Analysis of 62 synthetic cannabinoids by gas chromatography-mass spectrometry with photoionization.

Gas chromatography-mass spectrometry (GC-MS) in electron ionization (EI) mode is one of the most commonly used techniques for analysis of synthetic cannabinoids, because the GC-EI-MS spectra contain characteristic fragment ions for identification of a compound; however, the information on its molecular ions is frequently lacking. To obtain such molecular ion information, GC-MS in chemical ionization (CI) mode is frequently used. However, GC-CI-MS requires a relatively tedious process using reagent gas such as methane or isobutane. In this study, we show that GC-MS in photoionization (PI) mode provided molecular ions in all spectra of 62 synthetic cannabinoids, and 35 of the 62 compounds showed only the molecular radical cations. Except for the 35 compounds, the PI spectra showed very simple patterns with the molecular peak plus only a few fragment peak(s). An advantage is that the ion source for GC-PI-MS can easily be used for GC-EI-MS as well. Therefore, GC-EI/PI-MS will be a useful tool for the identification of synthetic cannabinoids contained in a dubious product. To the best of our knowledge, this is the first report to use GC-PI-MS for analysis of synthetic cannabinoids.

Introduction

In recent years, the harmful effects on human health from new psychoactive substances (NPSs), including synthetic cannabinoids, have become a serious social problem worldwide. Although almost all head shops selling the NPSs have been closed due to stringent control by the Ministry of Health, Labour and Welfare, as well as other organizations in Japan, such shops are still active in other countries. In addition, online sales activities continue at a rapid pace. The fastest and simplest method for identification of these NPSs is to record the electron ionization (EI) mass spectrum of a compound in question by gas chromatography–mass spectrometry (GC–MS) at 70 eV and to conduct a data search using the SWGDRUG Mass Spectral Library, for example, or Cayman Chemical Compounds Database. These databases are largely limited to EI mass spectra at 70 eV obtained by GC–MS, because of their excellent reproducibility. The only drawback of the EI mass spectra is that molecular or pseudo-molecular peaks are frequently very small or missing. For designer drugs including synthetic cannabinoids, there are many compounds showing very similar patterns of fragment peaks. In such cases, the appearance of a distinct molecular peak will be very useful for differentiating compounds with similar structures except for regioisomers.

The photoionization (PI) technique for MS is not new, having been developed about 60 years ago by Lossing and Tanaka [1]. After their discovery, PI received very little attention from the scientific community. However, in 2010, interest in PI was reignited with the description of the attachment of PI detection to “microfabricated planar glass GC”; the detection limit of mono-aromatics was sub-ng on columns [2]. A similar connection of PI to a portable GC system reported in 2013 showed a low detection limit less than 5 ppb for volatile organic compounds such as benzene, toluene, and styrene [3]. During our literature search on PI, we were surprised to find as many as seven articles on applications of PI published in international scientific journals in 2015–2016 [4-10]. Among these reports, various combinations of PI with atmospheric pressure MS [6, 7, 9] and with low-pressure MS [4, 10] were reported to provide extremely high sensitivity. It appears that PI technology is now under rapid development.

In the current study, we present GC–PI-MS spectra of as many as 62 kinds of synthetic cannabinoids, compared with those of GC–EI-MS spectra for the first time.

Materials and methods

Chemicals and their preparation

Sixty-two synthetic cannabinoids (for structures, see Fig. 1) were purchased from Cayman Chemical (Ann Arbor, MI, USA), and analytical-grade methanol and acetonitrile were obtained from Kanto Chemical (Tokyo, Japan). All but five synthetic cannabinoids were dissolved in methanol at a concentration of 100 μg/mL, to be used for mass spectra measurements; the exceptions were the five carboxylate compounds (FDU-PB-22, 5-fluoro-SDB-005, 5- fluoro-NPB-22, BB-22 and PB-22), each of which was dissolved in acetonitrile to give the same concentration in order to avoid thermal hydrolytic degradation in the presence of methanol [11].

Fig. 1

Sixty-two synthetic cannabinoids classified into 13 types on the basis of structure. Compounds subjected to gas chromatography–mass spectrometry (GC–MS) in electron ionization (EI) mode (20 compounds in total) are shown by double underlines

GC–MS conditions

GC–MS analysis was conducted using an Agilent 7890B gas chromatograph (Agilent Technologies, Santa Clara, CA, USA) connected to a JEOL JMS-Q1050 mass spectrometer with an EI/PI combination ion source (JEOL, Akishima, Japan) (Fig. 2). GC–PI-MS conditions were as follows: separation column, DB-5MS fused-silica capillary (30 m × 0.25 mm i.d., 0.25 μm film thickness; Agilent Technologies); injector temperature, 230 °C; interface temperature, 150 °C; injection mode, splitless; injection volume, 2 μL; helium carrier gas flow rate, 1.0 mL/min; oven temperature program, initial temperature at 60 °C (1-min hold) followed by ramping at 10 °C/min to 150 °C (3-min hold) and then ramping at 10 °C/min to 300 °C (22-min hold); MS ionization mode, PI; wavelength range of vacuum ultraviolet (VUV) beam for PI by a deuterium lamp, 115–400 nm; transparent window between the VUV lamp and ion source, MgF2; PI energy, 10.3 eV; ion source temperature, 150 °C; identification, scan mode; scan range, m/z 10–600. GC–EI-MS conditions were as follows: separation column, carrier gas flow rate, and oven temperature program, the same as those for GC–PI-MS; injector temperature, 250 °C; interface temperature, 200 °C; injection mode, split at 1:20; injection volume, 1 μL; electron energy, 70 eV; ion source temperature, 200 °C; identification, scan mode; scan range, m/z 40–500.

