Mills’ syndrome is an idiopathic, slowly progressive, spastic hemiparesis. We describe three cases that have been under review for a minimum of 11 years (range 11–19). In all patients, symptoms started in a leg, with a mean age of onset of 59 years (range 53–63). The only abnormality on laboratory investigations was a mildly elevated CSF protein in one case. MRI demonstrated focal T2 hyper-intensity located eccentrically in the cervical cord ipsilateral to the symptomatic side. No cerebral abnormality was demonstrated. Whilst visual and somatosensory evoked potentials were unremarkable, motor evoked potentials were abnormal in all patients: central motor conduction times were significantly prolonged unilaterally in two patients and bilaterally but asymmetrically in the third. Beta-band (15–30 Hz) intermuscular coherence, a potentially more sensitive method of assessing upper motor neuron integrity, was absent unilaterally in one patient and bilaterally in the other two. One patient developed amyotrophy and thus a picture of amyotrophic lateral sclerosis after 16 years, suggesting that Mills’ syndrome is part of the motor neuron disease spectrum. Both amyotrophy and subclinical contralateral upper motor neuron disease can therefore be features of Mills’ syndrome. However, even with the most sensitive electrodiagnostic techniques, unilateral upper motor neuron disease can remain the only abnormality for as long as 10 years. We conclude that whilst Mills’ syndrome should be classified as a motor neuron disorder, it is a distinct nosological entity which can be distinguished from amyotrophic lateral sclerosis, upper motor neuron-dominant amyotrophic lateral sclerosis and primary lateral sclerosis. We propose diagnostic criteria for Mills’ syndrome, and estimate a point prevalence of at least 1.2:1,000,000 based on our well-defined referral population in the North of England.
Introduction
A case of idiopathic, slowly progressive, ascending, spastic hemiparesis was first described in 1900 by Charles Mills [21]. Post-mortem findings from a subsequent patient, who had been symptomatic for 8 years and died of tuberculosis, showed degeneration of the crossed and uncrossed pyramidal tracts originating from the left motor cortex, but no Betz cell degeneration within the left precentral gyrus or attrition of anterior horn cells [23]. By 1906, Mills had gathered a further seven cases of the syndrome, including one case where symptoms began in the arm, leading to the additional epithet ‘unilateral descending paralysis’ [22].
Mills’ assertion that the syndrome represents a separate clinical entity—distinct from amyotrophic lateral sclerosis (ALS), primary lateral sclerosis (PLS) and multiple sclerosis – has remained controversial [20]. Despite the limited investigations available at the time, two of the ten patients in Mills’ original case series received alternative diagnoses (neurosyphilis/taboparesis and multiple sclerosis), with one further case excluded by concomitant optic atrophy and cranial nerve palsies. Twenty-six cases of Mills’ syndrome have been reported since 1906, mostly as single case reports, but only 16 of these conformed to Mills’ original description of an idiopathic, isolated, progressive, spastic hemiparesis (Table 1). Of the remainder, two cases were diagnosed with ALS and a further two with multiple sclerosis [20], one evolved into PLS and also developed an extrapyramidal syndrome [33], one was attributed to lacunar infarcts [6], and two were ascribed to frontotemporal dementia/motor neuron disease [3, 8]. In two further cases, the presentation involved significant cognitive or neuropsychiatric abnormalities [10, 19].
