Glasgow Coma Scale scores, early opioids, and 4-year psychological outcomes among combat amputees
By Galarneau, Michael | |
Proquest LLC |
Abstract-Morphine and fentanyl are frequently used for analgesia after trauma, but there is debate over the advantages and disadvantages of these opioids. Among combat amputees, intravenous (IV) morphine (vs IV fentanyl) after injury was associated with reduced likelihood of posttraumatic stress disorder (PTSD). The previous results were based on military health diagnoses over 2 yr postinjury. The present study followed psychological diagnoses of patients with amputation for 4 yr using military and
Key words: combat amputee, fentanyl, Glasgow Coma Scale,
Abbreviations: CI = confidence interval; EMED = Expeditionary Medical Encounter Database; GCS = Glasgow Coma Scale; ICD-9-CM = International Classification of Diseases, 9th Revision, Clinical Modification; IRB = institutional review board; ISS = Injury Severity Score; IV = intravenous; NHRC =
INTRODUCTION
Preventing posttraumatic stress disorder (PTSD) is a priority for military healthcare providers because of its adverse effects on health and financial costs [1-9]. For patients with serious combat limb injuries, PTSD can complicate and prolong rehabilitation [8]. PTSD is asso- ciated with more sick call visits, missed workdays, increased somatic symptoms [3], poor quality of life out- comes [5], and healthcare costs over
Most patients with amputation in our previous study (Melcer et al. [10]) received either morphine or fentanyl. Providers debate which of these opioids might be most appropriate for postinjury analgesia [15-17]. Unfortu- nately, little research has compared the psychological benefits of morphine or fentanyl. Early morphine was associated with reduced likelihood of PTSD among com- bat casualties injured between 2004 and 2006, but there was little evidence of fentanyl use [18]. More recently, fentanyl has gained support as an alternative to morphine [19]. The onset of morphine-induced analgesia occurs much more slowly than fentanyl [14]. However, mor- phine produces longer-lasting pain relief than does a simi- lar dose of fentanyl. We hypothesized that morphine reduced PTSD compared with fentanyl because mor- phine produced more long-lasting pain relief and/or was more effective at blocking memory for trauma than fen- tanyl [10,14,18,20]. Differences between morphine and fentanyl pharmacology and Āµ receptor subtypes in the brain [21] may also contribute to differences in the effects of these drugs on memory for trauma and PTSD prevention.
The psychological outcomes in our previous study were limited to diagnoses extracted from military data- bases [10,22] through 2 yr postinjury [22-23]. Little is known about the long-term psychological outcomes for combat amputees. They typically discharge from military service within the first 2 yr postinjury [6,24-25] and may receive postinjury care from military and/or
The present study followed short- (2 yr) and long- term (4 yr) psychological outcomes using both military and VA health data. It was hypothesized that extended loss of consciousness and intravenous (IV) morphine (vs fentanyl) within hours after injury would be associated with reduced rates of short-term PTSD diagnoses. As in the previous study, we expected this association between IV morphine and PTSD and mood disorder only among patients with TBI. We also expected a general increase in PTSD rates over the long term, based on VA health data showing relatively high rates of PTSD among military- separated combat veterans [31-32].
METHODS
Data Sources
This collaborative study was approved by the institu- tional review board (IRB) at the
In-Theater Injury and Medication Data
NHRC's Expeditionary Medical Encounter Database (EMED), formerly known as the
The EMED uses clinical encounter forms to capture patient data, including time of arrival at treatment facili- ties, mechanism of injury, Injury Severity Score (ISS) (based on Abbreviated Injury Scale scores assigned by EMED clinicians) [34], and Glasgow Coma Scale (GCS) scores. The EMED encounter forms also capture detailed treatment data, including medications administered dur- ing early postinjury resuscitation and trauma care, dos- ages, and routes of administration, as available. The encounter forms are completed by healthcare providers in-theater, either on paper or electronically, and are for- warded to the EMED at NHRC.
