Table 1.
Summary of included studies and findings for APOE allelic variants.
| Search Criteria [Title/Abstract/MeSH Terms]: (Chronic Traumatic Encephalopathy or Mild Traumatic Brain Injury or Concussion) and Apolipoprotein E | ||||||
|---|---|---|---|---|---|---|
| MTBI in Athlete Cohorts (8 Studies) | ||||||
| Author and Year | Study Type | N | Sex; Age | Description | Outcome Measures | Results |
| Cochrane et al., 2018 | MTBI, prospective, athletes | 250 collegiate athletes (95 football, 58 baseball/softball, 67 soccer, 18 basketball, 2 cross-country/track and field) | 184 male, 66 female; 19.0 ± 1.3 years old | APOE-ε2 carriers (n = 28), APOE-ε3 carriers (n = 128), APOE-ε4 carriers (n = 68), 24% self-reported a history of prior concussion. | Self-reported history of concussions and neurocognitive performance from Immediate Post-concussion Assessment and Cognitive Testing (ImPACT). | Apo-ε4 carriers had significantly slower reaction time (p = 0.002) as measured by the ImPACT. |
| Kristman et al., 2008 | MTBI, prospective, athletes | 318 collegiate athletes (43 football, 26 field hockey, 32 basketball, 23 ice hockey, 45 lacrosse, 49 rugby, 53 soccer, 47 volleyball) | 164 male, 154 female, mean age 20.5 ± 2.4 years (range 17–31) | 79 (24.8%) APOE-ε4(+) athletes | Concussions in athletes were diagnosed by the sport-medicine team and verified by a sport-medicine physician. | In the proportional hazards model, presence of the APOE-ε4 was not significantly associated with concussion (p = 0.68). |
| Merritt et al., 2016 | MTBI, prospective, athletes | 42 collegiate athletes (sports not defined) | 35 male, 7 female; subjects with mild concussions (14.3% LOC); ε4 carriers aged 19.9 ± 1.4 years, noncarriers aged 20.0 ± 1.6 years | 15 (35.7%) APOE-ε4(+) athletes, and 27 (64.3%) APOE-ε4(−) athletes | Team physicians determined TBI and concussed athletes were referred for neuropsychological testing post-injury. The Post-Concussion Symptom Scale was used to evaluate self-report symptoms. Physical and cognitive symptom clusters were each dichotomized into “symptoms present” versus “symptoms absent” groups | ε4-carriers associated with “symptoms present” group; ε4(+) athletes more likely to endorse physical symptoms than ε4(−) athletes (odds ratio (OR) = 5.25 (1.33–20.76); p = 0.015)). For cognitive symptoms, ε4-carriers associated with “symptoms present” group; ε4(+) athletes more likely to endorse cognitive symptoms than ε4(−) athletes, (OR = 4.75 (1.23–18.41), p = 0.020) |
| Merritt et al., 2018 | MTBI, prospective, athletes | 57 collegiate athletes (16 football, 11 basketball, 8 lacrosse, 7 rugby, 7 hockey, 4 soccer, 2 wresting, 2 other). | 44 males, 13 females; ε4 carriers 20.3 ± 1.4 years old, ε4 noncarriers 20.3 ± 1.4 years old | 20 athletes (35.1%) APOE-ε4(+); 37 athletes (64.9%) APOE-ε4(−) | Neurocognitive test battery including learning and memory, attention, processing speed, and executive functions: Brief Visuospatial Memory Test, Hopkins Verbal Learning Test; Symbol-Digit Modalities Test; Vigil Continuous Performance Test; Digit Span Test from the WAIS-III; Trail-Making Test; Penn State University Cancellation Test; Stroop Color-Word Test; ImPACT. | No significant differences were seen between athletes with and without the APOE-ε4 allele when examining mean neurocognitive scores (all p > 0.05). However, ε4(+) subjects were more likely to show a greater number of impaired neurocognitive scores post-injury compared to ε4(−) athletes (p < 0.05). More ε4+ athletes (40.0%; 8 of 20) fell in the impaired group compared with ε4- athletes (16.2%; 6 of 37; p = 0.046). APOE-ε4(+) athletes demonstrated greater neurocognitive variability than athletes without APOE-ε4 (p < 0.05). |