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Table 1
Summary of published cases conforming to Mills’ original description of an idiopathic isolated progressive spastic hemiparesis
MRI head: atrophy of right cerebral peduncle and pontine base
MRI cervical spine: NAD
NAD
SEP: NR
VEP: NR
MEP: NR
3 years
No
# fracture, Auto-Ab auto-antibodies, bil. bilateral, C9ORF72 chromosome 9 open reading frame 72, CCF congestive cardiac failure, ↑CCT increased central conduction times, CoD cause of death, CST corticospinal tract, CVA cerebrovascular accident (stroke), Dipl. diplopia, Fib fibrillation potentials, FLAIR fluid attenuation inversion recovery, FP fasciculation potentials, FTD frontotemporal dementia, FU follow-up, FUS fused in sarcoma, GCN giant cutaneous naevus, HTLV human T-lymphotropic virus, L left, LL lower limb, n/a not applicable, NAD no abnormality detected, NoR no response, NR not reported, Nyst. nystagmus, OA optic atrophy, OCB oligoclonal bands, Park. Parkinsonism, PET positron emission tomography, PSW positive sharp waves, R right, SOD1 superoxide dismutase 1, SPECT single-photon emission computed tomography, SPEP serum protein electrophoresis, SVD small vessel disease, T4 thyroxine, TARDBP TAR DNA-binding protein, TSH thyroid stimulating hormone, WML white matter lesion, WBC white blood cells, UL upper limb, Vert. vertigo, WM Waldenström’s macroglobulinaemia, WML white matter lesion
aIncomplete information
Here we report three cases of a slowly progressive spastic hemiparesis consistent with Mills’ original description, with follow-up ranging from 10 to 18 years. Electrodiagnostic features and findings on MRI are described. We conclude that Mills’ syndrome, whilst part of the motor neuron disease spectrum, is a distinct nosological entity, and propose diagnostic criteria based on the published literature and our own observations. We also estimate the prevalence of this rare syndrome.
Materials and methods
Ethics statement
Most investigations were carried out as part of routine clinical care. Studies of motor cortical evoked potentials (MEP) and coherence were approved by the local NHS research ethics committee (approval number 08/H0908/3) and conformed to the Declaration of Helsinki. All participants provided written informed consent.
Nomenclature
We use the term motor neuron disease (MND) to refer to the disease entity, and the term ALS to describe the specific phenotype involving a combination of upper and lower motor neuron dysfunction in the limbs.
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Patients
Three patients conforming to Mills’ original description of idiopathic progressive spastic hemiparesis were identified from the regional motor neuron disorders clinic. The referral population of this clinic includes the counties of Tyne & Wear, Northumberland, Durham and Cumbria, and encompasses 2.43 million people according to 2011 census data [24].
Patient 1
A 57-year-old right-handed female presented with a 4-year history of right leg weakness with equinovarus, and a reduction in grip strength in the right hand. Weakness was such that she had to lift her right leg in and out of her car with her hands. The following year, she began to experience numbness in the right hand as well as low back pain and urinary urgency. A course of intravenous methylprednisolone provided no benefit. Her condition slowly progressed but remained unilateral after 18 years, with no evidence of bulbar dysfunction. There have been no persistent sensory symptoms, though she has complained of cold extremities and acrocyanosis.
The patient was an ex-smoker. Her only past medical history of note was of curative (local) treatment for ductal breast carcinoma (11 years after onset of neurological symptoms). There was no family history of neurological disease.
Physical examination (initial presentation)
The gait was spastic and hemiparetic, but ambulation was unaided. There was a pyramidal catch in the right upper limb and obvious spasticity in the right lower limb. Mild pyramidal weakness (Medical Research Council (MRC) grade 4) and hyperreflexia were noted in the right upper and lower limb.
Physical examination (10 years after presentation)
There was an asymmetrical spastic paraparesis, worse on the right, and requiring a frame to ambulate. There were early flexion contractures of the fingers in the right hand with marked hypertonia in the right upper and lower limbs. Pyramidal weakness was noted in the right upper (MRC grade 4 proximally and grade 3 distally) and lower limb (MRC grade 3). Pathological hyperreflexia was now also evident in the left lower limb, but the left plantar response was flexor whereas the right was extensor.
Physical examination (12 years after presentation)
The patient had begun using a wheelchair after fracturing the right radius and ulna in a fall, and had been catheterised due to impaired mobility. She had evolved significant amyotrophy in the right hand and forearm.
Patient 2
In this right-handed female, left leg pain and weakness first became apparent at the age of 63. Her symptoms progressed; after 6 years she could no longer work and she began experiencing pain and weakness in the left arm. After a further 2 years she noted an unsteady gait and difficulty walking, as well as some urinary urgency. There was very little subjective progression in the subsequent 4 years.