Military Health Outcomes
Combat amputees, their associated anatomical levels of amputations (e.g., single or multiple, upper or lower limb), and subsequent psychological outcomes were identified by searching military health databases [22]. Military health data consist of inpatient and outpatient records, which include International Classification of Diseases, 9th Revision, Clinical Modification (ICD-9- CM) diagnostic codes via TRICARE Management Activ- ity. Records were merged from the Armed Forces Health Longitudinal Technology Application, based on inpatient and outpatient encounters by credentialed providers at military treatment facilities and government-reimbursed private clinics. Data were captured from
All patients in the present study first were identified in the military health databases as described. Subse- quently, VA investigators at the
Patients
We searched the military health databases to identify U.S. military personnel with major limb amputations (excluding fingers and/or toes alone) who were combat injured in the
At the onset of the
Research Design
This was a retrospective review of existing medical records of U.S. combat amputees injured from 2001 to 2008 in
The GCS scores, medication type, dosage, route of administration, and associated level of care for these data were extracted from in-theater patient encounter forms by trauma research nurses per standard EMED procedures [33]. Patients usually arrive at level 2 care 1-6 h postin- jury, while arrival at level 3 care typically occurs 2-24 h postinjury. GCS scores of 12 or less, which indicate at least moderate TBI and/or loss of consciousness greater than 30 min [37], at level 2 were used to assess the effect of injury-related alteration or loss of consciousness. Assessments of GCS may have been affected by opioid treatment or other medications. However, 12 percent of both the any morphine group and the fentanyl only group had GCS scores of 12 or less. Further, providers typically consider medication history when assessing GCS and TBI, including repeated GCS assessments to minimize the acute effects of medications on GCS or TBI.
The classifications of medications have been described previously [10]. Briefly, the medications recorded included antibiotics (e.g., cefazolin), general anesthetics (e.g., etomi- date), opioid analgesics (i.e., fentanyl or morphine), benzo- diazepines (e.g., midazolam), and paralytic and/or muscle relaxants (e.g., succinylcholine, suxamethonium, vecuronium bromide, pancuronium bromide, and/or rocuronium bromide). The U.S. military has established policies for in-theater storage and dispensing of controlled medications, which are carefully logged by physicians [38].
Preinjury psychological diagnoses were analyzed as available in military databases. Postinjury psychological diagnoses were identified in military and VA health data- bases with ICD-9-CM codes 290-319, excluding 305.10 (tobacco addiction). The primary outcome was a PTSD diagnosis (ICD-9-CM code 309.81) within 24 or 48 mo postinjury. Because previous research has shown that patients with at least two PTSD diagnoses (vs one) in health databases are more likely to have a criterion score on an independent PTSD Checklist-Military version sur- vey of 350, we included only patients documented with two or more PTSD diagnoses [39]. The remaining psycho- logical diagnoses were grouped as adjustment, anxiety, mood, substance abuse disorders, and "other" psychologi- cal diagnoses. Other psychological diagnoses included postconcussion syndrome, pain, sleep, and unspecified cognitive disorders.
Data Analysis and Study Retention
The overall study sample consisted of 258 patients with medication data recorded at level 1, 2, 3, or 4 or GCS scores available in the EMED. A subset of 145 patients had at least one level 2 medication (e.g., opioids, paralytics, or antibiotics) recorded with psychological outcomes. Of these 145 patients, 137 also had level 2 GCS scores (8 patients had missing GCS scores). The level 2 medica- tion sample consisted of 115 patients treated with any mor- phine (morphine alone or combined with fentanyl) or fentanyl alone (3 level 1 patients were included in this sub- set) and another 30 patients who received no opioids (i.e., no morphine or fentanyl). Prevalence for psychological outcomes was calculated across the first 24 mo for com- parison with previous study results [10]. Chi-square or Fisher exact test were used as appropriate to test for signifi- cant associations between medications and psychological outcomes. Logistic regressions then were conducted to model relationships between morphine (vs fentanyl) and psychological outcomes, especially PTSD, adjusting for TBI, injury year (2001-2006 vs 2007-2008), and loss of consciousness (as defined by a level 2 GCS score Ā£12).
Long-term prevalence of PTSD and other psychologi- cal disorders was also calculated for consecutive postin- jury years 1 through 4. Longitudinal random intercept models were constructed using the SAS Proc GLIMMIX procedure for Generalized Linear Mixed models (
RESULTS
Study Retention
All patients had at least 3 yr of military and/or VA outcomes data. For the level 2 medication sample (any morphine, fentanyl only, or no opioids), all 145 patients had data through 3 yr postinjury. Patients missing data for year 4 were included in analyses across years 3 and 4. For GCS analyses, 133 of 137 patients (97%) had out- comes data through 4 yr postinjury. Overall, 231 of 258 patients (88%) had military and/or VA data for all 4 yr postinjury.