| Abrahams et al., 2017 | MTBI retrospective, athletes (rugby) | 288 rugby athletes (121 high school, 116 club, 51 professional) | Males; controls younger than concussed group (19.2 ± 3.5 years vs. 20.5 ± 4.4 years; p = 0.008) | The concussed group (N = 160) reported 1.9 ± 1.0 prior concussions (45%: 1; 34.4%: 2; 8.8%: 3; 11.9%: 4 concussions) | Self-reported duration of symptoms (<1 week versus ≥1 week) | APOE-ε4 isoforms did not differ significantly between concussion and control groups. APOE-ε4 isoform frequency distribution did not differ significantly between duration of symptoms groups |
| Casson et al., 2014 | Chronic brain damage, retrospective cross-sectional, athletes | 45 retired National Football League (NFL) players | 45 males; 45.6 ± 8.9 years old (range, 30–60 years) | Athletes reported 6.9 ± 6.2 concussions (maximum 25) throughout their careers | MMSE, dysarthria, pyramidal system dysfunction, extrapyramidal system dysfunction, cerebellar dysfunction, depression, PHQ9, ImPACT. susceptibility weighted imaging (SWI) and diffusion tensor imaging (DTI) evaluation for brain injuries | APOE-ε4 allele present in 38% of players, a larger number than expected in the general male population (23–26%). No association of the APOE-ε4 genotype with anatomical magnetic resonance imaging (MRI), clinical neurologic, depression, or neuropsychological test results |
| Esopenko et al., 2017 | MTBI, retrospective, alumni athletes | 33 retired National Hockey League (NHL) players | 53 males; alumni athletes 54.3 ± 10.4 years old, controls 53.4 ± 10.2 years old, | Concussions in athletes were 4.8 ± 2.7; in controls were 0.6 ± 0.8; 9 alumni and 4 controls were ε4(+); 1 ε4/ε4, 2 ε2/ε4, rest were ε2/ε3 or ε3/ε3 | Self-reported history of concussion, cognitive function and questionnaires on psychosocial/psychiatric function | ε4-carriers associated with increased psychiatric complaints (p = 0.009) but not objective cognitive performance. Executive function associated with number of concussions after accounting for confounders (β = −0.55 and −0.39, p = 0.005 and p = 0.039 for concussion and age, respectively) |
| Tierney et al., 2010 | MTBI, retrospective, athletes | 196 collegiate athletes (163 football; 33 soccer) | 163 male football and 33 female soccer athletes, age was 19.7 ± 1.5 years old | 48 (24.5%) with 1 concussion, 9/48 (4.6%) with >1 concussions. ε2 and ε4 present in 35 (17.7%) and 62 (31.9%) athletes. | Self-reported history of concussions. | No association between ε4 and ε2 carriers and history of concussion. Significant association (OR = 9.8; p = 0.05) between carrying APOE rare alleles and prior concussions. |
| MTBI in Military Cohorts (5 Studies) | ||||||
| Author | Study Type | N | Sex; Age | Description | Outcome Measures | Results |
| Dretsch et al., 2017 | MTBI, retrospective, active-duty military | 458 military members from two brigade combat teams preparing to deploy to Iraq and Afghanistan | 430 male, 28 female; age was 26.0 ± 7.0 years | History of concussion in 36.5%, with 10.7% having 3+ concussions. 38% (162/430) of men with 1+ concussions, vs. 18% (5/28) of women | Self-reported history of concussions | APOE not associated with risk for concussions. Of ε3/ε4 or ε4/ε4 soldiers, 44.1% (41/93) had a history of one or more prior concussions compared with 34.5% (126/365) of the comparison group (OR = 1.50; p = 0.087) |
