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Article

APP, PSEN1, and PSEN2 Mutations in Asian Patients with Early-Onset Alzheimer Disease

by
Vo Van Giau
1,
Eva Bagyinszky
1,
Young Chul Youn
2,
Seong Soo A. An
3,* and
SangYun Kim
4,*
1
Graduate School of Environment Department of Industrial and Environmental Engineering, Gachon University, 1342 Sungnam-daero, Sujung-gu, Seongnam-si, Gyeonggi-do 461-701, Korea
2
Department of Neurology, College of Medicine, Chung-Ang University, Seoul 06973, Korea
3
Department of BionanoTechnology, Gachon Medical Research Institute, Gachon University, 1342 Sungnam-daero, Sujung-gu, Seongnam-si, Gyeonggi-do 461-701, Korea
4
Department of Neurology, Seoul National University College of Medicine & Neurocognitive Behavior Center, Seoul National University Bundang Hospital, 300 Gumidong, Bundang-gu, Seongnam-si, Gyeonggi-do 463-707, Korea
*
Authors to whom correspondence should be addressed.
Int. J. Mol. Sci. 2019, 20(19), 4757; https://doi.org/10.3390/ijms20194757
Submission received: 28 August 2019 / Revised: 12 September 2019 / Accepted: 23 September 2019 / Published: 25 September 2019
(This article belongs to the Special Issue Molecular Genetic of Alzheimer's Disease)
Browse Figures
Versions Notes

Abstract

:
The number of patients with Alzheimer’s disease (AD) is rapidly increasing in Asia. Mutations in the amyloid protein precursor (APP), presenilin-1 (PSEN1), and presenilin-2 (PSEN2) genes can cause autosomal dominant forms of early-onset AD (EOAD). Although these genes have been extensively studied, variant classification remains a challenge, highlighting the need to colligate mutations across populations. In this study, we performed a genetic screening for mutations in the APP, PSEN1, and PSEN2 genes in 200 clinically diagnosed EOAD patients across four Asian countries, including Thailand, Malaysia, the Philippines, and Korea, between 2009 and 2018. Thirty-two (16%) patients presented pathogenic APP, PSEN1, or PSEN2 variants; eight (25%), 19 (59%), and five (16%) of the 32 patients presented APP, PSEN1, and PSEN2 variants, respectively. Among the 21 novel and known non-synonymous variants, five APP variants were found in Korean patients and one APP variant was identified in a Thai patient with EOAD. Nine, two, and one PSEN1 mutation was found in a Korean patient, Malaysian siblings, and a Thai patient, respectively. Unlike PSEN1 mutations, PSEN2 mutations were rare in patients with EOAD; only three variants were found in Korean patients with EOAD. Comparison of AD-causative point mutations in Asian countries; our findings explained only a small fraction of patients, leaving approximately 84% (p = 0.01) of autosomal dominant pedigrees genetically unexplained. We suggest that the use of high-throughput sequencing technologies for EOAD patients can potentially improve our understanding of the molecular mechanisms of AD.

1. Introduction

Alzheimer’s disease (AD) is one of the most common neurodegenerative disorders, which accounts for up to 75% of all dementia cases [1,2]. AD can be categorized into two major types: Early-onset AD (EOAD) and late-onset AD (LOAD). EOAD is usually inherited autosomal dominantly, and occurs before the age of 60–65 years. Presenilin-1 (PSEN1; MIM #104311) [3], presenilin-2 (PSEN2; MIM #600759) [4], and amyloid protein precursor (APP; MIM #104760) gene mutations [5,6] and duplications [7] can cause autosomal-dominant EOAD. Mutations in these genes have been relatively rarely observed [8,9,10,11,12], since the prevalence is estimated to be 5.3 per 100,000 individuals [13]. The significance of APP, PSEN1, and PSEN2 in AD were confirmed by different genetic studies, and majority of these mutations share a common feature of exhibiting increased production of the Aβ1-42 peptide, associated with altered gamma secretase activity [5,14]. Among these three genes, PSEN1 mutations were more frequently observed in AD, since approximately 252 different mutations were reported (http://www.alzforum.org/mutations, accessed in June 2019). Mutations in APP and PSEN2 were less frequently observed, since only 35 pathogenic APP mutations and 20 pathogenic PSEN2 mutations have been reported (http://www.alzforum.org/mutations, accessed in June 2019).
Despite the fact that genomic sequencing and bioinformatics have dramatically improved the identification of other genetic risk factors over the last few years, the interpretation of rare variants remains a challenge [1,2,8,10,15,16]. Remarkably, the age of onset and disease progression is not only influenced by genetics, but also by both lifestyle and environmental factors [17,18,19,20,21]. These factors may cause altered gene expression by epigenetic modifications, thereby affecting AD pathology [1,17,19,22]. Although majority of these mutations of these three genes are associated with familial EOAD, follow the Mendelian rules, several de novo cases of AD have been reported in patients without any family history of dementia [10,23].
The fastest increase in the number of elderly individuals has been observed in the East Asian countries. Approximately 60% of all patients diagnosed with dementia inhabit the Asian countries [24]. However, the genetics of EOAD are not well characterized, since only a few reports are available regarding mutations in EOAD causative genes (Figure 1) [25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44]. Therefore, the aim of the present study was to report mutations in additional cases, including sporadic ones, since our last update from 2009 for Asian patients with EOAD. We performed a genetic screening for mutations in the PSEN1, PSEN2, and APP genes in 200 patients with EOAD.