Sample Characteristics
The overall study sample (N = 258) and the subsam- ple of patients with level 2 medication data (n = 145) and GCS scores (n = 137, 8 patients had missing GCS scores) had injury and demographic characteristics that were similar to those of all 857 patients with amputation injured from 2001 to 2008 (Table 1) [10]. (The EMED captured 258 of all 857 patients with amputation, primar- ily those treated at
Glasgow Coma Scale Scores and Psychological Diagnoses
Table 2 shows the prevalence of PTSD diagnoses during each of the first 4 yr after combat injury as a func- tion of GCS scores. Clinicians reviewed patient charts for evidence of medications before GCS assessments. Among patients with GCS of 12 or less, 14 of 20 individuals had no evidence of opioids or other narcotics before GCS assessment. Four patients had medication-induced uncon- sciousness (per intubation procedures) and two others received IV morphine (10 and 20 mg). During the first year, patients who sustained postinjury loss of conscious- ness (i.e., GCS Ā£12) had a trend for lower PTSD preva- lence than patients with higher GCS scores, but the finding was not statistically significant. Based on VA data sources, we also noted that PTSD prevalence increased, particularly for patients with lower GCS scores (i.e., GCS Ā£12). Our prior study found zero out of 20 patients had PTSD diagnoses in military data sources during the first 2 yr postinjury [10]. By comparison, we emphasize that the present study found seven PTSD cases for the same 20 patients when both VA and military data sources were combined. Finally, both GCS groups had similar PTSD rates during years 2 through 4.
Characteristics of Medications
The most frequently administered level 2 medications included IV antibiotics and opioid analgesics. The present study focused on opioid analgesics administered at level 2 combat trauma care facilities because these medications, given within hours of injury, have been shown to affect psychological outcomes [10,18]. Of the 145 patients in the level 2 medication group, 115 received morphine or fen- tanyl and 75 percent of these patients had dosage data. Another 30 patients received no opioids but had records of other medications. The median highest dose administered at level 2 was 10 mg for morphine and 100 Āµg for fentanyl. Because the analgesic effect of fentanyl is generally con- sidered 100 times more potent than morphine, the median dosages administered to patients in the present study were approximately equivalent for analgesic effectiveness [16].
Morphine, Fentanyl, and Psychological Diagnoses
Table 3 shows the level 2 medication sample (n = 145) comparing groups who received any morphine, fentanyl only, or no opioids; their associated ISS; and prevalence of patients with TBI, PTSD, or mood diagnoses. Preinjury psychological diagnoses, age (percentage Ā£25 yr old), and prevalence of TBI diagnoses did not differ significantly among the three groups. Across TBI status, the no opioids group had significantly higher ISSs than the any morphine or the fentanyl only (opioid-treated) groups (mean ISS: no opioids = 24.2, any morphine = 16.4, fentanyl only = 15.7; p < 0.001).
Short-Term Psychological Outcomes
During the first 2 yr postinjury, the no opioids group had significantly lower prevalence of PTSD (20%, n = 30) than the fentanyl group (53%, n = 32) (chi-square, p < 0.01), but not the morphine group (34%, n = 83). The no opioids group also had a significantly higher preva- lence of provider-documented loss of consciousness (50%, 15 of 30) than patients who received opioids (11%, 13 of 115) (p < 0.01). Providers advise that patients with severe injuries (i.e., ISS >20) are not candidates for opi- oid treatment because they are typically already uncon- scious with significant blood loss [17]. Therefore, the subsequent analyses focused on comparing patients who received opioid medications, either morphine or fentanyl.
Across TBI status, 34 percent of morphine-treated patients (n = 83) had PTSD during the first 2 yr postinjury compared with 53 percent of patients treated with fentanyl only (n = 32) (p < 0.05). Any morphine (vs fentanyl only) was significantly associated with a reduced prevalence of PTSD during years 1 and 2 (odds ratio [OR] = 0.37, 95% confidence interval [CI] = 0.15-0.90), adjusted for age, injury year, and log ISS. Table 3 also shows the morphine/ fentanyl association with PTSD by TBI status. Among patients with a TBI diagnosis, any morphine (vs fentanyl) had reduced odds of PTSD during years 1 and 2 (OR = 0.23, 95% CI = 0.07-0.82), adjusted for age, injury year, and log ISS. A similar analysis for patients with amputation without a TBI diagnosis did not show a significant associa- tion between morphine and PTSD. We conducted separate analyses for psychological diagnoses during the third and fourth years postinjury and found no statistically significant association between the early treatment of patients with IV morphine (vs IV fentanyl) and subsequent development of PTSD or mood diagnoses, regardless of TBI status.