Fig. 2

Schematic illustration of the EI and photoionization (PI)/EI combination source. a EI ion source: irradiation by thermal electrons generated from the filament to the sample. b PI/EI combination source: irradiation by vacuum ultraviolet (VUV) light from the ultraviolet lamp to the sample. It was possible to continuously obtain fragment ion information by EI and molecular ion information by PI

Results and discussion

Mass spectra obtained by GC–PI-MS

As an initial step in the GC–PI-MS methodology, it is very important to know the likelihood of molecular ion production for each target compound, depending on the ionization potential and the detector photon energy. In this work, we used 10.3 eV of photoionization energy that is used for general applications [12]. It is of great interest to obtain the mode of ionization for each synthetic cannabinoid. The 62 synthetic cannabinoids dealt with in this study encompassed almost every type of compounds. The GC–PI-MS protocol used here allowed us to observe the molecular ions for all 62 synthetic cannabinoids. The compounds used in this work can be categorized into three groups.

Group 1 comprises 35 compounds that generated only single molecular ions, including naphthoylindoles (19 compounds), carboxamide derivatives (5 compounds), benzoylindoles (5 compounds), naphthoylindazoles (2 compounds), naphthoylpyrroles (2 compounds), a naphthoylbenzimidazole (1 compound), and a naphthoylnaphthalene (1 compound) (Table 1).

Table 1

Grouping of the 13 types of synthetic cannabinoids according to mass spectra by gas chromatography–mass spectrometry in photoionization mode

Group 1 Molecular ion only (35 compounds)

①Naphthoylindoles (19 compounds)

AM2232, EAM-2201, JWH-007, JWH-015, JWH-016, JWH-019, JWH-020, JWH-022, JWH-072, JWH-080, JWH-081, JWH-098, JWH-149, JWH-182, JWH-210, JWH-213, JWH-398, JWH-412, AM1220 azepan isomer

②Carboxamide derivatives (5 compounds)

SDB-006, APICA, APICA JV-(5-fluoropentyl) derivative, MN-18, 5-fluoro-MN-18

③Benzoylindoles (5 compounds)

AM679, AM694, RCS-4, RCS-4 ortho isomer, AM2233 azepan isomer

⑨Naphthoylindazoles (2 compounds)

THJ-018, THJ-2201

⑩Naphthoylpyrroles (2 compounds)

JWH-307, JWH-030

⑫Naphthoylbenzimidazole (1 compound)

FUBIMINA

⑬Naphthoylnaphthalene (1 compound)

CB-13

Group 2 Molecular ion with smaller fragment ion(s) (18 compounds)

②Carboxamide derivatives (5 compounds)

APINACA, APINACA JV-(5-fluoropentyl) derivative, NNE1, 5-fluoro-NNEl, ADBICA

④Cyclopropyls (4 compounds)

A-836339, FUB-144, UR-144, XLR-12

⑦Quinolinyl carboxylates (3 compounds)

BB-22, PB-22, 5-fluoro-NPB-22

⑤Phenylacetylindoles (2 compounds)

JWH-250, JWH-251

⑥Carboxyindoles (2 compounds)

MEPIRAPIM, AB-001

⑧Naphthoyl carboxylate (1 compound)

5-Fluoro-SDB-005

⑪Cyclohexylphenol (1 compound)

CP-47,497

Group 3 Smaller molecular ions with a fragment ion as base peak (9 compounds)

②Carboxamide derivatives (3 compounds)

AB-CHMINACA, AB-FUBINACA, AB-PINACA

⑤Phenylacetylindoles (2 compounds)

JWH-203, cannabipiperidiethanone

①Naphthoylindole (1 compound)

AM1220

③Benzoylindole (1 compound)

AM2233

⑥Carboxyindole (1 compound)

AM1248

⑧Naphthoyl carboxylate (1 compound)

FDU-PB-22

Group 2 compounds generated molecular ions as the base peak as well as smaller fragment ion(s): carboxamide derivatives (5 compounds), cyclopropyls (4 compounds), quinolinyl carboxylates (3 compounds), phenylacetylindoles (2 compounds), carboxyindoles (2 compounds), a naphthoyl carboxylate (1 compound), and a cyclohexylphenol (1 compound).

