Calabria as a Genetic Isolate: A Model for the Study of Neurodegenerative Diseases
Abstract
:1. Introduction
2. Neurodegenerative Diseases, Issues, and Study Methodologies
3. Calabria as a Genetic Isolate for Neurodegenerative Diseases
3.1. Alzheimer’s Disease
3.2. Frontotemporal Dementia
3.3. Parkinson’s Disease
3.4. Niemann–Pick Type C Disease
3.5. Spinocerebellar Ataxia Type 17
4. Discussion
5. Conclusions
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
References
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Neurodegenerative Disease | Mutation or Variant | Patient(s) | Clinical Features | Neuroimaging/Neuropathology | Reference |
---|---|---|---|---|---|
Alzheimer’s Disease | PSEN1 I143V | Female proband of a four-generation family with history of dementia (11 subjects: 5 females, 6 males). Two more subjects were reported as affected by depression. | Onset at 55 years with personality changes, apathy, reduction of verbal fluency, and temporal and spatial disorientation. At 68, appearance of visual hallucinations, slurred speech, and rigidity. She became bedridden and died at 75. | The brain showed severe atrophy of the frontal and temporal lobes. Parenchymal amyloid-β (Aβ) deposits were abundant, diffuse grey structures, and contained Aβ42, but very little Aβ40. Amyloid angiopathy was absent. Neurofibrillary changes were severe. | [25] |
PSEN1 M84V | Three patients belonging to a large kindred affected by ADAD (14 over three generations). | Early-onset (mean age = 52.7 years), frontal executive syndrome, psychosis and spastic paraparesis. | Diffuse cortical and cerebellar atrophy. | [26] | |
PSEN1 E318G and PSEN2 Val139Met | One patient affected by late-onset familial AD. The father had died at about 80 years old with a picture of dementia clinically resembling that of the proband, and two sisters had died at 83 and 74 years old, both showing a progressive picture of dementia starting with memory impairment, cognitive deficits, time and space disorientation, and agitation evolving into a severe state of dementia. | Proband was 76 years old when he presented with memory and language deficits. Symptoms progressed very slowly together with episodes of spatial disorientation; he frequently showed mistakes in identifying relatives and friends and became temporally disoriented and unable to perform activities of daily living. Irritability and agitation were noticed by relatives, but only when the behavioral disorder worsened did the family ask for a neurological consultation, five years after the onset. Neurological examination was performed and found normal when the patient was 83; he exhibited moderate temporal and spatial disorientation, showing a selective and moderate impairment of verbal long-term memory and of abstract thinking. At 86, he showed dysphasic and incomprehensible speech, was unable to recognize children, and unable to walk alone. He was still alive but bedridden. | Bilateral hypoperfusion at the parietal–temporal lobes more marked in the right hemisphere. | [27] | |
PSEN2 Ser130Leu | One male patient with a familial history of two first-degree relatives with a PD without cognitive impairment. | Late-onset AD. At 81 years old, his wife noted progressive memory impairment and episodes of spatial disorientation while driving. His mood and personality changed. He started to shun social contact, losing interest in friends and in leisure activities; he developed delusions. On examination, the patient was depressed, apathetic, and evidenced moderate impairment of cognition. Neurological examination was normal. Six months later, the patient showed worsened memory functions. He rapidly developed language deficits, agitation, delusion, and hallucinations. One year later, the patient was amnesic, agnosic, aphasic, and showed mild bradykinesia. | Mild temporal atrophy without vascular lesions. | [28] | |
APP A713T * | PEC family (21 subjects: 13 males, 8 females) over the last three generations were identified as at risk or affected by dementia; 8 persons were reported to be affected by dementia through history (5 males, 3 females), and 5 were studied clinically and genetically (5 males); 8 asymptomatic at-risk subjects (3 males, 5 females) were also clinically and genetically investigated. Another two patients were identified in northern Italy and in the Walloon region of Belgium. All subjects shared a common ancestor who lived in Calabria 1000 years ago. | Early- or late-onset AD with severe cerebral amyloid angiopathy (CAA) and cerebrovascular lesions (CVLs), both in heterozygosis and in homozygosis. | Severe atrophy in parietotemporal cortices or frontoparietotemporal cortices and cerebrovascular lesions in the cortex with frontoparietotemporal hypoperfusion. | [12,29,30,31] | |