Longitudinal Analyses: Traumatic Brain Injury, Morphine, Fentanyl, and 4-Year Outcomes
Longitudinal models of PTSD outcomes over 4 yr postinjury included opioid treatment (any morphine vs fentanyl); TBI; and additional covariates, namely preinjury psychological diagnosis, log ISS, and age. There were no significant 3- or 2-way interactions involving the opioid variable using either two time points (i.e., years 1 and 2 vs years 3 and 4) or four time points (i.e., years 1, 2, 3, and 4). The longitudinal analysis with four time points (Figure 1) showed a statistically significant effect of opioid treatment (morphine vs fentanyl) on PTSD over time (adjusted OR = 0.40, 95% CI = 0.17-0.94). Among patients with TBI, morphine (vs fentanyl) was associated with reduced odds of PTSD, but the trend was not statistically significant (p = 0.06, adjusted OR = 0.25, 95% CI = 0.06-1.04, p = 0.06). Models were adjusted for time trend, log ISS, and age.
Table 4 shows rates of anxiety, adjustment disorders, and substance abuse among morphine- and fentanyl- treated patients according to TBI status. There were no significant associations between morphine (vs fentanyl only) for any of these psychological outcomes during years 1 and 2 or years 3 and 4 postinjury. Among patients with a TBI diagnosis, the morphine group showed numerically lower but not statistically significant rates of psychological diagnoses, particularly for anxiety diagno- ses during the first 2 yr postinjury.
Four-year psychological outcomes. Figure 2 shows the prevalence of psychological disorders during years 1, 2, 3, and 4 postinjury. Longitudinal analyses evaluated changes in the prevalence of each disorder across 4 yr postinjury (relative to year 1). There was a significant increase in PTSD prevalence across the four years (p < 0.001). By comparison to year 1, PTSD increased signifi- cantly during years 2, 3, and 4. By contrast, the prevalence of anxiety, adjustment, and mood disorders decreased sig- nificantly across the years (all p < 0.001, see Figure 1 notes). The prevalence of substance abuse did not change significantly across years. By the fourth year postinjury, PTSD had the highest prevalence of all disorders
Military versus combined military and
DISCUSSION
The present study is one of the first to investigate the effect of early postinjury medications on long-term psychological outcomes of combat amputees, based on military and VA health data beginning near the point of injury through the following 4 yr of recovery. The major findings were (1) although patients with extended loss of consciousness had numerically lower PTSD rates during the first year postinjury, the finding was not statistically significant and no further reduction was observed during subsequent years; (2) longitudinal modeling showed significantly reduced odds of PTSD for patients treated with morphine (vs fentanyl) across the 4 yr postinjury, after adjusting for postinjury year, age, and injury severity; (3) early treatment with IV morphine (vs IV fentanyl) was significantly associated with reduced PTSD rates, primarily among patients with TBI, during the first 2 yr postinjury; and (4) the association between IV morphine and reduced rates of PTSD does not appear to extend through the third and fourth years postinjury. A related finding was that PTSD prevalence increased sub- stantially after the first year postinjury, while the preva- lence of other psychological decreased across the 4 yr.
The finding that loss of consciousness (i.e., GCS Ā£12) was not associated with reduced PTSD contrasted with findings from our previous study [10]. Both studies showed similar trends for reduced PTSD following loss of con- sciousness during the first year postinjury. However, this association in the present study was not statistically signifi- cant when additional PTSD diagnoses were included from VA health data. Notably, military physicians often refer serious head/spinal injury patients to
The present study also found that patients treated with morphine had significantly reduced odds of PTSD than those treated with fentanyl. This finding extended our pre- vious study [10] by integrating the military and VA health data and by longitudinal modeling of the association between early opioids and PTSD outcomes across 4 yr postinjury. The effect of morphine on PTSD appeared strongest during the first 2 yr postinjury among patients with TBI. A previous study found postinjury morphine was associated with reduced likelihood of PTSD, but did not appear to find substantial use of fentanyl for compari- son [18]. As in our previous study, we hypothesized that the primary effect of morphine was to prevent PTSD and, secondarily, these patients were also less likely to develop mood disorders [43-44]. There is evidence that both TBI and morphine may interfere with the formation of memory of trauma and later PTSD [18,36]. This may explain why morphine was most effective among patients with TBI.