Three years after onset, she developed vertigo and was diagnosed with left vestibular failure, and 1 year later she suffered a sixth nerve palsy, which subsequently resolved. Pregabalin effectively controlled pain in her left arm and leg. There was no relevant family history.
Physical examination (4 and 8 years after presentation)
The gait was unsteady and broad-based. There was subtle weakness of the left upper limb (MRC grade 4 +) and the left hand was clumsy, with more obvious pyramidal weakness in the left lower limb (MRC grade 4). Tendon reflexes were symmetrically brisk throughout, with bilateral flexor plantar responses. There was hyperalgesia and allodynia in the left upper and lower limbs. No amyotrophy or fasciculation was evident.
Patient 3
This right-handed retired male noticed progressive weakness in the right leg at age 60, 2 months after a low velocity road traffic accident. Over the next 3 years, his exercise tolerance reduced to half a mile with a stick, and he developed some urinary urgency and difficulty in using cutlery because of weakness in his right hand.
His past medical history was remarkable only for gout, for which he took allopurinol. There was no pertinent family history.
Physical examination (5 years after presentation)
During ambulation there was circumduction of the right lower limb with mild right equinovarus. There was pyramidal weakness in the right upper (MRC grade 4) and lower limb (MRC grade 4 proximally, grade 2 distally). Tendon reflexes were pathologically brisk on the right, with an extensor plantar response on that side.
Physical examination (10 years after presentation)
The weakness in the right upper and lower limb had increased, but there was no amyotrophy or fasciculation. Results of investigations are summarised in Tables 2 and 3. MRI scans before 2012 were performed on a 1.5 T system. Subsequent MRI scans were acquired using a 3 T system. None of the patients were treated with riluzole.
Table 2
Laboratory investigations
Biochemistry
Haematology
Immunology
Virology
CSF
Patient 1
U&E NAD
Ca2+/P/ALP NAD
TSH/T4 NAD
CK NAD
CRP < 5 mg/l
Cholesterol 4.2 mmol/l
FBC NAD
Clotting NAD
ESR 2 mm/h
B12 305 ng/l (170–700)
SPEP NAD
Auto-Ab NAD
–
Protein 0.41 g/l (< 0.4)
WBC 1/mm3
OCB absent
Patient 2
U&E NAD
Ca2+/P/ALP NAD
TSH/T4 NAD
CK NAD
CRP < 5 mg/l
Cholesterol 4.2 mmol/l
FBC NAD
Clotting NAD
ESR 2 mm/h
–
–
Protein 0.29 g/l (< 0.4)
WBC < 1/mm3
OCB absent
Patient 3
U&E NAD
Ca2+/P/ALP NAD
TSH/T4 NAD
CK NAD
CRP < 5 mg/l
Cholesterol 5.3 mmol/l
FBC NAD
Clotting NAD
APA NAD
ESR 2 mm/h
B12 225 ng/l (170–700)
SPEP NAD
Auto-Ab NAD
HIV 1 + 2 (-)
Protein 0.7 g/l (< 0.4)
WBC < 1/mm3
OCB matched
ALP alkaline phosphatase, APA antiphospholipid antibodies, Auto-Ab auto-antibodies (extractable nuclear antibodies, nuclear antibodies, rheumatoid factor, gastric parietal cell antibodies, mitochondrial antibodies), Ca2+ calcium, CK creatine kinase, CRP C-reactive protein, ESR erythrocyte sedimentation rate, FBC full blood count, NAD no abnormality detected, P phosphate, SPEP serum protein electrophoresis, TSH thyroid stimulating hormone, T4 thyroxine, U&E urea and electrolytes, WBC white blood cells
Table 3
Neurophysiological findings
Sex
Age at onset (years)
NCS/EMG
SEP
VEP
MEP
Beta-band IMC
Time since onset (years)
Result
Time since onset (years)
Result
Time since onset (years)
Result
Time since onset (years)
Result
Time since onset (years)
Result
Patient 1
F
53
4
NAD
14
NAD
14
NAD
14
R UL/LL + L UL: ↑CMCT (L LL: NT)
14
L UL: absent (R UL/LL: NT as unable to perform task)
5
NAD
14
NAD
16
Fib/PSW R FDI/APB/EDC
FP R FDI/ADM/APB/EDC
Patient 2
F
63
6
NAD
10
NAD
10
NAD
9
L UL/LL: ↑CMCT
R UL/LL: NAD
9
L UL/LL: absent
R UL/LL: NAD
10
NAD
Patient 3
M
60
3
Fib R FDI
PSW R TA
Mild neurogenic R UL/LL
3
NAD
3
NAD
6