2. Results

2.1. Identified Gene Mutations of APP

Considering that the genetic background of EOAD in the Asian population is not well characterized [10,15], we reported non-synonymous mutations in 200 clinically diagnosed patients with EOAD across four Asian countries, including Thailand, Malaysia, the Philippines, and Korea between 2009 and 2018. A total of 32 mutation carriers, including affected relatives in EOAD families and sporadic cases, were found among the 200 patients. From the 21 novel and known non-synonymous variants, five APP variants were found in Korean patients, and one APP variant was identified in a Thai patient. Nine, two, and one PSEN1 variant was identified in Korean patients, Malaysian siblings, and a Thai patient, respectively. Unlike PSEN1 mutations, PSEN2 mutations were a rare in EOAD, with only three variants identified in Korean patients (Table 1). Moreover, the mutation spectrum associated with AD for all Asian countries is shown in Table 2 [29,31,32,45,46,47,48,49,50,51,52,53].
Six novel APP mutations were found in six out of 200 EOAD patients (Table 1). A novel mutation, c.2005G > C, p.(Val669Leu) substitution, present in a 56-year-old Korean female and two of her daughters [67]. The clinical features were typical of AD with aggravated diffuse brain atrophy and a small vessel ischemic lesion. The c.1810C > T, p.(Val604Met) mutation was found in a Thai patient with EOAD [12]. The patient was diagnosed in 2013 with AD presenting logopenic aphasia, and this variant appeared to be associated with the phenotype [12]. Three APP variants—c.674T > C (p.Val225Ala); c.1450C > T, (p.Pro484Ser); and c.890C > T, (p.Thr297Met)—were found in Korean patients with EOAD at an onset age between 60 and 65 years. Although these three variants have not been previously reported in the literature, their allele frequencies in the ExAC database are 0.00002471, 0.00003304, and 0.0002062, respectively. Only one novel APP mutation—c.1810C > T p.(Val604Met)—was identified during this screen in a Thai patient with EOAD; this mutation is presumed to be associated with altered APP function due to increased hydrophobicity of methionine in the helix [12]. Over 35 APP variants have been discovered in exons 16 and 17; of them, 10 have been reported in Asia (Table 2, Figure 2a). Remarkably, a novel mutation in the APP gene, Val669Leu, was discovered in a Korean female patient with AD [67]. She developed cognitive decline at the age of 56 years, and MRI scans showed mild global atrophy with medial temporal lobe predominance and hippocampal atrophy. The patient may have a positive history of the disease, since her mother was also diagnosed. APP V669L was predicted as the non-damaging variant by the PolyPhen2 and Sorting Intolerant From Tolerant (SIFT) tools. APP mutations are rare in Korean populations because of the presence of only one mutation in APP, V715M (V715M). APP V669L is located near the β-secretase cleavage site, adjacent to the Swedish APP (KM670/671NL) mutation (Figure 2b) [68]. This mutation may disrupt amyloid-beta metabolism.

2.2. Identified Gene Mutations of PSEN1

Twelve PSEN1 mutations were identified in 20 patients with EOAD (Table 1). Remarkably, a previously reported PSEN1 mutation—Val96Phe—was identified in two siblings from Malaysia. This mutation was reported previously in a Japanese family with disease onset in the late 40s or 50s [32]. Similar to Japanese patients, the disease onset in these siblings was in the 40s, and they presented symptomatic changes in behavior and personality, such as apathy and withdrawal. In addition, seven additional novel or known PSEN1 mutations, including Thr116Ile, Thr119Ile His163Pro, Leu226Phe, Gly209Ala, Leu232Pro [69], and Gly417Ala [11], have been identified in Korean patients with AD. Importantly, even though PSEN1 is the most commonly involved gene, with > 231 mutations reported as pathogenic in the Alzforum database (www.alzforum.org/mutations), this study did not find any PSEN1 mutation in the Thai and Philippine cohorts. Moreover, only three Malaysian patients with AD have been identified to carry a novel mutation, Glu280Lys [70]. As Korea is one of the fastest “aging countries” in the world, the number of AD, including EOAD, patients will rapidly increase [24]. The carriers of PSEN1 mutation presented with isolated and progressive cognitive decline. Another patient carrying the PSEN1 p.Gly417Ala substitution also exhibited an atypical presentation: Cerebellar ataxia and extra pyramidal with pessimism syndrome. According to the Alzheimer’s Research Forum database, more than 230 PSEN1 variants have been identified worldwide (www.alzforum.org/mutations). Among them, > 55 variants have been identified in Japan, Korea, the People’s Republic of China, Malaysia, and Thailand (Figure 3).