| Emmerich et al., 2016 | MTBI, retrospective, active-duty military | 120 demographically matched soldiers with prior deployment to Iraq or Afghanistan (21 with TBI, 34 with posttraumatic stress disorder (PTSD); 13 with TBI + PTSD; 52 controls) | 120 males; TBI subjects’ age was 25.9 ± 1.4 years, PTSD subjects’ age was 26.4 ± 1.3 years, TBI + PTSD subjects’ age was 29.9 ± 1.6 years old; control subjects’ age was 26.7 ± 1.0 years | 85 APOE-ε4(−) (control n = 37, TBI n = 16, PTSD n = 24, TBI + PTSD n = 8); APOE-ε4(+) n = 35 (control n = 15, TBI = 5, PTSD = 10, TBI + PTSD n = 5) | Self-reported history of TBI, including military-associated injury and all other traumas; alcohol use; medical history; prior deployments; current medications; PTSD symptoms; and depression. Blood samples for lipidomic analysis. | ε4(+) subjects exhibited higher plasma phospholipids levels than their ε4(−) counterparts within diagnostic groups. ε4 noncarriers showed decreased saturated fatty acids (SFA)- and monounsaturated fatty acids (MUFA)-containing phosphatidylethanolamine (PE) species for TBI, PTSD, and TBI+PTSD groups, compared with controls. ε4 carriers showed no significant differences between TBI and PTSD groups for SFA- and MUFA. Interaction between ε4-carriers and diagnosis of TBI+PTSD on MUFA-containing lysophosphatidylcholine (LPC) and lysophosphatidylethanolamide (LPE) species. |
| Han et al., 2009 | Mild to moderate TBI, retrospective, active-duty military | 53 military personnel | 42 male, 4 female; Mean age of APOE-ε4(+) was 22.6 ± 3.8 years, mean age of APOE-ε4(−) was 25.2 ± 6.1 years | 16 APOE-ε4(+), 30 APOE-ε4(−) | Job change (reduction in duties for any reason e.g., medical hold, rehabilitation or assignment to light/limited duties (n = 24), reduction due to TBI (n = 3), referral to Medical Board (n = 3), or administrative separation (n = 1)), using neuropsychological assessments | In ε4-carriers, job status was determined by a long-delay free recall on the CVLT-II. If the percent change between long-delay free recall and short-delay free recall (defined as ((long-delay free recall raw score) minus (short-delay free recall raw score))/(short-delay free recall raw score)) >3.55%, subjects correctly predicted as no change in work status (85.7% accuracy). If the percentage change was <3.55%, subjects were correctly predicted to have a change in their job status with 88.9% accuracy |
| Hayes et al., 2017 | MTBI, retrospective, veterans | 160 veterans of OEF/OIF and/or New Dawn | 149 male, 11 female; non-MTBI aged 32.9 ± 8.9 years, MTBI aged 30.6 ± 8.1 years | 55 with no MTBI, 105 with MTBI. ε4(+): 10/55 with no MTBI, 27/105 with MTBI | Linear models examined the main effect of APOE (ε4-carriers, n = 37; non-ε4 carriers, n = 123) and MTBI × APOE interaction factor on cortical thickness. | No main effect of APOE on cortical thickness; no MTBI/APOE interaction. |
| Nielsen et al., 2018 | MTBI, retrospective, veterans | 87 veterans with or without MTBI | Demographics not published | 47 veterans with MTBI and 40 controls | Hierarchical linear regression to evaluate the association between DNA methylation, MTBI, and APOE genotype with plasma APOE, controlling for age, sex, population structure, depression and PTSD | Plasma APOE associated with PTSD severity (p = 0.013). Higher APOE levels in ε3/ε3 compared to ε4 carriers (p = 0.031). Plasma APOE was associated with DNA methylation at CpG sites −877 (p = 0.021), and −775 (p = 0.014). The interaction factor ε4 × PTSD was associated with DNA methylation at CpG −675 (p = 0.009) |
| MTBI in Population-Based Cohorts (6 Studies) | ||||||
| Author | Study Type | N | Sex; Age | Description | Outcome Measures | Results |
| Lee et al., 2017 | MTBI, prospective, population-based | 189 patients from emergency departments (ED) of three hospitals | 76 male, 113 female; Mean age of ε4(+) was 42.2 ± 14.7 years and ε4(−) was 40.1 ± 15.2 years | 35 ε4(+), 154 ε4(−) | 1st week post-mTBI and 6th week post-mTBI) sleep assessments, using the Pittsburgh Sleep Quality Index (PSQI) | No difference in PSQI at baseline and week 6 between ε4-carriers and noncarriers. Both ε4 carriers and noncarriers exhibited improvement in overall PSQI scores between baseline and week 6 follow-up (carrier: baseline 8.3 ± 3.9, 6th week: 7.4 ± 4.9, p = 0.05; noncarrier: baseline 8.5 ± 4.4, 6th week: 8.1 ± 3.8, p = 0.03) |