Group 3 compounds generated a small molecular ion and a fragment ion as a base peak: carboxamide derivatives (3 compounds), phenylacetylindoles (2 compounds), a naphthoylindole (1 compound), a benzoylindole (1 compound), a carboxyindole (1 compound), and a naphthoyl carboxylate (1 compound) (Table 1).

The PI technique is unique in that the radical cation is produced by ultraviolet light radiation by depriving one electron from a target molecule with a low ionization threshold [6], while EI requires the deprivation of two electrons at a time for ion formation with relatively high ionization threshold. Therefore, the PI technique has been used as a convenient method for detecting stable neutral compounds such as volatile organic compounds or neutral oil components [2, 3, 6, 7, 9].

In the present study, which dealt with 62 synthetic cannabinoids, all compounds were able to be detected by GC–PI-MS. Furthermore, as many as 35 compounds showed only the molecular ions in their mass spectra, without the appearance of any fragment peaks, as described above. The compounds with fewer functional groups tended to show single molecular peaks in their mass spectra, such as the group of naphthoylindoles (19 compounds) (Table 1).

Figure 3 shows examples of mass spectra in the PI and EI modes for eight selected synthetic cannabinoids. While there were various types of mass spectra observed in the PI mode, all spectra showed peaks of molecular ions. In contrast, in the EI mode, the molecular/quasi-molecular peaks were not detected in two of the eight spectra (Fig. 3b, g). When fragment peak(s) appeared in a PI spectrum, the same fragment peak(s) also appeared in the corresponding EI spectrum (Fig. 3b, c, g).

Fig. 3

Examples of mass spectra for synthetic cannabinoids obtained by GC–MS in PI and EI modes and their probable fragmentation pathways

In the EI mode, 70 eV of ionization energy is typically used, because the high energy provides the most stable and reproducible results. Such a phenomenon is also the case for the PI mode; ionization energy of 10.0–10.6 eV is typically used for general applications [1, 12]. In the present study, 70 eV EI and 10.3 eV PI were used. Except for the ease in producing the molecular radical cations, the fragmentation modes in the EI and PI modes seem essentially similar, as exemplified with AB-CHMINACA, XLR-12, and AM1220 (Fig. 3b, c, g). As shown in the PI mode (Table 1), many synthetic cannabinoids showed a molecular radical cation together with a fragment ion (Fig. 3b, d, e–g), but only a few PI spectra showed more than one fragment peak (Fig. 3c). This means that most of the free electrons that played a role in creating a fragment ion became extinct at this stage. In the EI mode, the multiple free electrons generated have no capability of producing a molecular radical cation, but act to produce various types of fragment ions via the cleavage of bonds in α- and/or β- position against a heteroatom. It seems correct that fragmentation is nearly the same between the PI and EI modes at the early stage (Fig. 4), except for the unique capacity of the PI to produce molecular radical cations with a low threshold.

Fig. 4

Proposed mechanism of cleavage to form fragment ions in three synthetic cannabinoids measured by PI and EI. Further fragmentation occurred after cleavage of the α-bond in AB-CHMINACA and XLR-12 subjected to GC–EI-MS. No further fragmentation occurred in these compounds by GC–PI-MS

Here, we must mention GC–MS in chemical ionization (CI) mode. This technique is used to estimate the molecular weight of a target compound, and actually gives an intense peak due to [M + H]+, but sometimes gives an adduct ion produced by molecular binding with a reagent gas or its fragment, which makes the interpretation complicated. In addition, GC–CI-MS requires a reagent gas such as methane or isobutane, various conditions of which should be optimized beforehand; such a procedure is tedious (e.g., reagent gas selection, flow rate adjustment). Although it is possible for GC–CI-MS to share the same ionization chamber with GC–EI-MS, it is now common to use different GC–EI-MS and GC–CI-MS systems in order to use them under their optimal analytical conditions. In this respect, the PI device can be attached to most GC–EI-MS instruments under optimal conditions to share the same ionization chamber for both EI and PI modes. In our opinion, attaching the PI system to the EI chamber is the best option, because of the absence of adduct formation and low cost of installation. The PI technique appears to be superior to the CI mode for obtaining information on the molecular weight of a target compound.

Conclusions

In this study, the mass spectra of 62 synthetic cannabinoids were recorded by GC–PI-MS, and the mass spectra for 20 compounds were measured by GC–EI-MS for comparison. Most of the mass spectra obtained from the 62 synthetic cannabinoids by GC–PI-MS showed very simple patterns of either molecular ion only or a molecular ion plus only one fragment peak, providing useful information on the molecular weight of the target compound. Therefore, GC–EI/PI-MS will be a useful tool for identifying synthetic cannabinoids contained in a dubious product. The information on the ease of producing molecular radical cations by GC–PI-MS for synthetic cannabinoids will aid in the construction of a highly sensitive MS method using PI technology for analysis of a specific synthetic cannabinoid in biological samples. To our knowledge, this is the first report to use the PI technology for analysis of synthetic cannabinoids.