Frontotemporal dementia | GRN c.1145insA, A266P, and C126W | Twelve carriers of the c.1145insA, three carriers of the A266P, belonging and segregating in two different branches of the same large kindred (B-family). Two apparently sporadic patients, also of Bivongi, descending from a common founder identified in the sixth generation. | A difference in the age at onset was evident among the three groups (c.1145insA carriers (64.2 ± 12.5 years); A266P carriers (75.7 ± 2.9 years); C126W carriers (71 ± 8.5 years)). Three distinct FTD phenotypes correlated to each GRN mutation. Carriers of c.1145insA showed a more severe “frontal Gestalt” with marked distractibility, disinhibition, a greater impairment of social awareness, and language impairment developing into complete mutism (behavioral type). A266P carriers showed affective symptoms with apathy in 100% of cases, emotional unconcern, and verbal output reduction that remained stable for the entire course of the disease (affective type), while C126W carriers presented with paranoid delusions and agitation (delirious type). | Data not shown. | [10] |
GRN Cys139Arg | One male patient. The sister, deceased at age 70, was reportedly affected by a similar clinical picture of dementia. | At age 61, the patient presented with slow progressive personality changes and behavioral disturbances. He was playful and moriatic, unaware of his changes, and also displayed an alteration in eating behavior and motor stereotypes. He became unable to drive. Within 3 years indifference, apathy, and reduction of verbal fluency appeared; memory functions in contrast were relatively preserved. At age 69, the patient was mute, incontinent, and completely dependent on others for care. However, there was no evidence of any clinical motor impairment. | Not available. | [32] | |
Three patients coming from Calabria (patient CI2), Tuscany (patient TM1), and Lazio (patient LT3). CI2 had a family history of dementia and parkinsonism; TM1 had a family history of psychiatric disorders but not of dementia; LT3 had nine siblings, four of whom were affected by dementia without available DNA and blood samples. | The patients presented with different clinical pictures (TM1, bvFTD; CI2, semantic dementia, SD; and LT3, corticobasal degeneration, CBS) and showed a wide range of age at onset (55–80 years old), which confirmed the heterogeneity of clinical phenotypes associated with this mutation. | CI2: atrophy and hypometabolism of the left temporopolar and temporoparietal areas. TM1: cortical frontal atrophy associated with subcortical white matter abnormalities and hypometabolism in the bilateral parietotemporal and left frontal dorsolateral areas. LT3: marked atrophy of both frontal and temporal anterior lobes, asymmetric for left side, and a reduced perfusion in superior and medial frontal gyri and in temporoparietal areas. | [33] | ||
MAPT Val75Ala and PSEN2 Arg62His # | Two siblings; a male carrying the MAPT Val75Ala mutation and a female carrying the PSEN2 Arg62His mutation. Their mother presented with a mood disorder; their father died at 66 years from myocardial infarction; two more brothers were healthy. A paternal aunt and the paternal grandmother were affected by AD and PD, respectively. | The clinical picture shown by the affected subjects was consistent with early-onset FTD. Both siblings presented with a similar behavioral pattern of dementia characterized by insidious onset, disinhibition, loss of social awareness, and absence of insight. Impairment of executive functions evidenced involvement of the frontal lobe together with phonological verbal fluency which was severely impaired in both patients. They also shared perseveration and utilization behavior that are typical signs of frontal involvement. Memory functions were compromised at different levels due to the different stages of the disease; constructional apraxia was relatively spared in both. The patients were unaware of their pervasive changes. Both patients showed myoclonus and developed epileptic seizures. Through molecular analysis, we excluded other dementing disorders featuring myoclonus and epilepsy, such as familial AD and CJD. | The male patient showed a frontotemporal atrophy and frontomesial and frontoparietal left hypoperfusion. Theta and delta activities were present at the EEG in frontotemporal areas. The female patient showed a moderate cortical and subcortical atrophy and a marked hypoperfusion in frontal lobes prevalent on the left hemisphere. EEG showed diffuse slow waves. | [34] | |