| Liberman et al., 2002 | MTBI, prospective, population-based | 87 adult patients presenting with mild or moderate TBI to a shock trauma center | 48 males, 32 females; <30 years of age (n = 25), 30–49 years old (n = 28) and ≥50 years old (n = 27) | 18 ε4(+), 62 ε4(−) | 13 neuropsychological tests administered twice at 3 and 6 weeks post-injury | 90% with MTBI; 18 (22.5%) ε4-carriers, who had lower scores on 12 of 13 neuropsychological outcomes at visit 1 compared to noncarriers, 2 were significant (grooved pegboard test, p = 0.005; paced auditory serial addition task 2.8-s trial, p = 0.004). At visit 2, ε4(+) had lower adjusted mean scores on 11/13 neuropsychological outcomes, though none were statistically significant. |
| Muller et al., 2009 | MTBI, prospective, population-based | 59 patients with MTBI | 47 male, 12 female; Mean age 35.1 years (range 18–74) | 13 APOE-ε4(+), 46 APOE-ε4(−) | GCS in ED, head computed tomography (CT) and MRI, neurophysiological assessments at baseline and 6-months. Serum S100B was measured. | GCS < 15, TBI on CT/MRI, and serum S-100B > 0.14 μg/L predicted impaired cognitive performance at baseline and 6-months while APOE did not. APOE-ε4 genotype was the only independent factor significantly predicting less improvement from baseline to 6-months. |
| Sundstrom et al., 2007 | MTBI, prospective, population-based | 31 MTBI patients and 62 matched controls | 18 male, 13 female; Mean age 55.2 ± 13.6 years | APOE-ε4 present in 38.7% of MTBI subjects and controls | Self-reported pre and postinjury fatigue, anxiety, depression and sleep disturbance was compared within-group and between groups | In MTBI, fatigue was more commonly reported among ε4 carriers (58%) than noncarriers (32%). MTBI ε4-carriers were more often fatigued than controls with ε4 (58% vs. 17%, p = 0.02). No significant between-group differences between MTBI and controls without ε4 |
| Yang et al., 2015 | MTBI, prospective, population-based | 21 MTBI patients without dementia, 6 MTBI patients with dementia, and 10 controls without MTBI | 15 male, 22 female; (controls: 2 M, 8 F, aged 50.6 ± 6.8 years; MTBI without dementia: 9 M, 12 F, aged 53.7 ± 7.9 years; MTBI with dementia: 4 M, 2 F; aged 60.0 ± 7.5 years) | ε4 carriers: 5 of 21 MTBI without dementia, 4 of 6 MTBI with dementia, 1 of 10 controls | MMSE, amyloid-PET | ε4 frequency high in MTBI patients with dementia (p = 0.049). Linear regression between APOE-ε4 and average amyloid standardized uptake value ratio (SUVR) showed significant correlation for all subjects (p < 0.05) |
| Yue et al., 2017 | MTBI, prospective, population-based | 114 MTBI patients | 76 male, 38 female; aged 49.6 ± 13.6 for ε4(+); aged 39.7 ± 16.5 years for noncarriers | 79 ε4(−), 35 ε4(+) | 6-month verbal memory using the CVLT-II, including Short-Delay Free Recall (SDFR), Short-Delayed Cued Recall (SDCR), Long-Delay Free Recall (LDFR), and Long-Delay Cued Recall (LDCR). | ε4-carriers associated with long-delay verbal memory deficits (LDFR: B = −1.17 points, 95% CI (−2.33, −0.01), p = 0.049; LDCR: B = −1.58 (−2.63, −0.52), p = 0.004), and a marginal decrease on SDCR (B = −1.02 (−2.05, 0.00), p = 0.050). CT pathology was the strongest predictor of decreased verbal memory. |
| CTE in Athlete and Military Cohorts (4 Studies) | ||||||
| Author | Study Type | N | Sex; Age | Description | Outcome Measures | Results |