We emphasize caution in hypothesizing a relation- ship between morphine, fentanyl, and TBI and PTSD outcomes because of small sample sizes in the present study. There may have been unmeasured patient treat- ment or injury characteristics that determined whether individuals received morphine or fentanyl. It is possible such characteristics caused the differences in PTSD out- comes observed in the present study. However, our multi- variate analyses adjusted for patient characteristics such as age and injury severity and the morphine/fentanyl variable remained a significant predictor of PTSD. Future research should consider in-depth review of individual cases and provider interviews to detail the wide range of patient characteristics that might differ between mor- phine-treated and fentanyl-treated patients. Ultimately, prospective randomized trials, which may be possible at civilian trauma centers, can provide the strongest test of the effect of early opioids on psychological outcomes.
The primary clinical implication of the present study and our previous results [10,18] is that combat care physi- cians may consider PTSD prevention as a potential benefit of choosing early IV morphine (alone or combined with IV fentanyl) versus IV fentanyl alone [17-18,20]. IV mor- phine or morphine combined with fentanyl may interfere with postinjury neurological processes required for mem- ory of combat trauma and thereby protect against later PTSD [18,45]. Alternatively, the present results might be explained by the protective effects of morphine and/or the negative effects of fentanyl on PTSD. As discussed, these opioids have differences in opioid receptor subtypes in the brain and in the duration of their analgesia [14,21], which may explain their different effects on pain, traumatic mem- ory, and PTSD. A previous randomized study showed that postinjury pain was similar between morphine- and fen- tanyl-treated patients until 40 to 60 min after surgery, and thereafter fentanyl-treated patients reported more pain [17]. In practice, one may question whether medication shortly after a specific combat injury, such as amputation, might be effective in reducing PTSD. Combatants likely experience prior stressful events during deployment (e.g., firefights, witnessing injuries). However, patients who are wounded in combat and those with particularly severe injuries have the highest likelihood of later PTSD [2,4,46- 47]. Therefore, it appears reasonable to suggest that mor- phine treatment following a combat injury may reduce the likelihood of later PTSD.
Importantly, a second implication should be drawn from the finding that combat amputees have increased rates of PTSD over the first 4 yr postinjury. Specifically, military and VA providers should use routine healthcare visits (e.g., primary care) as an opportunity for regular and proactive screening for mental health disorders for several years after injury. One explanation is that new postinjury stressors or trauma [28-29] caused new cases of PTSD with delayed onset. Most amputees leave mili- tary service within the first year or two after injury [6,24] and typically make substantial and sometimes difficult lifestyle changes as civilians. Alternatively, healthcare utilization or reporting bias may have occurred both very early and also several years later postinjury. Nearly all patients with amputation receive appropriate psychologi- cal screening from military providers soon after injury [6,8]. However, patients may not have reported PTSD to military providers to avoid stigma or negative effect on their military career [2]. They may also have been diag- nosed with related conditions, including other anxiety and mood disorders [6]. Initial VA healthcare evaluations typically follow separation from military service, and patients may have been more likely to report mental health issues to VA providers at this time. These VA diag- noses likely will not be seen by their civilian employer and may facilitate VA benefits for appropriate treatment. (However, there is no strong evidence of an association between benefit seeking and PTSD [1].) In general, our finding that combat amputees have increasing prevalence of PTSD over the first 4 yr postinjury supports a sus- tained and proactive approach by military and VA health professionals to screen for mental health disorders.
Many studies of postinjury psychological outcomes of servicemembers injured in the
The strengths of the present study included access to casualty records in the EMED, which detailed specific patient injuries, early medications, and GCS scores. We also integrated military and VA health data from near point of injury through 48 mo postinjury for more than 90 per- cent of patients in the study sample. The primary limitation was small sample size. The diagnostic criteria for PTSD overlaps with other psychological disorders (e.g., TBI, mood, and postconcussion syndrome) and, therefore, cases of PTSD might have been misdiagnosed [32]. To minimize this problem, we included PTSD cases only for patients with at least two separate PTSD diagnoses [39].
