Hostname: page-component-cd9895bd7-q99xh Total loading time: 0 Render date: 2024-12-28T20:39:21.154Z Has data issue: false hasContentIssue false

Letter to the Editor: Exposure to nitrous oxide and intrusive memory formation in psychological trauma

Published online by Cambridge University Press:  17 July 2017

K. Fluegge*
Affiliation:
Institute of Health and Environmental Research, Cleveland, OH, USA
*
*Address for correspondence: K. Fluegge, Institute of Health and Environmental Research, Cleveland, Ohio 44118, USA. (Email: [email protected])
Rights & Permissions [Opens in a new window]

Abstract

Type
Correspondence
Copyright
Copyright © Cambridge University Press 2017 

Das et al. (Reference Das, Tamman, Nikolova, Freeman, Bisby, Lazzarino and Kamboj2016) conducted a study to assess the effect of nitrous oxide (N2O) on intrusions following a traumatic event. The researchers invited 50 adult participants to watch two graphic movie scenes, followed by a 30-min exposure of either 50% gas mixture of N2O in oxygen or medical air. Participants kept a daily record of intrusive memories for a week following the traumatic exposure. The authors noted that the incidence of intrusions decreased by as much as 50% the day after viewing in the N2O group. However, in participants experiencing dissociation following the traumatic event, N2O exposure produced an increased intrusion frequency. These results led the authors to conclude that N2O may speed the decline in intrusive memory frequency following a traumatic event, presumably through its inhibitory action on central glutamatergic signaling. Though, the reverse may be true in dissociated individuals, and this finding was underemphasized by the authors, as indicated by the study's title, and the subsequent media reports commenting on the study. This concern is underscored by previous paradoxical findings on the link between subanalgesic N2O exposure and human memory.

Ramsay et al. (Reference Ramsay, Leonesio, Whitney, Jones, Samson and Weinstein1992) reported that subjects breathing N2O required a greater number of acquisition trials to reach a learning criterion (i.e., number–noun pairs). Though N2O exposure during acquisition of material decreased accessibility of the information, the ability to recall the material 2 weeks later improved compared with placebo. Importantly, correlational analyses suggested that this enhanced N2O-mediated delayed recall did not appear to be dependent on the increased number of trials during acquisition in the N2O-exposed group. Taken together, these findings suggest that N2O exposure during acquisition or in already dissociated individuals may affect enhanced delayed recall.

In addition to the links between N2O exposure and memory, we have proposed through repeated epidemiological investigations and review that exposure to trace levels of environmental emissions of N2O, which, in addition to its clinical usefulness, also acts as a pervasive agricultural and combustion air pollutant, may precipitate neurodevelopmental impairment in vulnerable populations. Our epidemiological investigations to date have associated the use of nitrogen fertilizers in agriculture – as the most concentrated source of environmental N2O emissions – with hospitalization for attention-deficit hyperactivity disorder (ADHD), representing a severely impaired phenotype (Fluegge, Reference Fluegge2016a ; Fluegge & Fluegge, Reference Fluegge and Fluegge2017). Our review of this novel hypothesis discussed the known physiological mechanisms of low-dose N2O exposure from both in vitro and in vivo models, including disruption of the cholinergic system (Suzuki et al. Reference Suzuki, Ueta, Sugimoto, Uchida and Mashimo2003), endogenous release of dynorphin, and activation of the kappa opioid receptor (KOR) (Branda et al. Reference Branda, Ramza, Cahill, Tseng and Quock2000) as well as activation, at subanalgesic levels, of the corticotropin-releasing factor and brainstem noradrenergic nuclei (Zhang et al. Reference Zhang, Davies, Guo and Maze1999; Sawamura et al. Reference Sawamura, Obara, Takeda, Maze and Hanaoka2003). Moreover, we cited preclinical animal studies and clinical evidence in human subjects demonstrating significant cognitive impairment and alterations in neurotransmission from trace levels of exposure to N2O (Fluegge, Reference Fluegge2016a ). Additionally, chronic recreational N2O may lead to psychiatric symptoms, including dissociation (van Amsterdam et al. Reference van Amsterdam, Nabben and van den Brink2015). These specific physiological targets may directly affect attention-related neural networking as well as neural correlates of trauma-related psychopathology (Fluegge, Reference Fluegge2016b ).