MAPT V363I | One female proband of a three-generation family with four other subjects who were carriers of the same mutation asymptomatically. However, only the proband was homozygous for the A allele of PGRN SNP rs9897526 and for methionine at 129 codon of the PRNP gene, suggesting that the genotype of some modifier dementia genes might contribute to the pathogenic effect of the MAPT V363I variation. | The proband was 53 years old when, after an infectious episode, she began to manifest visual hallucinations and progressive personality changes. She became disinhibited with inappropriate jocularity; she touched everything and everyone and stopped people in the street to say that she was seeing angels. Insight was absent. She danced all day, listened to music, drew on the walls, and refused cooking and home management. In contrast with an excessive use of make-up, she neglected personal hygiene. She became totally unable to work and began treatment with haloperidol. Apathy, emotional blunting, reduction of verbal initiative, early incontinence, and inability to perform daily living activities appeared. No improvement arose when the treatment was stopped. At the age of 56 years, the patient was excessively smiling, echolalic, answered only simple questions, sang old songs, but continued to dress correctly. She was untestable; both pyramidal and supraspinal signs were present. Although symptoms gradually progressed to complete mutism and hyperorality, she continued to manage known environments. The patient was clinically diagnosed with FTD. Within 3 years, the patient became amimic, showing myoclonus, and presenting with massive flexor rigidity of the neck and both arms; walking became impossible. She died at the age of 61 years. | Massive cortical and subcortical atrophy. | [35] | |
MAPT IVS9 − 15T > C and IVS10 + 4A > C | One female proband. The IVS10 + 4A > C mutation was present in the proband’s mother and in four maternal uncles. The IVS915T > C mutation was present in the proband’s father and one of her sisters, while only one sister had both mutations and showed slight verbal memory disturbances together with mild deficit in attention and concentration. Both the proband and her sister with both mutations were heterozygous for MAPT H1/H2; APOE genotypes were, respectively, ε2/ε3 and ε3/ε3, and the M129V polymorphism of the PRNP gene was MM in the proband and VV in her sister. | The proband shown presenile dementia with a clinical picture characterized by apathy, depression, and absence of insight, followed by pyramidal and extrapyramidal signs consistent with FTD. | Autopsy of the proband’s brain revealed a massive and selective atrophy of the frontal and temporal lobes, severe atrophy of the caudate nucleus and of the white matter; the hippocampus was destroyed. An exceptional neuronal loss in all layers of the frontotemporal and insular cortices with intense protoplasmatic gliosis were present. Abundant neurofibrillary tangles and Pick body-like inclusions in neurons, tufted astrocytes, and coiled bodies in oligodendrocytes, consistent with an increased expression of 3R tau. | [36] | |
PRNP P39L | Patient 1: male with four other family members affected by behavioral disturbances and cognitive impairment suggestive of FTD. Patient 2: Male with no family history suggestive of dementia, although his mother was referred to as an irritable and willful person. She was impulsive and bossy like the patient and in the later years of her life showed signs of hand tremor. | Both patients shared a frontal dementia dominated by a dysexecutive syndrome and severe behavioral disturbances, whereas psychotic signs such as delusions or hallucinations were absent. Neither patient developed any of the typical clinical signs associated with prion diseases, such as myoclonus or cerebellar ataxia. | Patient 1: Cortical atrophy with a marked involvement of mesial, frontal, temporal, and posterior parietal regions in the left side, besides some lacunar ischemic subcortical lesions. Hypoperfusion of frontotemporoparietal cortical areas with relative sparing of the occipital lobe, brainstem, and cerebellum. EEG did not show any typical periodic complexes of prion diseases. Patient 2: Diffuse cortical atrophy prominent in mesial frontal, temporal, and posterior parietal regions, mainly in the left side. EMG and EEG were normal. | [37] | |
PSEN1 Val412Ile | FUS family of four affected subjects in two generations. | The patients shared a similar clinical picture, which included behavioral disorder and deficits on neuropsychological tests, fulfilling the clinical criteria for FTD, despite the AD expected phenotype caused by PSEN1 mutations. | Two patients presented diffuse cortical hypometabolism; the other two were unavailable for neuroradiological examinations. | [32] | |