2.3. Identified Gene Mutations of PSEN2

We also discovered the following three PSEN2 mutations in Korean patients for the first time: Arg62Cys, His169Asn [9], and Val214Leu. Arg62Cys (CGC TGC) was discovered in the Asian population for the first time by our research group. The mutation was identified in a patient with dementia. Memory impairment, personality change, and disorientation appeared at the age of 49 years. Val214Leu was one of the first PSEN2 mutations identified in an Asian population. In addition, it is the first mutation identified in the TM-IV region of PSEN2. Val214Leu mutation was identified in the following two unrelated patients: A 70-year-old patient with AD-type dementia and a 56-year-old patient with memory impairment. The exact family history is unknown for both patients. A pathogenic mutation p.His169Asn in the PSEN2 gene in a Korean patient with EOAD has also been identified [9]. PolyPhen-2 and SIFT software analyses predicted this mutation to be a probable damaging variant. The mutation was identified in a 58-year-old woman who was presented with progressive memory decline in her 50s. The patient had an apolipoprotein E genotype (APOE) ε 3/3 polymorphism. The family history of the proband generations was negative for any neurological disease, indicative of a de novo case of AD. All living family members declined genetic testing. Interestingly, PSEN2 p.His169Asn mutation was previously identified in one patient with familial LOAD and one patient with sporadic frontotemporal dementia (FTD) from People’s Republic of China [40]; however, the pathogenic nature has not been clarified yet. Compared with the two Chinese patients, the Korean patient showed similar clinical manifestation with the proband with frontal variant AD. Although no additional mutation was reported at residue 169 of the PSEN2 protein, the p.His169Asn mutation was found in the conserved TM-III region of PSEN2, containing the pathogenic variants (p.M174V and p.S175C), based on the algorithms to predict the pathogenicity of the mutations described by Guerreiro et al. [71] More than 40 missense and frameshift mutations in the PSEN2 gene have been reported so far; however, until 2019, no pathogenic mutation has been found in PSEN2 in any Asian country. The findings of this study as well as those of recent studies revealed novel and known PSEN2 variants in Korean and Chinese patients (Figure 4).

