Abstract
Objective: To characterize prospectively the cognitive profile in ALS.
Methods: Clinically definite ALS patients (11 men, 2 women), age 39.9 to 74.0 years (mean age, 54.2 ± 9.6 years; mean disease duration, 21.1 ± 10.5 months) underwent neuropsychologic, language, and speech testing followed by MR 1H spectroscopy (4 T). Five spousal control subjects completed an identical protocol. Eight ALS patients participated in follow-up studies at a 6-month interval.
Results: Relative to control subjects, ALS patients showed mild impairment in word generation, recognition memory (faces), and motor-free visual perception. Bulbar-onset patients showed greater impairment in a number of measures (working memory, problem solving/cognitive flexibility, visual perception, and recognition memory for words and faces), and cognitive impairment appeared more progressive over time. ALS patients demonstrated anomia on a confrontation naming test, with no significant problems following commands or repeating. Speech motor performance scores and intelligibility scores were not significantly different. No significant declines in forced vital capacity, forced expiratory volume, or peak expiratory flow rates were observed. Although normal at initial testing (T1), MR 1H spectroscopy demonstrated a reduction of the N-acetylaspartate/creatine (NAA/Cr) ratio in the nondominant precentral motor strip across the two testing intervals. In contrast, the NAA/Cr ratio obtained from the anterior cingulate gyrus at T1 was already reduced in bulbar-onset patients (p < 0.001), whereas no deficits were observed in limb-onset individuals in the same region.
Conclusions: Bulbar-onset ALS patients with cognitive impairments and neuronal loss in the anterior cingulate gyrus subsequently developed more profound neuropsychological dysfunction whereas both language and speech capabilities remained relatively preserved. Of note, the absence of bulbar signs did not predict an absence of cognitive decline.
Traditionally, ALS is considered to be largely restricted to motor neurons. The clinical or neuropathologic involvement of nonmotor systems has been held to be extremely rare or restricted to specific variants of the disease.1 However, the contemporary view of ALS now encompasses a more widespread disorder in which motor neurons are selectively vulnerable but in which nonmotor involvement can also be observed readily.2,3 The occurrence of cognitive impairment in ALS is one such nonmotor phenomenon.
Although the clinical characterization of impairments of cognition in ALS remains to be defined in its entirety, it is best categorized as a frontotemporal dementia.4 The actual frequency of cognitive impairment in ALS is unknown. When encountered, the features are an insidiously progressive behavioral disorder with affective symptoms, impairments of verbal fluency, word-finding difficulties, lexical disorganization, and reliance on stereotypic utterances.5 We report a prospective analysis of the earliest clinical manifestations of impaired cognition in ALS.
Methods.
Patient selection.
Patients were recruited from the Motor Neuron Diseases Clinic at the University of Western Ontario using a convenience sampling technique. All patients conformed to the diagnosis of clinically definite ALS (El Escorial criteria).6 Inclusion criteria included an age of older than 35 years, English as the primary language, the absence of previous neurologic conditions (e.g., head injury, stroke), and the use of amitriptyline. All ALS patients but one were right handed. All control subjects were right handed. Thirteen patients with ALS (11 men, 2 women), age 40 to 74 years at the time of symptom onset (mean, 54.2 ± 9.6 years) with a mean disease duration of 21.1 ± 10.5 months at initial testing (T1), participated in the study. Eight ALS patients had limb onset of the disease whereas five had bulbar onset. Five spousal control subjects also participated in all aspects of the study except for pulmonary function testing and MRS. When possible, a second test (T2) was performed 6 months after the initial assessment. All testing paradigms were performed on the same day, with the neuropsychological testing completed first to avoid excess fatigue. Pulmonary function testing was performed on the day of assessment for each ALS patient.
Neuropsychological evaluation.
Both the patients and control subjects completed a 2-hour standardized battery of neuropsychological tests at T1 and T2. Tests were chosen to minimize the requirements of speech production and manual motor movement; to be reliable, valid, and sensitive; and to allow for an adequate range of performance. The panel of tests offered breadth in that most major realms of cognition were assessed. Not all patients completed all tests. For example, if motor deficits were apparent, a patient received the oral version and not the written version of the word fluency task. All raw test scores were compared with age- and education-corrected normative data, and were converted into standard z scores with a mean of 0 and an SD of 1. Only descriptive statistics were performed due to the small and uneven sample sizes. Group means less than −1.0 SDs were considered impaired for the purposes of this exploratory study. Similarly, difference scores greater than 1.0 SD were considered meaningful differences.