R UL/LL: ↑CMCT
L LL: NAD (L UL: NT)
6
R UL/LL: absent
L LL: absent (L UL: NT as unable to perform task)
4
Fib R FDI
PSW R TA
Mild neurogenic R UL/LL
5
Mild chronic neurogenic R UL
No Fib/PSW
6
Mild chronic neurogenic R UL
No Fib/PSW
ADM abductor digiti minimi, APB abductor pollicis brevis, ↑CMCT increased central motor conduction times, EDC extensor digitorum communis, FDI first dorsal interosseous, Fib fibrillation potentials, FP fasciculation potentials, IMC intermuscular coherence, L left, NAD no abnormality detected, NT not tested, PSW positive sharp waves, R right, TA tibialis anterior
Neurophysiology
Evoked potentials
For somatosensory and visual evoked potentials (SEP, VEP), results were compared to local normative data. For MEP, results were compared to a previously published normative dataset [9].
Intermuscular (EMG–EMG) coherence
Coherence was estimated from electromyography (EMG) recordings performed during a precision grip task (upper limb) or a foot rocking task (lower limb). For the upper limb, coherence spectra were calculated between extensor digitorum communis (EDC) and first dorsal interosseous (FDI), as well as between flexor digitorum superficialis (FDS) and FDI; for the lower limb, they were computed between medial gastrocnemius (MG) and extensor digitorum brevis (EDB), and between tibialis anterior (TA) and EDB. Detailed methods were published previously [12, 16].
Literature review
We searched Scopus, Ovid and Pubmed for publications on “Mills syndrome” in English or German, and reviewed the reference lists of the papers retrieved. Publications in other languages, including a French series of three patients with Mills’ syndrome [17], were therefore not included in the review.
Results
Table 2 summarises the results of laboratory investigations. In one patient, the CSF showed a mildly elevated protein level and matched oligoclonal bands; serum and urinary protein electrophoresis was normal. All remaining results, including CSF parameters in the other two patients, were unremarkable.
MRI brain was unremarkable in all cases. Findings for MRI of the cervical spine are illustrated in Fig. 1. In all three patients, sagittal and axial T2 weighted images returned hyper-intense signals from the lateral corticospinal tract at the cervical level, ipsilateral to the symptomatically weak limbs. In patient 1, the T2 hyper-intensity was in the left lateral aspect of the cervical cord at the C3 to C5 vertebral levels (Fig. 1a, b). In patient 2, the focal T2 hyper-intensity involved the left lateral aspect of the cord at C3/4 levels (Fig. 1c, d). In patient 3, the hyper-intensity involved the right anterolateral aspect of the cord at the C1/2 level (Fig. 1e, f). All three cases demonstrated signal abnormality involving the cervical cord, which was eccentric in location and involved more than one vertebral level in length.
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The results of neurophysiological investigations are summarised in Table 3. Patient 1 did not show any abnormalities on nerve conduction studies (NCS) and EMG until 16 years after symptom onset. Those abnormalities included profuse fibrillation potentials, positive sharp waves and fasciculation potentials, together with unstable neurogenic voluntary motor unit action potentials in forearm and intrinsic hand muscles of the right upper limb, consistent with possible ALS according to Airlie House/Awaji criteria. Patient 2 exhibited no abnormality on NCS/EMG over a period of 12 years. Patient 3 showed evidence of mild neurogenic change with evidence of spontaneous activity in an intrinsic hand muscle and lower limb muscles 3 and 4 years after onset, but when examined subsequently only mild chronic neurogenic changes were found without evidence of progression.