As described in our previous study, IV morphine and IV fentanyl have the potential for adverse side effects that may negatively affect hemodynamics. Physicians are encouraged to consider the present results along with military guidelines, which emphasize careful evaluation of trauma patient status before administering these medi- cations [14]. Finally, opioids have great potential for addiction, and consequently, providers should exercise caution and appropriate follow-up for patients receiving morphine and/or fentanyl for analgesia [48].CONCLUSIONS
The present study found that combat amputees treated with early IV morphine (vs IV fentanyl) had sig- nificantly reduced PTSD and mood diagnoses during the first 2 yr after injury. These results included both military and VA health data. These associations were specific to patients with a TBI diagnosis. In contrast, morphine was not associated with reduced rates of other psychological outcomes (e.g., adjustment, anxiety, and substance abuse disorders). However, the present study found that early IV morphine was not associated with reduced PTSD rates during the third and fourth year postinjury. Finally, we found a substantial increase in the prevalence of PTSD over the first 4 yr postinjury, a result based on combining military and VA health data to more accurately capture these outcomes. Further research should determine the generality of the present findings to nonamputees with serious combat limb injuries.
ACKNOWLEDGMENTS
Author Contributions:
Drafted manuscript:
Contributed significantly to drafting "Introduction" and "Discussion" sections of manuscript:
Critically reviewed manuscript:
Conducted literature review:
Assisted in analysis:
Responsible for overall scientific conduct of study, including military institutional review board (IRB) documentation:
Integrated military medication data and military and VA health outcomes data, preparing all files for analysis:
Oversaw VA data collection and analysis, including IRB documentation for VA healthcare data:
Worked with national VA health data centers for data extraction and analysis:
Conducted longitudinal modeling of medications and psychological outcomes:
Organized medication data extracted from casualty records:
Conducted longitudinal analyses of psychological disorders:
Presented results at Military Health Services Research Symposium,
Developed overall clinical approach for classification of medications and psychological outcomes:
Assisted in extraction of medication data from casualty records:
Reviewed individual casualty records to document postinjury shock and/or loss of consciousness:
Directly coded and collected specific medication data from casualty records:
Developed access to health databases and casualty records containing injury severity scores and early postinjury medication data:
Financial Disclosures: The authors have declared that no competing interests exist.
Funding/Support: This material was based on work supported by the
Additional Contributions: This study, and the manuscript itself, bene- fited greatly from advice and assistance from the clinicians, epidemiolo- gists, technical writers, database analysts, and programmers working on the Expeditionary Medical Encounter Database project at the
Institutional Review: The study was approved by the IRBs at the NHRC (IRB 2007.0016) and by the Research and Development Com- mittee of the
Participant Follow-Up: The authors do not plan to inform participants of the publication of this study because contact information is unavailable.
Disclaimer: The views expressed in this article are those of the authors and do not reflect the official policy or position of the Depart- ment of the
This article and any supplementary material should be cited as follows:
Melcer T, Walker J, Bhatnagar V, Richard E, Han P, Sechriest VF 2nd, Lebedda M, Quinn K, Galarneau M. Glasgow Coma Scale scores, early opioids, and 4-year psychological outcomes among combat amputees. J Rehabil Res Dev. 2014;51(5):697-710.
http://dx.doi.org/10.1682/JRRD.2013.06.0143
REFERENCES
1. Dohrenwend BP, Turner JB,
2. Hoge CW, Castro CA, Messer SC, McGurk D, Cotting DI, Koffman RL. Combat duty in
3. Hoge CW, Terhakopian A, Castro CA, Messer SC, Engel CC. Association of posttraumatic stress disorder with somatic symptoms, health care visits, and absenteeism among
4. MacGregor AJ, Shaffer RA, Dougherty AL, Galarneau MR, Raman R, Baker DG, Lindsay SP, Golomb BA, Corson KS. Psychological correlates of battle and nonbattle injury among Operation Iraqi Freedom veterans. Mil Med. 2009;174(3):224-31. [PMID:19354083] http://dx.doi.org/10.7205/MILMED-D-03-9107
5. Pittman JO, Goldsmith AA, Lemmer JA, Kilmer MT, Baker DG. Post-traumatic stress disorder, depression, and health-related quality of life in OEF/OIF veterans. Qual Life Res. 2012;21(1):99-103. [PMID:21516356] http://dx.doi.org/10.1007/s11136-011-9918-3
6. Melcer T, Sechriest VF, Walker J, Galarneau M. A comparison of health outcomes for combat amputee and limb salvage patients injured in
7.
8. Wain HJ, Bouterie A, Oleshansky M. Psychiatric intervention for the orthopedically injured. In: Pasquina PF, Cooper RA, editors. Care of the combat amputee.