3. Discussion

In this study, we performed genetic screening for mutations in the APP, PSEN1, and PSEN2 genes in 200 clinically diagnosed EOAD patients across four Asian countries, including Thailand, Malaysia, the Philippines, and Korea from 2009 to 2018, and identified 21 novel and known missense mutations. According to Guerreiro’s algorithm [71], pathogenicity was considered as “definite” for two APP, “probable” for nine PSEN1, and “possible” for three PSEN2 mutations. The pathological effect of the known mutations deserves discussion because of incomplete penetrance, nonpathogenicity, or a wide range of age onset [41,47,52,56,57,58,59,60,61,63,64,65].
This study detected six mutations in APP, among patients under 65 years of age. Among them, only one APP, the Val669Leu mutation, was located in the amyloid processing area. The patient with APP Val669Leu presented had a progressive short-term memory impairment, as observed in typical AD. However, atypical symptoms of AD, including focal signs and symptoms, were also observed. Frontal lobe impairment (depression, apathy, and disinhibition), epileptic seizures, and myoclonus were also observed. As APP is responsible for the disease it is located relatively near to the beta secretase cleavage site; therefore, Val669Leu may interfere with the normal proteolytic processing of APP. This mechanism is thought to involve alternative proteolytic processing pathways [5,6,7,47,72].
PSEN1 c.286G > T, p.(Val96Phe) substitution was identified in two siblings from Malaysia. This was the second report of the PSEN1 Val96Phe mutation among EOAD patients in Asia. Patients presented similar phenotypes like the previously described Japanese patients: The disease onset was in their 40s, and they presented a symptomatic change in behavior and personality, such as apathy and withdrawal. PSEN1 Val96Phe mutation is considered pathogenic and can lead to an increase in Aβ42 level and Aβ42/Aβ40 ratio in cell cultures [32]. These findings suggest that mutations in TM-I may be responsible for pathogenic mutations in EOAD. Cellular studies with different mutations (including Val96Phe) suggest that TM-I plays a significant role in APP trafficking and amyloid peptide cleavage. Therefore, we speculate about an underestimation of its frequency. In addition, two PSEN1 mutations—Trp165Cys [73] and p.Ala285Val—were identified in a 53-year-old male who presented memory decline, followed by disorientation, and in a 46-year-old woman who presented with progressive memory dysfunction, respectively. Both patients had probable EOAD, and the family history was positive in them. Both mutations were previously shown to have increased Aβ42 and decreased Aβ40 levels. Moreover, both mutations could elevate the Aβ42/Aβ40 ratio by impairing the gamma secretase functions [49,59,72,74,75,76].
Similar to APP and PSEN1 mutations, PSEN2 mutations can also enhance Aβ production and contribute to AD development. An extensive literature search for PSEN2 mutations was conducted. Thirty-eight PSEN2 mutations have been reported yet, and most of these mutations were identified in European and African populations. Until now, only five missense mutations have been reported in Asian populations. Asn141Tyr was identified in a Chinese Han patient with EOAD [77], Gly34Ser was found in a Japanese patient [4], and three possibly pathogenic mutations—Arg62Cys, Val214Leu, and His169Asn—were reported in this study. PSEN2 mutations are associated with variable penetrance and a wide age range of disease onset, from 45 to 88 years [78,79]. PSEN2 is a transmembrane protein and a component of γ-secretase intramembrane protease, and is involved in various signaling pathways in AD development [80,81].
In an EOAD patient cohort, the estimated mutation frequencies for the three genes were < 1% for APP, 6% for PSEN1, and 1% for PSEN2 [82]. Together, they explain only 5% to 10% of the mutational profile in patients with EOAD [82,83]; however, approximately 90% of the mutations remain genetically unexplained [1,84]. With the exception of Korea, the People’s Republic of China, Taiwan, and Japan, limited reports are available on EOAD-associated mutations in Asian countries (Table 2). Two APP mutations have been identified in patients from Thailand [12] and Iran [85]. Recently, a novel PSEN1 mutation was reported in a Malaysian family [70]. Our primary goal was to provide clinicians a list of variants that can be accurately used in genetic counseling. Considering our whole cases, this goal is achieved for 9% mutations reported in the Asian population. Limited reports are available regarding EOAD-associated mutations in other East Asian countries. Hence, our investigators have begun efforts for screening AD-related mutations across Asian countries through collaborations. Compared with Caucasian patients, over 30 novel EOAD-associated mutations have been found in the APP, PSEN1, and PSEN2 genes in Asian patients (http://www.alzforum.org/mutations). Since the overall population and aging population in most Asian countries is increasing, genetic testing of patients with AD and other types of dementia is important for the diagnosis of dementia.
A limitation of this study is the absence of functional assessment of the possible and probable pathogenic variants, which could simplify their classification [8]. Moreover, only three genes were analyzed. It is possible that de novo mutations in other genes are also involved in the genetic determination of sporadic forms [16,18,86,87,88,89,90]. The limited number of resolved pedigrees and large number of genetically unexplained EOAD patients indicate that additional causal genes remain to be discovered. The next step involves performing whole exome/genome sequencing on negatively screened families and sporadic cases.
In conclusion, among the distinct mutations in the Asian patients and isolated cases in the Asian population, definite pathogenicity accounted for less than 16%, leaving a large group of autosomal dominant pedigrees genetically unexplained. In addition, our findings suggest that continuing the investigation of families harboring known mutations and the elucidation of the missing genetic etiology in unexplained EOAD patients has a vast potential to improve our understanding about the complexity of AD [1,10,15,90,91]. We also suggest that the use of high-throughput sequencing technologies for patients with EOAD and data integration from other -omics analyses (epigenomics, proteomics, transcriptomics, and metabolomics) might help in better understanding the underlying molecular mechanisms of AD.

4. Materials and Methods

Two-hundred patients with EOAD from the University Hospitals of Korea, Malaysia, Thailand, and the Philippines were recruited between 2009 and 2018. All patients underwent a comprehensive clinical examination, including personal medical and family history assessment and neuropsychological assessment. For each patient, AD diagnosis was established using the National Institute of Aging–Alzheimer’s Association (NIA–AA) criteria [92]. The project received ethics approval from the Seoul National University College of Medicine of Seoul National Bundang Hospital (SNUH), and written informed consent was obtained from all participants according to the requirements of the Seoul National Bundang Human Research Committee (B-1302/192-006, approval date: 15/03/2013). All procedures involving human participants were conducted in accordance with the ethical standards of the institutional and/or national research committee and 1964 Helsinki Declaration and its later amendments.