VEP and SEP were normal but MEP were abnormal in all patients. In patients 2 and 3, MEP were only abnormal in the symptomatic limbs, whilst patient 1 also showed abnormal MEP in the asymptomatic left upper limb (Fig. 2).
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We also measured intermuscular coherence (Fig. 3). In patients 1 and 2, the limbs with absent coherence matched those with abnormal MEP. Interestingly, there was no significant coherence in any of the muscle pairs tested in patient 3, including in the left lower limb which was asymptomatic, normal on examination, and had shown normal MEP.
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Discussion
Here we present one of the largest, most clinically homogeneous case series of idiopathic, slowly progressive, ascending hemiparesis since Mills’ original description [21]. Unlike most of the previously published case reports (Table 1), the cohort of patients included in this series came from a single geographically defined referral population. Patients underwent prolonged follow-up with repeated clinical investigations, including MRI and clinical neurophysiology. Only one of our patients progressed to a syndrome compatible with ALS. As a consequence, we have been able to better define this clinical entity.
Only 23 cases of ‘pure’ Mills’ syndrome (if one excludes cases in which alternative diagnoses were confirmed or are likely) have been reported in the English or German language literature (Table 1) [3, 6, 8, 10, 19, 20, 22, 33], with an average length of follow-up of 16 years (range 1.5–35 years). Clinical features in our case series are consistent with those described previously, and mean follow-up was similar at 13 years (range 10–18). Combining data from our series with the 23 previously published cases (total n = 26), the mean age of onset was 44 (range 6–68), mean follow-up was 11 years (range 1.5–35), the M:F ratio was 13:11 and symptoms started in one leg in two-thirds of cases.
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Two of our patients complained of urinary urgency (patient 1 and 3). This has only been reported in one previous case [14]. Patient 1 also complained of acrocyanosis and patient 2 of mild pain in the affected limb. Sensory symptoms, including limb pain, were described in the original series [22] and acrocyanosis was reported in a separate case, though the latter was attributed to multiple lacunar infarcts [6]. Patient 1 developed amyotrophy and thus an ALS-like phenotype after 16 years, highlighting the spectral nature of motor neuron disorders. This contrasts with a previous case where unilateral amyotrophy developed gradually alongside spasticity over 12 years before presentation [27]; in a further case, unilateral atrophy was noted at presentation, 10 years after symptom onset [11]. No amyotrophy was reported for the remaining past cases. Whilst mild but noticeable amyotrophy can occur as a consequence of disuse, particularly in a disease running a protracted course, the extent of amyotrophy in patient 1 was greater than could be ascribed to this.
Patient 3 noticed symptoms a few weeks after recovering from a low velocity road traffic accident. A similar temporal relationship to trauma was noted in a previous case report, in which paresis began developing soon after the patient had sustained open fractures of the same limb [28]. For MND, a potential link with preceding trauma has long been an area of controversy. Whilst some studies have reported a significantly elevated risk for at least 1 year after significant head or limb trauma [5, 32], given the known delays between presymptomatic disease onset, weakness and ultimately diagnosis, an aetiopathogenic role for trauma in MND seems biologically implausible [1]. Instead this association is more likely to reflect a greater risk of falls in incipient MND. We consider it likely that the association between Mills’ syndrome and trauma is also coincidental.
An important diagnosis to consider in an evolving hemiparesis, paraparesis or tetraparesis is the central demyelinating disorders including multiple sclerosis. Notably, in our case series, there was no evidence of these on CSF studies, VEP or SEP.
Whilst acute demyelination is distinguishable from gliosis on MRI T2 or FLAIR sequences because of oedema (and enhancement with contrast), the chronic changes of demyelination are not. In multiple sclerosis, demyelinating lesions, particularly those within the spinal cord, do not typically respect anatomical boundaries, have indistinct borders (for example, see axial MRI sections from patients 2–4 in the figure published in [29]) and are confined to one vertebral segment [4]. By contrast, the MRI signal changes observed in our cohort were confined strictly to the lateral funiculus, with defined, demarcated borders, and extended for two or more vertebral segments on sagittal images. This latter feature is atypical for multiple sclerosis (or solitary sclerosis) and therefore suggests alternative aetiologies including Wallerian degeneration and gliosis [2].