VCP D395A | Three siblings (two sisters; one brother) with a possible family history of dementia (the father died in a psychiatric hospital at 60 years old). | Early-onset behavioral variant of FTD without inclusion body myopathy (IBM) and Paget’s disease of bone (PDB), unlike many reports on VCP disease. | Patient 1: diffuse cortical atrophy prominent in frontal and temporal regions and hypoperfusion in frontal and temporal convolutions of the left hemisphere and upper frontal circumvolution of the right hemisphere. Patient 2: diffuse cortical atrophy prominent in the frontal lobes and bilateral frontoparietotemporal hypoperfusion. Patient 3: diffuse cortical atrophy and bilateral frontoparietotemporal hypoperfusion. | [38] | |
Parkinson’s disease | LRRK2 p.Phe1227Leu | One female patient with family occurrence of Parkinson’s disease. | Onset at 65 years with bradykinesia. The patient also developed tremor at rest and rigidity accompanied by depression. | Data not shown. | |
LRRK2 p.Gly1520Ala | One male patient with family occurrence of Parkinson’s disease. | Onset at 68 years with bradykinesia and freezing of gait. The patient also developed tremor at rest, postural tremor, rigidity, and postural instability. | Data not shown. | [11] | |
LRRK2 p.Ile2020Ser | One male patient without family occurrence of Parkinson’s disease. | Onset at 51 years with bradykinesia. The patient also developed tremor at rest, rigidity, dyskinesias, and postural instability, accompanied by depression. | Data not shown. | ||
Niemann–Pick type C Disease+ | NPC1 p. F284LfsX26 | One female patient with a family history of late-onset dementia. | The 68-year-old patient, with moderate congenital mental retardation and poor acquisition of language and judgment abilities, was affected by a progressive supranuclear palsy-like syndrome. The NPC-SI score was 116 indicating high suspicion of NPC. The onset was at 64 years, with speech, gait impairment, and postural limb tremor. In the following years, she developed progressive cognitive deterioration with prominent executive dysfunction and behavioral disturbances. She also showed loss of autonomous ambulation, anarthria, severe dysphagia, global bradykinesia with small-step gait, freezing, and postural instability, vertical gaze palsy, fixed oral and cranium–cervical dystonia with anterocollis, right focal limb dystonia, axial and right limb cogwheel rigidity, and ideomotor apraxia. Severe dementia was detected with apathy, sleep disturbances, and irritability. The patient also presented steatosis, hepatomegaly, and moderate cholesterol accumulation compatible with a variant biochemical phenotype. Plasma levels of cholestane-3β,5α,6β-triol were normal. | Severe midbrain atrophy (“hummingbird sign”) and marked cortical atrophy with reduced striatal uptakes in the left putamen. | [14] |
NPC1 c.1947 + 8G > C | One female patient with family history of depression. | Patient was a 62-year-old with mild mental retardation, affected by corticobasal syndrome. The NPC-SI score was 97 indicating high suspicion of NPC. Onset at 32 years with depressive symptoms, evolving into apathy, emotional lability, and short-term memory impairment at 41 years. Both “absence-like” seizures and gelastic cataplexy with sudden weakness associated with strong emotions, particularly laughter, occurred. At 56 years, the patient appeared emotionally flat and apathetic, with moriatic and imitative behaviors, wandering, binge eating, and craving for sweets. She had insight of her symptoms, but she was emotionally indifferent and quite theatrical in reporting them. She became careless and incurred an ocular injury with a mishandled pen, losing sight in her right eye. In subsequent years, she developed frontal dementia, showing impaired abstract reasoning, attention, and awareness, as well as anomia and dressing apraxia. Clinical examination detected mild gait impairment and left limb hemidystonia associated with pyramidal syndrome, ideomotor apraxia, echolalia, and mirror movements. Vertical gaze was normal. Neuropsychological evaluation confirmed a prominent impairment of executive functions, abstract reasoning, and judgment abilities associated with environmental dependency. Abdominal echotomography showed slight hepatomegaly. Filipin staining was negative and plasmatic levels of cholestane-3α,5β,6α-triol were normal. | Severe frontal, parietal, and occipital cortical atrophy, mainly in the right side, and atrophy of the left temporal lobe and diffuse cortical hypoperfusion, mainly in the left temporoparietal region. | ||