4.1. Genetic Analyses

Genetic analyses were performed on DNA extracted from whole blood. Sanger sequencing, next-generation sequencing (NGS) and whole exon sequencing (WES) were employed to search for mutations in the APP, PSEN1, and PSEN2 genes in patients with both sporadic and family history of AD. APOE genotypes comprising the APOE ε2, ε3, and ε4 alleles were assayed [15]. To confirm the presence of the identified mutations, standard sequencing was performed in both directions using the previously used primer set [1,2]. Prior to sequencing, PCR products were purified using the GeneAll PCR protocol kit (Seoul, Korea), following the manufacturer’s protocol. Big Dye Terminator Cyclic sequencing was performed on an ABI 3730XL DNA Analyzer (http://eng.bioneer.com/home.aspx, Bioneer Inc., Dajeon, Korea). The sequenced product was aligned using the NCBI Blast tool (http://blast.ncbi.nlm.nih.gov/Blast.cgi), and chromatograms were screened using the DNA BASER (http://www.dnabaser.com). Mutations and sequence variants were identified from the NCBI Gene (http://www.ncbi.nlm.nih.gov/gene) and UniProt (http://www.uniprot.org) databases. Briefly, patients with EOAD were analyzed by high-throughput sequencing, following the schematic diagram shown in Figure 5.

4.2. Bioinformatics

To determine whether APP, PSEN1, and PSEN2 variants presented rare or common polymorphisms, the variants were checked in the Korean Genome Reference Database (http://152.99.75.168/KRGDB/menuPages/firstInfo.jsp) for their novelty. The full genome sequences of 622 asymptomatic individuals were obtained by whole genome sequencing. In addition, variants were also checked in other large-scale genome reference databases, including the 1000 Genomes (http://www.internationalgenome.org/) and Exome Aggregation Consortium (ExAC; http://exac.broadinstitute.org) databases. Polymorphism phenotype v2 (PolyPhen-2) and Sorting Intolerant From Tolerant (SIFT) were used to predict whether the amino acid change would be disruptive to the encoded protein.

Author Contributions

Conceptualization: V.V.G., E.B., S.S.A.A., Y.C.Y., and S.Y.K.; Investigation: V.V.G., S.S.A.A., Y.C.Y., and S.Y.K.; Formal Analysis: V.V.G, and E.B.; Writing-Original Draft Preparation and Writing-Review & Editing: V.V.G; Supervision and project administration: S.S.A.A., Y.C.Y. and S.Y.K.

Funding

This research was supported by a National Research Foundation of Korea (NRF) grant awarded by the Korean government (NRF-2017R1A2B4012636 & NRF-2019R1G1A109740011).

Acknowledgments

The authors would like to thank Gaik-Siew Ch’ng (Department of Genetics, Kuala Lumpur Hospital, Kuala Lumpur, Malaysia), Vorapun Senanarong (Faculty of Medicine Siriraj Hospital, Mahidol University, Bangkok, Thailand), and Antonio D. Ligsay (Institute for Neurosciences, St. Luke’s Medical Center, Philippine) for their continued collaboration for research on neurodegeneration.

Conflicts of Interest

The authors declare no conflict of interest.

