1. Vestibular Dysfunction in �Active Duty Personnel �Deployed to OEF/OIF LCDR Dennis Faix, MC, USN
Navy Environmental and Preventive Medicine Unit FIVE
2. Vestibular Dysfunction Investigation 2 Background�Events leading to Investigation
3. Vestibular Dysfunction Investigation 3 Preliminary Steps Initially: 12 cases of “Larium toxicity”
Confirmed diagnosis with outside expert
Background rate of dizziness/VOR dysfunction
Developed case definition
Now only ten cases
Multiple (ototoxic) exposures
Apparent cluster in one small unit
4 cases from 33-member Navy Tactical Dissemination Module (TDM) team
4. Vestibular Dysfunction Investigation 4 Methods Case-control study looking at multiple exposures
Surveyed two units stationed at AASAB at same time
Investigator-administered telephone survey, 188 questions
Navy TDM (n=33, 100%) ? 4 cases
Army 286th ADB (n=18, ~10%) ? 2 cases
Medical record review of cases (n=9, 75%)
Serum mefloquine levels (n=26, 55%)
Mefloquine tablet testing (n=3, 43%)
Review of clinic mobilization process
5. Vestibular Dysfunction Investigation 5 Results�Demographics & Medical History Overall there were no clinically significant demographic difference between cases and controls
ADB group was younger, active duty
No significant difference in medical history
Except for PMH of motion sickness
Cases tended to be deployed longer than controls, but not significantly
6. Vestibular Dysfunction Investigation 6 Results�Timeline of Deployment, Mefloquine Use and Symptoms for Cases
7. Vestibular Dysfunction Investigation 7 Results�Combat Stress Exposures
8. Vestibular Dysfunction Investigation 8 Results�Neuropsychiatric Symptoms (TDM group)
9. Vestibular Dysfunction Investigation 9 Results�Neuropsychiatric Symptoms (ADB group)
10. Vestibular Dysfunction Investigation 10 Results�Malaria Chemoprophylaxis Exposures (TDM group only)
11. Vestibular Dysfunction Investigation 11 Results�Chart review & Tablet Testing Three of 9 records reviewed had documentation of pre-deployment health assessments
None had documentation of counseling or screening prior to issuance of mefloquine
Post-Deployment Health Assessment in 6 of 9 charts
Mefloquine tablets tested by FDA
No abnormalities in quality, constitution
Tablets held up well to individual issue and deployment to desert environment
12. Vestibular Dysfunction Investigation 12 Discussion�Limitations Small numbers (pilot study)
Potential Bias
Selection bias
Recall bias
Misclassification bias
Patient X
OIC of TDM group while deployed to AASAB
Instructed team to seek medical care if they took mefloquine
Informed teammates, Senator Feinstein and lay press of “link” with mefloquine
Currently suing Lariam manufacturer
13. Vestibular Dysfunction Investigation 13 Discussion�Biological Plausibility Acute neurotoxicity of mefloquine
Anxiety, dizziness are known acute side effects, no evidence of long-term effects
Disruption of endoplasmic reticulum and gap junction channels reported (Dow, 2003; Cruikshank 2004)
Known association between anxiety disorders and vestibular dysfunction
Nearly 3 times as many persons with self-reported dizziness had symptoms of anxiety compared to persons without dizziness in large, U.K. study (Yardley, 1998)
Individuals with anxiety may exhibit abnormal findings on rotational chair testing (Rolf, 1996)
Interaction of effects of mefloquine and combat stress? Cruikshank, S. J., M. Hopperstad, et al. (2004). "Potent block of Cx36 and Cx50 gap junction channels by mefloquine." Proc Natl Acad Sci U S A 101(33): 12364-9.
Recently, great interest has been shown in understanding the functional roles of specific gap junction proteins (connexins) in brain, lens, retina, and elsewhere. Some progress has been made by studying knockout mice with targeted connexin deletions. For example, such studies have implicated the gap junction protein Cx36 in synchronizing rhythmic activity of neurons in several brain regions. Although knockout strategies are informative, they can be problematic, because compensatory changes sometimes occur during development. Therefore, it would be extremely useful to have pharmacological agents that block specific connexins, without major effects on other gap junctions or membrane channels. We show that mefloquine, an antimalarial drug, is one such agent. It blocked Cx36 channels, expressed in transfected N2A neuroblastoma cells, at low concentrations (IC(50) approximately 300 nM). Mefloquine also blocked channels formed by the lens gap junction protein, Cx50 (IC(50) approximately 1.1 microM). However, other gap junctions (e.g., Cx43, Cx32, and Cx26) were only affected at concentrations 10- to 100-fold higher. To further examine the utility and specificity of this compound, we characterized its effects in acute brain slices. Mefloquine, at 25 microM, blocked gap junctional coupling between interneurons in neocortical slices, with minimal nonspecific actions. At this concentration, the only major side effect was an increase in spontaneous synaptic activity. Mefloquine (25 microM) caused no significant change in evoked excitatory or inhibitory postsynaptic potentials, and intrinsic cellular properties were also mostly unaffected. Thus, mefloquine is expected to be a useful tool to study the functional roles of Cx36 and Cx50.