Pietrzak et al. (Reference Pietrzak, Naganawa, Huang, Corsi-Travali, Zheng, Stein, Henry, Lim, Ropchan, Lin, Carson and Neumeister2014) conducted a novel brain-imaging study wherein they have linked the brain KOR to a constellation of symptoms among trauma victims. The authors administered a radioactive tracer to the KOR to all participants and compared the PET brain scans of healthy volunteers v. those clinically diagnosed with severe trauma-related psychopathology, including PTSD. Results indicated a negative correlation between KOR availability in the amygdala–anterior cingulate cortex–ventral striatal neural circuit and symptoms of loss (i.e., dysphoria), indicating that dynorphinergic excess may desensitize brain KOR, contributing to more intense dysphoric symptoms among prior trauma victims. Animal studies show that pharmacological KOR blockade administered before extinction sessions – and not before or after the conditioning – did not led to a decrease in freezing behavior in extinction sessions (Bilkei-Gorzo et al. Reference Bilkei-Gorzo, Erk, Schürmann, Mauer, Michel, Boecker, Scheef, Walter and Zimmer2012), confirming that excess dynorphinergic-mediated KOR desensitization or blockade may contribute to trauma-related psychopathology.

Chronic, intermittent exposure (i.e., 6 h/day, 5 days a week for 2 weeks) to trace levels of N2O pollution (i.e., as low as 50 ppm, 0.005%) decreased dopamine levels in the corpus striatum of CD-1 mice (p < 0.05) (Abdul-Kareem et al. Reference Abdul-Kareem, Sharma and Drown1991). The depression in dopamine levels may be associated with compensatory increases in striatal dynorphinergic activity (Steiner & Gerfen, Reference Steiner and Gerfen1998), given the role that dynorphin opioid peptides play in N2O-mediated antinociception especially at low doses before higher order anesthetic mechanisms are induced (Branda et al. Reference Branda, Ramza, Cahill, Tseng and Quock2000). Collectively, these studies support the hypothesis that exposure to N2O may affect memory formation in a time and exposure-dependent manner. Importantly, though, the extent of direct modulation of opioidergic signaling (i.e., KOR desensitization) after the traumatic event due to trace environmental N2O-mediated dynorphinergic reactivity may not only enhance delayed recall among prior trauma victims, but also facilitate co-morbid psychiatric conditions, like ADHD (Spencer et al. Reference Spencer, Faraone, Bogucki, Pope, Uchida, Milad, Spencer, Woodworth and Biederman2016; Fluegge, Reference Fluegge2016b), as our prior epidemiological investigations have discussed.

Acknowledgements

The author has indicated no financial relationships relevant to this article to disclose.

Declaration of Interest

The author reports no conflict of interest relevant to this article to disclose.

Ethical Approval

This paper does not contain any studies with human participants or animals performed by the author.