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Figure 1. Distribution of APP, PSEN1, and PSEN2 mutations in Asian countries. The fastest increase in the number of elderly individuals has been observed in Asian countries with approximately 60% of all patients diagnosed with dementia. The countries from which the gene mutations are reported are shown in purple.
Figure 1. Distribution of APP, PSEN1, and PSEN2 mutations in Asian countries. The fastest increase in the number of elderly individuals has been observed in Asian countries with approximately 60% of all patients diagnosed with dementia. The countries from which the gene mutations are reported are shown in purple.
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Figure 2. (a) Mutated APP residues identified in Asian countries are shown in different colors. (b) Location of Val669Leu in APP and mutations located near the β-secretase cleavage site. The nearest mutation is the “Swedish APP” mutation. Additional mutations located near the β-secretase cleavage site are the protective Ala673Thr and the pathogenic Ala673Val.
Figure 2. (a) Mutated APP residues identified in Asian countries are shown in different colors. (b) Location of Val669Leu in APP and mutations located near the β-secretase cleavage site. The nearest mutation is the “Swedish APP” mutation. Additional mutations located near the β-secretase cleavage site are the protective Ala673Thr and the pathogenic Ala673Val.
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Figure 3. Mutated PSEN1 residues identified in the Asian countries are shown in different colors. The predicted membrane topology of PSEN1 with the nine transmembrane domains (green shaded boxes) and boundaries between coding exons is shown. TM, transmembrane domain.
Figure 3. Mutated PSEN1 residues identified in the Asian countries are shown in different colors. The predicted membrane topology of PSEN1 with the nine transmembrane domains (green shaded boxes) and boundaries between coding exons is shown. TM, transmembrane domain.
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Figure 4. Mutated PSEN2 residues identified in the Asian countries are shown in different colors. The predicted membrane topology of PSEN2 with the nine transmembrane domains (yellow shaded boxes) and boundaries between coding exons are shown. TM, transmembrane domain.
Figure 4. Mutated PSEN2 residues identified in the Asian countries are shown in different colors. The predicted membrane topology of PSEN2 with the nine transmembrane domains (yellow shaded boxes) and boundaries between coding exons are shown. TM, transmembrane domain.
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Figure 5. High-throughput sequencing strategy for identifying gene variants in AD patients. The flow chart illustrates the major steps of the working procedure from patient sample analysis to the identification of mutation.
Figure 5. High-throughput sequencing strategy for identifying gene variants in AD patients. The flow chart illustrates the major steps of the working procedure from patient sample analysis to the identification of mutation.
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Table
Table 1. APP, PSEN1, and PSEN2 mutations discovered in Asian early-onset Alzheimer’s disease (EOAD) patients between 2009 and 2018.
Table 1. APP, PSEN1, and PSEN2 mutations discovered in Asian early-onset Alzheimer’s disease (EOAD) patients between 2009 and 2018.
GeneProtein ChangeNucleotide ChangeExonAPOEAOO (Years)GenderFamily HistoryPathogenicity PredictionClinical SignificancePopulation
PolyPhenSIFT
APPp.Glu145Lysc.433G > A4ε3/ε355FYD: 0.932T:0.496Located outside of the amyloid progressing regionKorean
p.Val225Alac.674T > C7ε3/ε365FYD: 932T: 0.496
p.Thr297Metc.890C > T7ε3/ε360FYD: 0.98D: 0.0
p.Pro484Serc.1450C > T11ε4/ε461FYP: 0.765T: 0.063
p.Val604Metc.1810C > T14ε3/ε355MYB: 0.450T: 0.095Thai
p.Val669Leuc.2005G > C17ε3/ε355FYB: 0.017T: 0.16Novel mutation, may cause EOADKorean
PSEN1p.Val96Phec.286G > T4ε3/ε440MYD: 1.0T: 0.002Known pathogenic mutation (EOAD)Malaysian
ε3/ε440FN
p.Thr116Ilec.335C > T5ε3/ε338FYD: 1.00D: 0Known pathogenic mutation (EOAD)Korean
ε3/ε341FY
p.Thr119Ilec.356C > Tε3/ε364FYD: 1.00D: 0Novel mutation, may be involved in EOAD
p.His163Proc.488A > C4ε3/ε337FYD: 1.00D: 0Novel mutation, may be involved in EOAD
p.Trp165Cysc.695G > T6ε3/ε353MYD: 1.00D: 0.001Known pathogenic mutation (EOAD)
p.Glu184Glyc.551A > G7ε3/ε337FYD: 0.878D: 0.005Known pathogenic mutation (EOAD)
p.Gly209Alac.626G > C7ε3/ε354FYD: 1.00D: 0Novel mutation, may be involved in EOAD