9. Cesur R, Sabia JJ, Tekin E. The psychological costs of war: military combat and mental health [Internet]. Cambridge (MA):
10. Melcer T, Walker J, Sechriest VF 2nd, Lebedda M, Quinn K, Galarneau MR. Glasgow Coma Scores, early opioids, and posttraumatic stress disorder among combat amputees. J Trauma Stress. 2014;27(2):152-59. [PMID:24668780] http://dx.doi.org/10.1002/jts.21909
11. Matis G, Birbilis T. The Glasgow Coma Scale-a brief review. Past, present, future. Acta Neurol Belg. 2008;108(3): 75-89. [PMID:19115670]
12. Teasdale G, Jennett B. Assessment of coma and impaired consciousness. A practical scale. Lancet. 1974;304(7872): 81-84. [PMID:4136544] http://dx.doi.org/10.1016/S0140-6736(74)91639-0
13. Chiu KB, deRoon-Cassini TA, Brasel KJ. Factors identifying risk for psychological distress in the civilian trauma population. Acad Emerg Med. 2011;18(11):1156-60. [PMID:22044521] http://dx.doi.org/10.1111/j.1553-2712.2011.01206.x
14. Fox DJ, Saunders LD, Menk EJ, Middaugh R. Intravenous anesthesia. In: Zajtchuk R, Bellamy RF, Grande CM, editors. Anesthesia and perioperative care of the combat casualty.
15. Black IH, McManus J. Pain management in current combat operations. Prehosp Emerg Care. 2009;13(2):223-27. [PMID:19291561] http://dx.doi.org/10.1080/10903120802290778
16. Kacprowicz RF, Johnson TR, Mosely DS. Fentanyl for pain control in Special Operations. J Spec Ops Med. 2008; 8(1):48-53.
17. Claxton AR, McGuire G, Chung F, Cruise C. Evaluation of morphine versus fentanyl for postoperative analgesia after ambulatory surgical procedures. Anesth Analg. 1997;84(3): 509-14. [PMID:9052292]
18. Holbrook TL, Galarneau MR, Dye JL, Quinn K, Dougherty AL. Morphine use after combat injury in
19. Wedmore IS, Kotwal RS, McManus JG, Pennardt A, Talbot TS, Fowler M, McGhee L. Safety and efficacy of oral transmucosal fentanyl citrate for prehospital pain control on the battlefield. J Trauma Acute Care Surg. 2012;73(6 Suppl 5):S490-95. [PMID:23192075] http://dx.doi.org/10.1097/TA.0b013e3182754674
20. Bryant RA, Creamer M, O'Donnell M, Silove D, McFarlane AC. A study of the protective function of acute morphine administration on subsequent posttraumatic stress disorder. Biol Psychiatry. 2009;65(5):438-40. [PMID:19058787] http://dx.doi.org/10.1016/j.biopsych.2008.10.032</p>
21. Pasternak GW. Preclinical pharmacology and opioid combinations. Pain Med. 2012;13(Suppl 1):S4-11. [PMID:22420604] http://dx.doi.org/10.1111/j.1526-4637.2012.01335.x
22. Gunderson EK, Garland CF, Miller MR, Gorham ED. Career History Archival Medical and Personnel System. Mil Med. 2005;170(2):172-75. [PMID:15782842]
23.
24. Stinner DJ,
25. Melcer T, Walker GJ, Galarneau M, Belnap B, Konoske P. Midterm health and personnel outcomes of recent combat amputees. Mil Med. 2010;175(3):147-54. [PMID:20358702] http://dx.doi.org/10.7205/MILMED-D-09-00120
26.