References

Abdul-Kareem, HS, Sharma, RP, Drown, DB (1991). Effects of repeated intermittent exposures to nitrous oxide on central neurotransmitters and hepatic methionine synthetase activity in CD-1 mice. Toxicology and Industrial Health 7, 97108.Google Scholar
Bilkei-Gorzo, A, Erk, S, Schürmann, B, Mauer, D, Michel, K, Boecker, H, Scheef, L, Walter, H, Zimmer, A (2012). Dynorphins regulate fear memory: from mice to men. Journal of Neuroscience 32, 93359343. doi: 10.1523/JNEUROSCI.1034-12.2012.Google Scholar
Branda, EM, Ramza, JT, Cahill, FJ, Tseng, LF, Quock, RM (2000). Role of brain dynorphin in nitrous oxide antinociception in mice. Pharmacology, Biochemistry, and Behavior 65, 217221.CrossRefGoogle ScholarPubMed
Das, RK, Tamman, A, Nikolova, V, Freeman, TP, Bisby, JA, Lazzarino, AI, Kamboj, SK (2016). Nitrous oxide speeds the reduction of distressing intrusive memories in an experimental model of psychological trauma. Psychological Medicine 46, 17491759. doi: 10.1017/S003329171600026X.Google Scholar
Fluegge, K (2016a). Does environmental exposure to the greenhouse gas, N2O, contribute to etiological factors in neurodevelopmental disorders? A mini-review of the evidence. Environmental Toxicology and Pharmacology 47, 618. doi: 10.1016/j.etap.2016.08.013.Google Scholar
Fluegge, K (2016b). The association between PTSD and ADHD: does the association reveal a PTSD-somatoform subtype? A reply to Spencer et al. (2015). Journal of Clinical Psychiatry 77, e1149. doi: 10.4088/JCP.16lr10630.Google Scholar
Fluegge, K, Fluegge, K (2017). Exposure to ambient PM10 and nitrogen dioxide and ADHD risk: a reply to Min & Min (2017). Environment International 103, 109110. doi: 10.1016/j.envint.2017.02.012.Google Scholar
Pietrzak, RH, Naganawa, M, Huang, Y, Corsi-Travali, S, Zheng, MQ, Stein, MB, Henry, S, Lim, K, Ropchan, J, Lin, SF, Carson, RE, Neumeister, A (2014). Association of in vivo κ-opioid receptor availability and the transdiagnostic dimensional expression of trauma-related psychopathology. JAMA Psychiatry 71, 12621270. doi: 10.1001/jamapsychiatry.2014.1221.Google Scholar
Ramsay, DS, Leonesio, RJ, Whitney, CW, Jones, BC, Samson, HH, Weinstein, P (1992). Paradoxical effects of nitrous oxide on human memory. Psychopharmacology (Berl) 106, 370374.Google Scholar
Sawamura, S, Obara, M, Takeda, K, Maze, M, Hanaoka, K (2003). Corticotropin-releasing factor mediates the antinociceptive action of nitrous oxide in rats. Anesthesiology 99, 708715.CrossRefGoogle ScholarPubMed
Spencer, AE, Faraone, SV, Bogucki, OE, Pope, AL, Uchida, M, Milad, MR, Spencer, TJ, Woodworth, KY, Biederman, J (2016). Examining the association between posttraumatic stress disorder and attention-deficit/hyperactivity disorder: a systematic review and meta-analysis. Journal of Clinical Psychiatry 77, 7283. doi: 10.4088/JCP.14r09479.Google Scholar
Steiner, H, Gerfen, CR (1998). Role of dynorphin and enkephalin in the regulation of striatal output pathways and behavior. Experimental Brain Research 123, 6076.CrossRefGoogle ScholarPubMed
Suzuki, T, Ueta, K, Sugimoto, M, Uchida, I, Mashimo, T (2003). Nitrous oxide and xenon inhibit the human (alpha 7)5 nicotinic acetylcholine receptor expressed in Xenopus oocyte. Anesthesia and Analgesia 96, 443448.Google Scholar
van Amsterdam, J, Nabben, T, van den Brink, W (2015). Recreational nitrous oxide use: prevalence and risks. Regulatory Toxicology and Pharmacology 73, 790796. doi: 10.1016/j.yrtph.2015.10.017.CrossRefGoogle ScholarPubMed
Zhang, C, Davies, MF, Guo, TZ, Maze, M (1999). The analgesic action of nitrous oxide is dependent on the release of norepinephrine in the dorsal horn of the spinal cord. Anesthesiology 91, 14011407.Google Scholar