p.Leu226PheCTC > TTC7ε3/ε337FYD: 1.00D: 0Known pathogenic mutation (EOAD)
p.Leu232Proc.695T > C7ε3/ε337MYD: 1.00D: 0Novel mutation, may be involved in EOAD
p.Glu280Lysc.826G > A8ε3/ε348MYD: 1.00D: 0Novel mutation, may be involved in EOADMalaysian
ε3/ε355FY
ε3/ε357MY
p.Ala285Valc.854C > T8ε3/ε346FND: 1.0D: 0.015Known pathogenic mutation (EOAD)Korean
p.Gly417Alac.1250G > C12ε3/ε337MND: 1.00D: 0Novel mutation, may be involved in EOAD
PSEN2p.Arg62Cysc.184C > T5ε3/ε349MND: 0.877D: 0.05Known mutation, may be involved ADKorean
p.His169Asnc.505C > A6ε3/ε356FYD: 1.00D: 0Known mutation, May be involved AD
p.Val214Leuc.640G > A7ε3/ε356MYD: 0.836D: 0.09May be involved AD
ε3/ε470FYD: 0.836D: 0.09May be involved AD
Abbreviations: MC, number of mutations carriers in the family; AOO, age of onset ranges in the family; DD, disease duration (at death or last examination); APOE, apolipoprotein E genotype; F, familial; S, sporadic; Y, yes, U, unknown; D, damaging; AD, Alzheimer’s disease; EOAD: early-onset Alzheimer’s disease.
Table
Table 2. The spectrum of APP, PSEN1, and PSEN2 mutations found in Asian countries.
Table 2. The spectrum of APP, PSEN1, and PSEN2 mutations found in Asian countries.
GeneExonCodon, MutationLocation in the ProteinAge of Onset, Clinical CharacteristicsPathogenic NatureCountryReferences
APP3p.Glu145LysN-terminal50s/Familial, EOADLocated outside of the amyloid progressing regionKoreaThis study
4p.Val225AlaN-terminal65/Familial, EOADThis study
7pThr297MetN-terminal60s/Familial, EOADThis study
8p. Pro484SerN-terminal60s/Familial, EOADThis study
14p.Val604MetN-terminal55/Familial, EOADPathogenicThailandThis study
16p.Val669LeuN-terminal56 years; AD with a positive family historyLocated nearby the β-secretase cleavage site of APP, right next to the Swedish APP (Lys, Met670/671Asn, Leu) mutationKoreaThis study
p.Asp678AsnN-terminal59–65 years/familial, EOADProbably pathogenic, may enhance the toxic amyloid oligomer formationJapanWakutani et al., 2004 [25]
17p.Glu693delN-terminal44 years/familial, EOAD/MCIEnhances the toxic amyloid oligomer formationJapanTomiyama et al., 2008 [26]
p. Val710GlyTM-I65–82 years/Familial, AD, ParkinsonismProbably pathogenicChina, TaiwanThajeb et al. 2009 [27]
p. Thr714AlaTM-I47–55 years/Familial, EOAD, epilepsyProbably pathogenicIranPasalar et al. 2002 [28]
p.Val715MetTM-I41 years/
Familial EOAD		Expressed in HEK293 cells, revealed 2* decrease in Abeta 40 levels. Might destroy the cleavage of gamma secretase at site at Abeta40KoreaPark et al., 2008 [29]
p.Val717IleTM-I53 years/Familial, EOADIncreased Abeta42/Abeta40 ratio in CHO and HEK293 cellsJapanYoshioka et al., 1991 [30]
54 years/unknown, EOADThailandJiao et al., 2014 [31]
p. Ile718LeuTM-I65–82 years/Familial, AD, ParkinsonismProbably pathogenicChina, TaiwanThajeb et al., 2009 [27]
p.Leu720SerTM-I65–82 years/Familial, AD, ParkinsonismProbably pathogenicChina, TaiwanThajeb et al. 2009 [27]
4p.Leu85ProTM-I26 years, Juvenile EOADAbeta42/Abeta40 ratio increased in HEK293JapanAtaka et al. 2004 [54]
p. Val96PheTM-IEOAD, 49–60 years2.1 * increased Abeta 42/40 ratio in COS-1 cellsJapanKamino et al. 1996 [32]
p.Val97LeuTM-IEOADHigher beta secretase activity in human neuroblastoma cellsChinaFang et al. 2006 [33]
p. Phe105CysHL-I59 years/Familial, EOADSurvival of mutant neuroblastoma cells droppedChinaJiao et al., 2014 [31]
5p. Gly111ValHL-IEOAD; 59 years/FamilialIncreased ratios of secreted Aβ42/Aβ40 in vitro studyChinaQiu et al., 2019 [53]
p. Thr116IleHL-ILate 30s–early-40s years; EOAD with a probable familialPossible pathogenic mechanisms of mutationKoreaThis study
p. Thr119IleHL-I49–64 years; EOAD with a probable familial
p.Glu120LysHL-I40–65 years/Familial, EOADProbably pathogenicIranAkbari et al., 2013 [34]
p.Glu123LysHL-I26–45 years, EOAD, myoclonus, epilepsyAbeta42/total Abeta increased in COS-1 cells (2.7 *) and in HEK293 (4 *) cellsJapanYasuda et al. 1999 [35]
p.Ala136GlyTM-IIUnknown, EOADSurvival of mutant neuroblastoma cells dropped, deleterious effectsChinaFang et al., 2007 [36]
p.Met139IleTM-II38 years/Familial, EOADRatio of Abeta42/total Abeta increased in COS-1 cell lines.KoreaKim et al., 2010 [37]
p. Ile143ThrTM-II26–45 years, EOAD, myoclonus, epilepsyAbeta42/total Abeta increased in COS-1 cells (2.7 *) and in HEK293 (4 *) cellsJapanArai et al., 2008 [38]
p.Tyr154AsnTM-II40–60 years, EOAD, spastic paraparesisPathogenic nature might be associated with the missing aromatic ring.JapanHattori et al., 2004 [47]