Tests utilized in the neuropsychological assessment included 1) executive skills: Wisconsin Card Sorting Test (WCST; one-deck version; perseverative responses [WCSTpr], total errors [WCSTterr]), Controlled Oral Word Association (number of words, CFL), and Thurstone Written Word Fluency (number of words [SWords]); 2) concentration/working memory: Consonant Trigrams Test (ConTrig; mean across three trials); 3) memory: Rey Auditory Verbal Learning Test (total across five trials, delayed recall), Recognition Memory Test (RMT; total number of words recalled [RMTWords], total number of faces recalled ]RMTFaces]); 4) visual–perceptual and visual–constructional skill: Motor Free Visual Perception Test (MFVPT; total correct), Block Design Test (Wechsler Adult Intelligence Scale–revised age-scaled score); and 5) mood/personality functioning: Geriatric Depression Scale (GDS; number of items endorsed) and the Neuropsychiatric Inventory (NPI, total score).
Language assessment.
ALS and control subjects completed tests of language and discourse at T1 and T2 (table 17-11). Written responses on the standardized language tests and the discourse tasks were collected and analyzed from subjects whose spoken language was unintelligible.
Language tests and discourse protocol
The standardized language tests comprise a comprehensive set of expressive and receptive measures that reflect linguistic processes thought to be affected by cognitive impairment. Language samples were collected according to the standardized protocol of the “cookie theft” picture description subtest from the Boston Diagnostic Aphasia Examination.9 Discourse samples were collected according to the protocol for topic-directed interviews (TDIs), based on Ripich and Terrell12 in their analyses of the discourse of subjects with AD and other neurogenic disorders.11 The TDIs were initiated using the starter phrase “Tell me about ___________” and included the following five topics: 1) your family, 2) where you were born and raised, 3) your health right now, 4) the jobs you had or the work you did, and 5) what you do each day. Different interviewers collected the TDI data at T1 and T2 to eliminate the effect of shared background knowledge.
All raw test scores were converted to z scores. Student’s t-tests were used to compare the z scores of the language subtest raw scores between ALS patients and control subjects at T1 and T2. Intragroup comparisons also were made between T1 and T2 using paired t-tests. t-Tests also were completed for comparisons of the z scores between bulbar and nonbulbar patients, bulbar patients and control subjects, and limb-onset patients and control subjects. Intragroup comparisons were made for the bulbar and nonbulbar groups between T1 and T2. The alpha level was set at p < 0.10, with familywise corrections made because of the multiple comparisons.
Speech motor control assessment.
Stimulus materials were chosen to describe three levels of speech production—namely, respiratory–laryngeal, resonatory, and oral articulatory. The items included sustained maximum phonation time (MPT), sound repetitions (diadochokinesis [DDK]), and speech intelligibility. These word stimulus items (Word Intelligibility Test [WIT]) were produced once by each subject at each assessment period, with the order and sequence randomized.13 All speech data were tape recorded and analyzed acoustically via special computerized speech analysis software,14 or were analyzed perceptually (WIT) by a panel of listeners. Averages and variability scores were calculated. Initial statistical analyses comparing ALS patients as a group with control subjects were completed employing independent t-tests at the T1 and T2 assessment periods. Subsequently, statistical analyses examined the performance of bulbar- and limb-onset ALS subgroups over time.
MR spectroscopy.
Patients were studied in a Varian (Palo Alto, CA)/Siemens (Erlangen, Germany) Unity Inova 4-T whole-body research scanner. A quadrature radio frequency (RF) coil of our own design was used for transmission and reception.15 The patient’s head was placed in a Plexiglas holder and was packed in firmly using foam to minimize motion. The RF coil was slid over the holder. Global shimming was performed on the whole head, using first- and second-order shims. Proton spectra (1H) were acquired using a single-voxel short echo time STEAM spectrum (echo time, 20 msec; modulation time, 30 msec; repetition time, 1.5 sec; 256 averages) in each of the anterior cingulate and the right primary motor cortex. The voxel size was 3 mL, and the shim was touched up using the first-order shims in each of the two areas. Water line widths of 8 Hz were typical. Voxels were localized by using a three-dimensional T1-weighted anatomic image, as we did previously.16 Unsuppressed water spectra were also acquired for quantification and spectral referencing. The total study lasted less than 1 hour.