27. Potter BK, Scoville CR. Amputation is not isolated: An overview of the US Army Amputee Patient Care Program and associated amputee injuries. J Am Acad Orthop Surg. 2006;14(10 Spec No.):S188-90. [PMID:17003197]
28. Copeland LA, Zeber JE, Bingham MO, Pugh MJ, Noƫl PH, Schmacker ER, Lawrence VA. Transition from military to VHA care: Psychiatric health services for
29. Horesh D, Solomon Z, Zerach G, Ein-Dor T. Delayed-onset PTSD among war veterans: The role of life events throughout the life cycle. Soc Psychiatry Psychiatr Epidemiol. 2011;46(9):863-70. [PMID:20582726] http://dx.doi.org/10.1007/s00127-010-0255-6
30. Andrews B, Brewin CR, Philpott R, Stewart L. Delayedonset posttraumatic stress disorder: A systematic review of the evidence. Am J Psychiatry. 2007;164(9):1319-26. [PMID:17728415] http://dx.doi.org/10.1176/appi.ajp.2007.06091491
31. Cohen BE, Gima K, Bertenthal D, Kim S, Marmar CR, Seal KH. Mental health diagnoses and utilization of VA non-mental health medical services among returning
32. Lew HL, Pogoda TK, Hsu PT, Cohen S, Amick MM, Baker E, Meterko M, Vanderploeg RD. Impact of the "polytrauma clinical triad" on sleep disturbance in a department of veterans affairs outpatient rehabilitation setting. Am J Phys Med Rehabil. 2010;89(6):437-45. [PMID:20489391] http://dx.doi.org/10.1097/PHM.0b013e3181ddd301
33. Galarneau MR, Hancock WC, Konoske P, Melcer T, Vickers RR, Walker GJ, Zouris JM. The
34. Copes WS, Champion HR, Sacco WJ, Lawnick MM, Keast SL, Bain LW. The injury severity score revisited. J Trauma. 1988;28(1):69-77. [PMID:3123707] http://dx.doi.org/10.1097/00005373-198801000-00010
35. Armed Forces Health Surveillance Center. Deploymentrelated conditions of special surveillance interest. MSMR. 2011;18(9):17-19.
36. MacGregor AJ, Shaffer RA, Dougherty AL, Galarneau MR, Raman R, Baker DG, Lindsay SP, Golomb BA, Corson KS. Prevalence and psychological correlates of traumatic brain injury in operation iraqi freedom. J Head Trauma Rehabil. 2010;25(1):1-8. [PMID:20051901] http://dx.doi.org/10.1097/HTR.0b013e3181c2993d
37.
38. Benedek DM, Schneider BJ, Bradley JC. Psychiatric medications for deployment: An update. Mil Med. 2007;172(7): 681-85. [PMID:17691678]
39. Gravely AA, Cutting A, Nugent S, Grill J, Carlson K, Spoont M. Validity of PTSD diagnoses in VA administrative data: Comparison of VA administrative PTSD diagnoses to self-reported PTSD Checklist scores. J Rehabil Res Dev. 2011;48(1):21-30. [PMID:21328160] http://dx.doi.org/10.1682/JRRD.2009.08.0116
40. Akaike H. A new look at the statistical model identification. IEEE Trans Automat Contr. 1974;19:716-23. http://dx.doi.org/10.1109/TAC.1974.1100705
41. Hoge CW, McGurk D, Thomas JL, Cox AL, Engel CC, Castro CA. Mild traumatic brain injury in U.S. Soldiers returning from
42. Schneiderman AI, Braver ER, Kang HK. Understanding sequelae of injury mechanisms and mild traumatic brain injury incurred during the conflicts in
43. Brown TA, Campbell LA, Lehman CL, Grisham JR, Mancill RB. Current and lifetime comorbidity of the DSM-IV anxiety and mood disorders in a large clinical sample. J Abnorm Psychol. 2001;110(4):585-99. [PMID:11727948] http://dx.doi.org/10.1037/0021-843X.110.4.585
44. Forbes D, Elhai JD, Lockwood E, Creamer M, Frueh BC, Magruder KM. The structure of posttraumatic psychopathology in veterans attending primary care. J Anxiety Disord. 2012;26(1):95-101. [PMID:22036064] http://dx.doi.org/10.1016/j.janxdis.2011.09.004
45. Fletcher S, Creamer M, Forbes D. Preventing post traumatic stress disorder: Are drugs the answer? Aust N Z J Psychiatry. 2010;44(12):1064-71. [PMID:21070102] http://dx.doi.org/10.3109/00048674.2010.509858
46. Koren D, Norman D, Cohen A, Berman J, Klein EM. Increased PTSD risk with combat-related injury: A matched comparison study of injured and uninjured soldiers experiencing the same combat events. Am J Psychiatry. 2005;162(2):276-82. [PMID:15677591] http://dx.doi.org/10.1176/appi.ajp.162.2.276
47. MacGregor AJ, Corson KS, Larson GE, Shaffer RA, Dougherty AL, Galarneau MR, Raman R, Baker DG, Lindsay SP, Golomb BA. Injury-specific predictors of posttraumatic stress disorder. Injury. 2009;40(9):1004-10. [PMID:19524912] http://dx.doi.org/10.1016/j.injury.2009.04.006
48. Malchow RJ, King KK, Chan BL, Weeks SR, Tsao JW. Pain management among soldiers with amputations. In: Pasquina PF, Cooper RA, editors. Care of the combat amputee.
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