Trimethyl phosphate
1,3,5- Trinitrobenzene
Tris(2, 3 -dibromopropyl) phosphate
Tri-p-tolyl phosphate(c)
Warfarin
8
8
8
8
8
8
8
8
8
8
8
a
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
8
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
M
759-73-9
10595-95-6
684-93-5
615-53-2
59-89-2
100-75-4
930-55-2
152-16-9
301-12-2
101-80-4
56-38-2
608-93-5
82-68-8
62-44-2
136-40-3
50-06-6
95-54-5
108-45-2
106-50-3
103-85-5
298-02-2
2310-17-0
732-11-6
13171-21-6
85-44-9
120-62-7
23950-58-5
1120-71-4
51-52-5
108-46-3
83-79-4
81-07-2
94-59-7
57-24-9
95-06-7
13071-79-9
95-94-3
58-90-2
961-11-5
3689-24-5
107-49-3
509-14-8
62-55-5
39196-18-4
297-97-2
108-98-5
584-84-9
95-53-4
52-68-6
95-95-4
126-68-1
1582-09-8
137-17-7
512-56-1
99-35-4
126-72-7
78-32-0
81-81-2
U176
U177
U178
U176
P085
P157
U303
U187
U320
U268
P093
P145
U19Q
U270
U193
U334
U273
U202
U203
U277
P149
U308
P109
P1 12
U128
P04S
P040
P104
U223
U328
P139
U332
U259
U310
U234
U235
P001
ND
S
ND
ND
ES
S
S
LR
ND
S
S
S
S
S
ND
S
ND
ND
S
ND
S
S
S
S
S
S
S
ND
LR
S
ND
ND
S
S
S
S
S
S
S
ES
S
ND
S
ND
S
S
S
S
ND
S
ES
S
S
S
S
LR
S
ND
(a) 8 = Appendix VIII; M = Michigan list.
(b) S - apparently suitable for GC-MS analysis
LR - low response; response factor, versus phenanthrene-D10, less than 0.02
ND - not detected
ES - expected to be suitable for GC-MS analysis but not detected in this study.
fc) Substituted for the non-specific mixture, tricresyl phosphate.
-------�
S. V. Lucas and R. A. Kornfeld are with Battelle Columbus Laboratories.
Columbus, OH 43201-2693.
J. E. Longbottom is the EPA Project Officer (see below).
The complete report, entitled "GC-MS Suitability Testing of RCRA Appendix
VIII and Michigan L ist A nalytes," (Order No. PB 87'-227674 /A S; Cost: $ 13.95.
subject to change) will be available only from:
National Technical Information Service
5285 Port Royal Road
Springfield. VA 22161
Telephone: 703-487-4650
The EPA Officer can be contacted at:
Environmental Monitoring and Support Laboratory
U.S. Environmental Protection Agency
Cincinnati. OH 45268
-------�
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