The N-acetylaspartate (NAA) and creatine (Cr) peaks were quantified using Lorentzian line shapes with a peak-fitting algorithm supplied by Varian. Both frequency and line width were allowed to vary. The spectral baseline was flat and required no postprocessing. The reported ratios are ± SE, derived from the variances for each of the three groups, classified by location.
Results.
Clinical characteristics.
Thirteen ALS patients (11 men, 2 women) were studied at T1. Eight patients completed the neuropsychology, language, and speech assessments at T2, but only six of these eight patients completed the second MRS study due to sialorrhea or an inability to tolerate recumbency. Three patients died before T2 could be undertaken and one patient withdrew from the study after T1.
The mean age at onset at the time of the first symptom was 54.2 ± 9.6 years (range, 39.9 to 74.0 years). Eleven cases were sporadic and two were familial (in the absence of a known family history of dementia or cognitive impairment). At T1, the mean disease duration from symptom onset was 21.1 ± 10.5 months, with the second assessment occurring after a mean interval of 5.8 ± 0.3 months. ALS patients and control subjects did not differ in age (± 0.28 years, p = 0.78) or years of education (± 0.71 years, p = 0.49). Pulmonary functions demonstrated the patients to be early in the course of their disease state, with no significant impairments observed on measures of forced vital capacity, forced expiratory volume, and peak expiratory flow rates at either T1 or T2. Two of the eight patients could not perform pulmonary function tests at T2 due to physical limitations.
Neuropsychological results.
Intragroup comparisons across testing sessions.
As shown in table 2, no major changes (i.e., >1.0 SD) on any cognitive measures were noted over time for the ALS patients. ALS patient performance declined slightly on five variables (negative difference scores) and improved slightly on six variables (positive difference scores). The only variable on which ALS patients performed in the impaired range was SWords. This impaired score was evident during both testing sessions. Neuropsychiatric symptoms measured by the NPI in the ALS group as reported by spouses increased over time, although none of the ALS patients was depressed as measured by the GDS. Symptoms on the NPI varied widely among patients, ranging from no discernible symptoms to obvious symptoms in the areas of agitation, anxiety, delusions, disinhibition, apathy/indifference, and irritability/liability. In contrast, the control group performed within normal limits across all measures. Significant improvement (i.e., >1.0 SD) across time was noted on RMTFaces. Slight improvements were noted on seven other variables, and performance declined slightly on three variables for the control group.
Neuropsychological results: group means (ALS patients and control subjects) and difference scores (z scores)
Intergroup comparisons within testing sessions.
At T1, ALS patients performed overall less well across tests (mildly impaired to high-average range) compared with control subjects, whose performance ranged from the low-average to superior range. Table 2 reveals that ALS patients performed worse than control subjects on only one measure at T1: MFVPT. However, intergroup comparisons at T2 indicate many more cognitive differences. ALS patients performed more than 1 SD below control subjects on four measures: CFL, SWords, RMTFaces, and MFVPT.
Bulbar-onset versus limb-onset ALS patients.
Separate examination of the bulbar-onset and limb-onset groups revealed that the bulbar patients showed cognitive impairment (i.e., z scores less than −1.0 SD) across more measures. Although both groups showed impaired SWords at T1, the bulbar-onset group was also impaired on ConTrig and RMTFaces. At T2, the gap between groups increased farther. The limb-onset group was again impaired only on SWords whereas the bulbar-onset group was impaired on five variables: SWords, ConTrig, RMTFaces, WCSTpr, and WCSTterr.
The bulbar- and limb-onset ALS groups were compared with each other and the control subjects at T1 and T2. The only significant difference observed at T1 was poorer performance on MFVPT by the bulbar-onset group when compared with the control subjects. However, by T2, many significantly different scores were noted. Compared with control subjects, both the bulbar- and limb-onset groups performed more poorly on CFL, SWords, and RMTFaces. However, the bulbar-onset group also performed more poorly than control subjects on ConTrig, WCSTpr, WCSTterr, and MFVPT. Lastly, when the bulbar- and limb-onset groups were compared directly, the bulbar group performed more poorly across several variables, including ConTrig, WCSTpr, WCSTterr, MFVPT, RMTWords, and RMTFaces.
Language.