Dow, G. S., T. H. Hudson, et al. (2003). "The acute neurotoxicity of mefloquine may be mediated through a disruption of calcium homeostasis and ER function in vitro." Malar J 2(1): 14.
BACKGROUND: There is no established biochemical basis for the neurotoxicity of mefloquine. We investigated the possibility that the acute in vitro neurotoxicity of mefloquine might be mediated through a disruptive effect of the drug on endoplasmic reticulum (ER) calcium homeostasis. METHODS: Laser scanning confocal microscopy was employed to monitor real-time changes in basal intracellular calcium concentrations in embryonic rat neurons in response to mefloquine and thapsigargin (a known inhibitor of the ER calcium pump) in the presence and absence of external calcium. Changes in the transcriptional regulation of known ER stress response genes in neurons by mefloquine were investigated using Affymetrix arrays. The MTT assay was employed to measure the acute neurotoxicity of mefloquine and its antagonisation by thapsigargin. RESULTS: At physiologically relevant concentrations mefloquine was found to mobilize neuronal ER calcium stores and antagonize the pharmacological action of thapsigargin, a specific inhibitor of the ER calcium pump. Mefloquine also induced a sustained influx of extra-neuronal calcium via an unknown mechanism. The transcription of key ER proteins including GADD153, PERK, GRP78, PDI, GRP94 and calreticulin were up-regulated by mefloquine, suggesting that the drug induced an ER stress response. These effects appear to be related, in terms of dose effect and kinetics of action, to the acute neurotoxicity of the drug in vitro. CONCLUSIONS: Mefloquine was found to disrupt neuronal calcium homeostasis and induce an ER stress response at physiologically relevant concentrations, effects that may contribute, at least in part, to the neurotoxicity of the drug in vitro.
Cruikshank, S. J., M. Hopperstad, et al. (2004). "Potent block of Cx36 and Cx50 gap junction channels by mefloquine." Proc Natl Acad Sci U S A 101(33): 12364-9.
Recently, great interest has been shown in understanding the functional roles of specific gap junction proteins (connexins) in brain, lens, retina, and elsewhere. Some progress has been made by studying knockout mice with targeted connexin deletions. For example, such studies have implicated the gap junction protein Cx36 in synchronizing rhythmic activity of neurons in several brain regions. Although knockout strategies are informative, they can be problematic, because compensatory changes sometimes occur during development. Therefore, it would be extremely useful to have pharmacological agents that block specific connexins, without major effects on other gap junctions or membrane channels. We show that mefloquine, an antimalarial drug, is one such agent. It blocked Cx36 channels, expressed in transfected N2A neuroblastoma cells, at low concentrations (IC(50) approximately 300 nM). Mefloquine also blocked channels formed by the lens gap junction protein, Cx50 (IC(50) approximately 1.1 microM). However, other gap junctions (e.g., Cx43, Cx32, and Cx26) were only affected at concentrations 10- to 100-fold higher. To further examine the utility and specificity of this compound, we characterized its effects in acute brain slices. Mefloquine, at 25 microM, blocked gap junctional coupling between interneurons in neocortical slices, with minimal nonspecific actions. At this concentration, the only major side effect was an increase in spontaneous synaptic activity. Mefloquine (25 microM) caused no significant change in evoked excitatory or inhibitory postsynaptic potentials, and intrinsic cellular properties were also mostly unaffected. Thus, mefloquine is expected to be a useful tool to study the functional roles of Cx36 and Cx50.
Dow, G. S., T. H. Hudson, et al. (2003). "The acute neurotoxicity of mefloquine may be mediated through a disruption of calcium homeostasis and ER function in vitro." Malar J 2(1): 14.