| Stern et al., 2013 | CTE, retrospective, athletes | 36 athletes (29 football (22 pro, 4 college, 3 high school), 3 hockey, 1 wrestling, 3 boxing (1 pro, 2 amateur)) with neuropathologically confirmed CTE | All male; aged 56.8 ± 21.9 years (range 17–98) | APOE-ε4 genotype distribution was 3% ε2/ε3, 63% ε3/ε3, 26% ε3/ε4, and 9% ε4/ε4 | Next-of-kin interviewed for neuropsychiatric, social/occupational histories, dementia, depression, changes in cognition, behavior, mood, motor function, and ADLs | Proportions of APOE genotypes (i.e., ε4/ε4, ε4 carriers, and ε4 noncarriers) in this CTE sample were significantly different from those found in an age-matched normative sample (p < 0.05). Primary difference between this CTE sample and population norms was a greater proportion of ε4/ε4 in this sample (p < 0.05). More ε4/ε4 in the cognition group than expected (p < 0.05). Relative proportions of APOE in the 10 subjects with dementia did not differ significantly from those seen in Alzheimer’s (p > 0.05) |
| Mckee et al., 2013 | CTE, retrospective, athletes, military veterans, and civilians | 80 athletes (22 veterans), 3 military veterans, 1 civilian with history of falls, 1 civilian with history of self-injurious head banging behavior; 18 age- and sex-matched controls | 84 males, 1 female; Mean age of 54.2 ± 23.3 years (age range 14–98) | Of all subjects, including controls, 21 were carriers of Apo-ε4, 5 were homozygous for Apo-ε4 | Post-mortem brains of subjects with histories of repetitive MTBI were analyzed for evidence of CTE. Hyperphosphorylated tau pathology ranged in severity from focal pathology in the frontal lobe to a more global tauopathy, allowing for a progressive staging of pathology in these subjects. APOE genotyping was performed | In the 68 subjects diagnosed with CTE, the proportion of carrying at least one APOE-ε4 allele was not significantly different than that observed in the general population (p = 0.334) |
| Omalu et al., 2011 | CTE, case series, athlete | 14 pro athletes (8 football, 4 wrestling, 1 boxing, 1 mixed martial arts, 3 high school football) | Subjects male; age range 16–52 years | ε3/ε3 in 6 athletes (60%), ε3/ε4 in 2 athletes (20%), ε2/ε3 in 1 athlete (10%), ε2/ε4 (10%) in 1 athlete. 9 of the pro athletes (90%) with at least 1 ε3 allele. 7 of 10 pro athletes with known APOE genotype had CTE (70%). For the 3 deceased high school football players, the APOE genotype in 1 case could not be determined (blood samples were not available), and the genotypes in the other 2 were ε3/ε3 and ε3/ε3 | Histochemical and immunohistochemical brain tissue analysis for CTE changes and apolipoprotein E genotyping | Three pro athletes carried APOE-ε4, two of which (ε3/ε4 genotype) were positive for CTE, and the remaining (ε2/ε4 genotype) negative for CTE |
| Omalu et al., 2011 | CTE, case report, military | Case report of a military individual | 27-year-old male | The APOE genotype was ε3/ε4 | Histochemical and immunohistochemical brain tissue analysis for CTE changes | Autopsy, as well as gross and histomorphological examination of this brain revealed CTE changes similar to those observed in USA athletes |
| CTE in an Institutionalized Cohort (1 Study) | ||||||
| Author | Study Type | N | Sex; Age | Description | Outcome Measures | Results |
| Shively et al., 2017 | Leucotomy, case series, institutionalized | 5 institutionalized patients with schizophrenia and history of surgical leucotomy, with post-diagnosis survival of >40 years | 2 male, 3 female; Ages were 67, 70, 77, 87, and 89 years | Three of 5 are APOE-ε4 carriers, with the other 2 having ε3/ε3 genotype | Immunohistochemistry for abnormally hyperphosphorylated tau, beta-amyloid, antigen CD68; H&E stains on tissue sections for general morphology/structure | The three ε4-carriers showed scattered β-amyloid plaques in the overlying gray matter, which were not seen in the two ε3/ε3 patients |
APOE: apolipoprotein E gene; CI: confidence interval; CT: computed tomography; LOC: loss of consciousness; MMSE: Mini Mental State Exam; OEF: Operation Enduring Freedom; OIF: Operation Iraqi Freedom; TBI: traumatic brain injury.