Four ALS patients provided written responses on language tests and the discourse tasks at T1. Two patients provided written responses at T2—one who wrote at T1 and one who spoke at T1. The two significant differences in language performance between the ALS and control subjects at T1 and T2 consisted of significantly poorer confrontation naming among the ALS subjects at T1 (t[13] = −3.12, p = 0.008) and poorer single-word vocabulary comprehension (Peabody Picture Vocabulary Test–III [PPVT-III]; t[16] = −2.28, p < 0.05). An analysis of naming errors shows that the ALS patients produced verbal paraphasias (e.g., “yell” for target word “funnel”) and semantic paraphasias (e.g., “nut” for target word “acorn”). ALS patients produced significantly fewer self-corrective utterances than control subjects at T2 on the discourse tasks (t[10] = −2.63, p < 0.05). There were no significant changes in language over time for the following subgroup comparisons: ALS (all patients) versus control subjects, bulbar versus nonbulbar patients, bulbar versus control subjects, and nonbulbar versus control subjects. There were no significant differences over time for the bulbar and the nonbulbar patients.
Speech.
Independent t-tests of MPT revealed that as a group, ALS patients did not differ significantly from the control subjects at T1 (t[15] = −1.14, p = 0.13) and at T2 (t[10] = −0.80, p = 0.28). Paired t-tests used to compare ALS patient MPT at T1 and T2 did not yield significant differences between the two periods (t[(6] = −0.42, p = 0.69). Independent t-tests at T1 and T2 showed no significant speech production differences between the bulbar- and limb-onset groups.
When MPT duration for the production of the sustained vowel /a/ was analyzed between values obtained at T1 and T2, there was a decrease in MPT values for three limb-onset patients and the one bulbar-onset patient. Three limb-onset patients showed an increase in MPT at the 6-month follow-up. However, none of these changes were found to be significant using Wilcoxon’s matched-pairs signed rank test (T = 6, p = 0.05).
DDK was compared between the ALS patients and the control subjects at both T1 and T2 using an independent t-test. The results indicated significantly slower rates of repetition of “puh” (t[12.82] = −4.52, p = 0.001), “tuh” (t[12.03] = −4.20, p = 0.001), “kuh” (t[11.80] = −4.19, p = 0.001), and “puh-tuh-kuh” (t[15] = −2.84, p = 0.013) for the ALS group than the control subjects at T1. Similarly, at T2, ALS patients as a group produced significantly slower DDK rates than control subjects for “puh” (t[10] = −2.38, p = 0.039), “tuh” (t[10] = −2.61, p = 0.026), “kuh” (t[10] = −2.71, p = 0.002), and “puh-tuh-kuh” (t[10] = −3.20, p = 0.010).
No significant differences were found between the bulbar- and the limb-onset groups at T1 on any of the repetition tasks. However, both the bulbar- and the limb-onset groups demonstrated slower DDK rates than the control subjects. Similarly, at T2, both ALS subgroups were lower in articulatory repetition rates than the control subjects.
All patients were judged to be more than 90% intelligible at T1. Wilcoxon’s matched-pairs signed rank test did not yield significant changes in mean percent intelligibility scores over time (T = 6, p = 0.05).
MR spectroscopy.
As illustrated in table 3, at T1 MRS demonstrated a significant neuronal loss in both the anterior cingulate gyrus and the motor strip of the bulbar-onset group of patients as reflected by reductions in the NAA/Cr ratio. Although limb-onset patients failed to demonstrate significant neuronal losses at T1, at T2 neuronal loss was evident in the motor region. No bulbar-onset patients were able to complete T2 MRS due to difficulties with sialorrhea.
MRS results (NAA/Cr ratios; mean ± SE)
Discussion.
Although cognitive impairments consistent with frontotemporal impairment have been documented in ALS, the current study is the first attempt to follow patients with ALS over time with regard to their cognitive functioning using a multimodal, multidisciplinary approach.17 We observed that cognitive impairment is a frequent occurrence early in the disease process and is associated with a loss of neurons of the anterior cingulate gyrus as measured by MRS.
The neuropsychological results indicate that as a group our ALS patients scored in the impaired range (compared with normative data) on tests of written word fluency at both T1 and T2. Relative to control subjects, our ALS patients performed more poorly on only one measure at T1—MFVPT. However, by T2, the ALS patients demonstrated at least mild impairment relative to control subjects in oral and written word generation, recognition memory (faces), and motor-free visual perception. Bulbar-onset patients showed greater impairment than limb-onset patients at both time points across several domains of function including working memory, problem-solving/cognitive flexibility, episodic memory (recognition memory for words and faces), and visual–perceptual skill. Cognitive impairment in the bulbar-onset group but not the limb-onset group appeared to progress over time, involving more cognitive skills at T2 compared with T1.