BACKGROUND: There is no established biochemical basis for the neurotoxicity of mefloquine. We investigated the possibility that the acute in vitro neurotoxicity of mefloquine might be mediated through a disruptive effect of the drug on endoplasmic reticulum (ER) calcium homeostasis. METHODS: Laser scanning confocal microscopy was employed to monitor real-time changes in basal intracellular calcium concentrations in embryonic rat neurons in response to mefloquine and thapsigargin (a known inhibitor of the ER calcium pump) in the presence and absence of external calcium. Changes in the transcriptional regulation of known ER stress response genes in neurons by mefloquine were investigated using Affymetrix arrays. The MTT assay was employed to measure the acute neurotoxicity of mefloquine and its antagonisation by thapsigargin. RESULTS: At physiologically relevant concentrations mefloquine was found to mobilize neuronal ER calcium stores and antagonize the pharmacological action of thapsigargin, a specific inhibitor of the ER calcium pump. Mefloquine also induced a sustained influx of extra-neuronal calcium via an unknown mechanism. The transcription of key ER proteins including GADD153, PERK, GRP78, PDI, GRP94 and calreticulin were up-regulated by mefloquine, suggesting that the drug induced an ER stress response. These effects appear to be related, in terms of dose effect and kinetics of action, to the acute neurotoxicity of the drug in vitro. CONCLUSIONS: Mefloquine was found to disrupt neuronal calcium homeostasis and induce an ER stress response at physiologically relevant concentrations, effects that may contribute, at least in part, to the neurotoxicity of the drug in vitro.
14. Vestibular Dysfunction Investigation 14 Conclusions Cases had evidence of vestibular abnormalities most commonly seen with migraine or anxiety-related dizziness, and not that seen with ototoxicity.
The rate of balance disorders and dizziness among these subjects is within the reported normal range in the general population. However, the actual rate for these disorders in an active duty population is unknown.
No evidence that mefloquine or any known vestibulotoxic agent was associated with the vestibular dysfunction exhibited in these cases.
15. Vestibular Dysfunction Investigation 15 Conclusions Cases reported higher levels of combat stress and neuropsychiatric symptoms as compared to controls, suggesting that combat-related stressors may be associated with vestibular dysfunction.
An interaction between mefloquine and combat stress cannot be ruled out
Documentation of pre-deployment health assessments and appropriate mefloquine screening was not found in the medical records reviewed.
16. Vestibular Dysfunction Investigation 16 Recommendations Further study on possible interaction between mefloquine, vestibular dysfunction and combat stress
Exploit existing databases (pharmacy, deployment, PDHA, etc)
Selected survey of redeploying personnel
DOD-wide case finding for a larger case control study
Establish baseline dizziness and VOR abnormality rates among active duty personnel
Study underway at NMCSD; 10% complete
Re-emphasize DOD guidance regarding pre-deployment medical screening
Force Health Protection Prescription Products
Pre-Deployment Health Assessments
17. Vestibular Dysfunction Investigation 17 Acknowledgements Centers for Disease Control and Prevention
CAPT Peter Bloland, USPHS
Aaron Mendelsohn, PhD
CAPT Monica Parise, USPHS
LCDR Snehal Shah, USPHS
Navy Environmental and Preventive Medicine Unit FIVE
CAPT Dean Bailey, MC, USN
LCDR Julie Howe, MC, USN
LCDR Andrew Vaughn, MC, USN
LCDR Todd Wagner, MC, USN
Navy Health Research Center
Defense Medical Surveillance System (AMSA)
Food and Drug Administration
18. BACKUP SLIDES
19. Vestibular Dysfunction Investigation 19 Background�Events prior to investigation Fort Bragg suicides/homicides
Lay press reports
AFEB recommendation
Keep mefloquine
VA letter
Blue ribbon panel
Mefloquine recall to wholesale level secondary to possible contamination
20. Vestibular Dysfunction Investigation 20 Methods�Case Definition Cases must be DOD Personnel (active duty, reserve, or civilian) deployed as part of Operation Iraqi Freedom or Operation Enduring Freedom since January 1, 2002, and
Report new onset of dizziness during or after deployment lasting two weeks or more as a single episode or multiple episodes, and
Have no other identifiable etiology including, vestibular neuronitis, Meniere’s disease, head trauma, acoustic neuroma, benign paroxysmal positional vertigo (BPPV), labyrinthitis, or prior ear surgery, and
Demonstrate unsteadiness of gait while walking or while standing still on physical exam, and
Have VOR asymmetry on Rotational Chair Testing independently confirmed by two subject matter experts.
21. Vestibular Dysfunction Investigation 21 Methods�Case Selection (Tactical Dissemination Module)
22. Vestibular Dysfunction Investigation 22 Methods�Case Selection (Air Defense Battery)
23. Vestibular Dysfunction Investigation 23 Methods�Survey Deployment history
Medical history
Medication history
Environmental exposure history
Symptoms
Combat stress history
188 questions total
24. Vestibular Dysfunction Investigation 24 Methods�Tablet Analysis 7 individuals reported leftover tablets available
3 individual actually sent tablets in for testing
Sent to FDA for analysis