NPC2 p.V30M | One female patient without family history of NPC. | Patient was 52 years old and affected by corticobasal syndrome. The NPC-SI score was 132 indicating high suspicion for NPC. Onset at 39 years with pain in the left shoulder and hand clumsiness that led to a reduced ability to perform housework. After three years, the patient showed planning and executive deficits and difficulties in word finding. She developed motor slowing and gait disturbances and was unresponsive to L-DOPA. Personality changed with apathy, fatuous and childish behavior, and emotional incontinence. By the age of 50 years, we observed progressive worsening of gait and the patient was constrained to a wheelchair, in addition to exhibiting speech disorder, dysphagia, severe frontal dementia, and visual hallucinations. Concurrently, she presented with myoclonic jerks, generalized epileptic seizures, and REM sleep behavior disorder. At first clinical examination, the patient showed a severe akinetic–rigid syndrome associated with gait apraxia and freezing, dysarthria and speech apraxia, vertical gaze palsy and oculomotor apraxia, focal limb, and trunk dystonia. Non-fluent aphasia and ideomotor apraxia were also detected. Filipin staining was inconclusive, showing a few cells with weak fluorescent perinuclear vesicles. Plasmatic levels of cholestane 3α,5β,6α-triol were normal. | Severe atrophy of the right frontal and parietal lobes and moderate atrophy of the cerebellar hemispheres and severe hypometabolism of the occipital and parietal cortical areas with a reduced striatal uptake in the right putamen. | ||
NPC2 c.441 + 1G > A | One male patient with a family history of cognitive impairment, psychiatric symptoms, and substance addiction. | A 70-year-old patient affected by corticobasal syndrome. The NPC-SI score was 111 indicating high suspicion of NPC. Onset at 61 years, with difficulties in word finding, personality changes, and inability to drive. At 67 years, he was incapable of oral expression and writing and experienced difficulties in using and recognizing common objects. Daily activities were progressively abandoned because of both impaired action planning and disrupted awareness of positions and spatial relationships of objects in the environment. Memory was not compromised. Nocturnal myoclonus was reported. At 68 years, visual hallucinations, confabulation, and delusions. Simultaneously, he developed an extrapyramidal syndrome with gait impairment, action tremor, and rigidity as well as global disuse of the right limbs, without improvement on withdrawal of antipsychotic drugs. Clinical examination at age 67 showed vertical gaze palsy, non-fluent aphasia, speech apraxia, ideomotor oculomotor and orofacial apraxia, and postural limb tremor. After three years, additions to the neurological picture included anarthria and right asymmetric akinetic–rigid parkinsonism with gait apraxia, dystonia, and myoclonic jerks of the right limbs. Cognitive evaluation confirmed non-fluent aphasia, agraphia, constructive apraxia, disorientation, and executive dysfunction. Behavioral assessment revealed persistent hallucinations, delusions, apathy, lability and agitation, anxiety, and wandering. Filipin staining revealed moderate intracellular cholesterol accumulation compatible with a “variant biochemical phenotype”. Plasma levels of cholestane-3α,5β,6α-triol showed normal values. | Cortical atrophy of the frontal and parietal areas and the left temporal lobe with asymmetrical cortical hypoperfusion in the left posterior associative areas. | ||
Spinocerebellar Ataxia Type 17 | TBP CAG/CAA repeat expansion | Sixteen individuals affected (four men and twelve women) across five generations of a large kindred. | Initial presenile frontal-type dementia with behavioral symptoms, ataxia, rigidity, and dystonic movements. | Global atrophy of the cerebral and cerebellar cortices. The main neuropathological characteristics of the autopsied case were a low brain weight, atrophy of the frontotemporal cortex, nerve cell loss in the precentral gyrus, the primary visual cortex, the striatum, and the thalamic dorsomedial nucleus, pseudohypertrophic degeneration of the inferior olive, and severe loss of Purkinje cells. | [13] |
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Bruno, F.; Laganà, V.; Di Lorenzo, R.; Bruni, A.C.; Maletta, R. Calabria as a Genetic Isolate: A Model for the Study of Neurodegenerative Diseases. Biomedicines 2022, 10, 2288. https://doi.org/10.3390/biomedicines10092288
Bruno F, Laganà V, Di Lorenzo R, Bruni AC, Maletta R. Calabria as a Genetic Isolate: A Model for the Study of Neurodegenerative Diseases. Biomedicines. 2022; 10(9):2288. https://doi.org/10.3390/biomedicines10092288
Chicago/Turabian StyleBruno, Francesco, Valentina Laganà, Raffaele Di Lorenzo, Amalia C. Bruni, and Raffaele Maletta. 2022. "Calabria as a Genetic Isolate: A Model for the Study of Neurodegenerative Diseases" Biomedicines 10, no. 9: 2288. https://doi.org/10.3390/biomedicines10092288
APA StyleBruno, F., Laganà, V., Di Lorenzo, R., Bruni, A. C., & Maletta, R. (2022). Calabria as a Genetic Isolate: A Model for the Study of Neurodegenerative Diseases. Biomedicines, 10(9), 2288. https://doi.org/10.3390/biomedicines10092288