As a group, ALS patients were not depressed at either T1 or T2. Patient neuropsychiatric profiles differed widely, ranging from no symptoms to obvious changes in the areas of delusions, agitation, anxiety, disinhibition, apathy/indifference, and irritability/lability. Neuropsychiatric symptoms in the ALS group as reported by their spouses increased over the two testing sessions.
The neuropsychological results are generally consistent with previous studies of cognitive function in ALS that have documented deficits in frontal functions such as mental flexibility, verbal and nonverbal fluency, and abstract reasoning18; in memory for verbal and visual (pictorial) material18-20; and in performance on the WCST.20 In addition, our observations of deficits in word fluency, working memory, and problem-solving ability, along with the neuropsychiatric changes, are consistent with a frontotemporal localization. These results are also in keeping with the neurocognitive deficits observed in other frontotemporal dementias, including Pick’s disease and frontal lobe degeneration.21 Somewhat less expected in the current study were the difficulties shown by ALS patients on some nonverbal measures involving visual–perceptual ability. However, as indicated in the Zakzanis study,21 this type of deficit may be secondary to frontal-executive dysfunction.
We also found that our ALS patients were significantly poorer at T1 on confrontation naming of pictures than were control subjects only at T1. Previous studies that examined the profile of cognitive impairment in patients with ALS have identified anomia as a prominent feature.22,23 Stereotypic words and phrases, phonemic and semantic paraphasias, impaired confrontation naming, and poor word and letter fluency characterized the anomia of our ALS patients.
No significant differences were observed between the ALS patients and control subjects over time on any of the naming or language measures. This is unexpected given previous research that identified potential areas of reduced language performance in ALS patients with suspected cognitive impairment. However, the lack of significant differences is not entirely surprising given the heterogeneity of language performance among our ALS patients. Moreover, the lack of differences may be due to the small sample of ALS patients, especially at T2, when fewer ALS patients completed the language assessment.
When compared with control subjects, ALS patients performed more poorly on MPT tasks at both assessment periods, although differences in MPT did not reach significance. The observation that the limb-onset subjects showed overall numerically higher MPT values at both assessment sessions is consistent with the expected pattern that the bulbar group would demonstrate greater respiratory–laryngeal impairment. Although the bulbar patients did not show significant decline over time, most of the original bulbar patients were only assessed once because of mortality. When both testing periods are assessed, a moderate decline in respiratory–phonatory function is observed. This finding compares favorably with previous reports.24
Although as a group our ALS patients did show slower DDK rates than the control subjects, measures of DDK rates also failed to differentiate bulbar- and limb-onset patients.25 No significant decreases in repetition rates were noted in either ALS subgroup over time. Mean speech intelligibility measures were also not different statistically over time. Of the bulbar- and limb-onset patients who completed both assessment sessions, only two limb-onset and one bulbar-onset patient demonstrated notable reductions in speech intelligibility. As with the other measures (MPT, DDK), the small number of patients within and across assessment sessions precluded meaningful analysis of results. Arguably, measures of DDK and speech intelligibility could be considered assessment tools sensitive enough to detect the onset of bulbarlike symptoms in subjects otherwise diagnosed clinically with primarily limb involvement.26
Our results suggest that the earliest manifestations of cognitive impairment in ALS can be detected by the appearance of difficulties on tests of word fluency, visual perceptual ability, and confrontation naming, in the absence of significant impairments in oromotor function. A bulbar-onset patient may be more vulnerable to cognitive impairments. Progression over time is marked, in our selected group of patients, by greater degrees of cognitive impairment, with less deterioration in language, speech, or respiratory parameters. Thus, it is of considerable interest that reductions in the NAA/CR ratio of the anterior cingulate gyrus in bulbar patients are evident early in the course of cognitive impairment, and that these reductions correlate with the appearance of impaired cognition. Whether prospective studies of this region will serve as a predictor of the development of impaired cognition remains to be determined. However, it is known that MRS is a sensitive measure of early neuronal loss in ALS.27,28 Furthermore, our observations suggest that an early, significant loss of neurons of the anterior cingulate gyrus occurs in ALS, and that this occurs in association with the induction of cognitive impairment.
- Received February 12, 1999.
- Accepted June 14, 1999.
References
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