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Electrophysiological examination is important in helping to define alternative progressive upper motor neuron syndromes [15, 26]. A complete set of NCS, needle EMG and evoked potentials was reported for only two of the reviewed previous cases [13, 33] but is provided for all cases presented here. Whilst needle EMG, SEP and VEP are important in excluding other diagnoses, MEP can confirm the presence of corticospinal tract disease. MEP have been reported in three previous cases [28, 30, 33] and showed unilaterally prolonged central motor conduction times and—in one case—borderline central motor conduction times in the contralateral lower limb. In our cohort, abnormalities in central motor conduction times were also unilateral, except in patient 1, where MEP were also delayed in the asymptomatic contralateral upper limb when tested 14 years after onset (Fig. 2; Table 3).
It has been suggested that intermuscular coherence analysis is more sensitive than MEP in detecting corticospinal tract dysfunction [12]. Intermuscular coherence is mediated by an efferent–afferent feedback loop and thus depends on the integrity of both the corticospinal tract and afferent pathways [35]. All patients who were able to perform the coherence task on the (most) affected side had abnormal coherence on that side, which could only be attributed to disease in the corticospinal tract because sensory NCS and SEP were normal. Patient 1 had abnormal coherence in the asymptomatic upper limb, consistent with the results of MEP. In patient 3, the upper limbs exhibited unilaterally abnormal MEP but bilaterally abnormal coherence. This suggests the presence of subclinical corticospinal tract disease on the clinically unaffected side, and supports the notion that intermuscular coherence is more sensitive than MEP in detecting corticospinal tract disease.
Similar to patient 1, some past cases exhibited upper motor neuron signs contralateral to the side of onset [14, 27], and post-mortem histology, which was performed in two previous cases, demonstrated bilateral degeneration of the corticospinal tract [11, 23]. Together with the electrophysiological evidence of bilateral corticospinal tract involvement, these features might be viewed as consistent with PLS. However, if diagnostic criteria for PLS [26] are strictly applied these require symmetry at presentation (or within 4 years) and permit pseudobulbar palsy as a first presentation, which has never been described in Mills’ syndrome. Betz cells in the precentral gyrus are absent or reduced in PLS but are preserved in Mills’ syndrome, thus further supporting the notion that Mills’ syndrome is a distinct entity. The absence of positivity for TAR DNA-binding protein 43 in a recent case also distinguishes Mills’ syndrome from MND [11].
Our proposed diagnostic algorithm for Mills’ syndrome, encompassing features based on previously published criteria for PLS [26], upper motor neuron-dominant ALS [15] and ALS [7], is outlined in Fig. 4. If our criteria are satisfied, based on our experience and review of the literature, a number of statements can be made with regard to prognosis. First, no patient with the condition has yet died directly from Mills’ syndrome. Second, the shortest delay between symptom onset and the appearance of features typical of ALS is 12 years and the longest follow-up without evidence of progression to ALS is 26 years to date. Finally, disability accumulates slowly. In our cohort, only one patient became dependent on a wheelchair after 14 years of symptoms.
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Our referral population encompasses 2.43 million people, according to 2011 census data [24], leading to a point estimate of 1.2:1,000,000 for the prevalence of Mills’ syndrome. This is likely to be an underestimate, mainly because patients with Mills’ syndrome in primary or secondary care are more likely to receive alternative, more common diagnoses such as stroke. However, we hope that the provision of clear diagnostic criteria will improve case ascertainment and allow more accurate prevalence estimates in the future.
Acknowledgements
This research was supported by grants from the Wellcome Trust (grant number WT089893MA, SRJ) and the National Institute for Health Research (Grant number ACLNEUR03, MRB). The authors would like to thank the patients who participated in this study.
Compliance with ethical standards
Conflicts of interest
On behalf of all authors, the corresponding author states that there is no conflict of interest.
Ethical standards
Most investigations were carried out as part of routine clinical care. Studies of motor cortical evoked potentials (MEP) and coherence were approved by the local NHS research ethics committee (approval number 08/H0908/3) and conformed to the Declaration of Helsinki.
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