6p.His163ArgHL-II43–50 years/5 Japanese families, both familial and de novo casesAbeta42/Abeta40 ratio increased 2 * in COS1 cell linesJapanKamino et al., 1996 [32]
p.His163ArgHL-II43–50 years/5 Japanese families, both familial and de novo casesAbeta42/Abeta40 ratio increased 2 * in COS1 cell linesKoreaHong et al., 1997 [48]
p.His163ProHL-II35 years/de novo EOAD, parkinsonismThe rigid proline might result abnormalities in the border of HL-II and TM-IIIKoreaThis study
p.Trp165GlyTM-III34–38 years; EOAD with strong familiarThe small glycine is a rare amino acid in the helixJapanHiguchi et al., 2000 [55]
p.Trp165CysTM-III55 years; memory decline, followed by difficulty in finding ways and had a strong family history of dementiaIncreased Aβ42 and decreased Aβ40 production in vitro; elevated Aβ42/Aβ40 ratioKoreaThis study
45 years; EOAD, a severe form of the illness, with cerebral and cerebellar atrophies and rapid deteriorationIndiaSyama et al., 2018 [49]
p.Ile167delTM-III38 years/familial; EOAD, spastic paraparesisDeletion might result abnormal conformation in TM-IIIChinaJiao et al., 2014 [31]
p.Ser169delTM-IIIEOAD, 42–50 years/familialMissing –OH group might result a missing H-bound in the TM-IIIChinaGuo et al., 2010 [43]
p.Leu173PheTM-III47–50/familial; EOAD with parkinsonismElevated Abeta42 levels and Abeta42/Abeta40 ration in neuroblastoma cellsJapanKasuga et al. 2009 [50]
7p.Glu184AspHL-III40s years; EOAD, DLB-like phenotypeThe smaller asparatic acid might change the loop conformationJapanYasuda et al. 1997 [35]
p.Glu184GlyHL-III40s years; probable autosomal dominant EOAD, frontal variant formResulting potential functional alterations; may also disturb the splicing near exon 7ThailandThis study
p.Gly206SerTM-IV30–35 years/familial, EOADProbably pathogenicKoreaPark et al., 2008 [29]
p.Gly209ArgTM-IV46–53 years, EOADArginine might result extra stress inside the helix and form abnormal hydrogen bondsJapanSugiyama et al., 1999 [44]
p.Gly209AlaTM-IV54 years; MCI with depression, followed by progressive deterioration in verbal and visual memoryThe extra –CH3 group in alanine might result extra stress inside the TM-IV regionKoreaThis study
p.Ile213ThrTM-IV42–47 years, EOADIncreased (1.7 * Abeta)JapanKamino et al., 1996 [32]
p.Gly217AspHL-IV42–47 years/familial, EOADIncreased (1.7 * Abeta)JapanTakao et al., 2002 [52]
p.Leu226PheTM-V37 years; de novo, Aβ plaques observedResults elevated Abeta42/Abeta40 ratio in HEK293 cellsKoreaThis study
p.Leu226ArgTM-V60 years/familial, EOADProbably pathogenicChinaMa et al., 2019 [41]
p.Glu311ArgTM-V> 65 years, familial, LOADOverproducing toxic Aβ species and enhancing tau phosphorylationChinaDong et al., 2017 [56]
p.Leu232ProTM-V37 years/familial; EOADThe rigid proline might result serious torsion in the TM-V since proline is helix breakerKoreaThis study
p.Met233ThrTM-V34 years/de novo, EOAD, rapid progressive memory impairmentElevated (3.2 *) Abeta42/Abeta40 levels in CHO cellsKoreaPark HK et al., 2008 [29]
p.Phe237IleTM-V35 years/de novo, EOAD, spastic paraparesisProbably pathogenicJapanSodeyama et al. 2001 [57]
p.Leu248ProTM-VI42 years/familial, EOADProline is a helix breaker, resulting in torsion in TM-IVChinaJiao et al., 2014 [31]
p.Leu250ValTM-VI40–51 years/Familial, EOAD, myoclonus, seizuresProbably pathogenicJapanFuruya t al., 2003 [58]
8p.Ala260ValTM-VI27–46 years/Familial, EOAD, Pick inclusions1.5 * Increased Abeta42/total Abeta in COS1 cellsJapanIkeda et al., 1996 [59]
p.Gly266SerHL-VI(a)35–44 years, EOAD, spastic paraparesis, aphasiaProbably pathogenicJapanMatsubara-Tsutsui et al., 2002 [60]
p.Arg 269HisHL-VI(a)46–67 years/Familial, EOAD, myoclonusUnknownJapanKamimura el al., 1998 [61]
p.Glu273AlaHL-VI(a)46–67 years/Familial, EOAD, myoclonusUnknownJapanKamimura el al., 1998 [61]
p.Glu280AlaHL-VI (MA)48–57 years/Familial, EOAD, parkinsonismProbably pathogenicJapanTanahashi et al., 1996 [62]
p.Glu280LysHL-VI (MA)48–57; EOADProbably pathogenicMalaysiaThis study
p.Leu282PheHL-VI (MA)51 years, familial, EOADProbably pathogenicJapanHamaguchi et al., 2009 [63]
p.Pro284LeuHL-VI (MA)32 years, cotton-wool plaques and neurofibrillary tangles or amyloid angiopathy in brainProbably pathogenicJapanTabira et al., 2002 [64]
p.Ala285ValHL-VI (MA)46 year/de novo, EOADThe Abeta42/total Abeta ratio increased; Abeta40/total Abeta and Abeta38/total Abeta ratios decreasedKoreaThis study
50.5 years, two familiesJapanIkeuchi et al., 2008 [65]
p.Leu286ValHL-VI (MA)47 yearsIncreases in the Abeta42/total Abeta ratio (1.5 *) and Abeta42/Abeta40 ratio (2.1 *)JapanIkeuchi et al., 2008 [65]
Intron 8Exon9 del-47.5 years, in EOAD with spastic paraparesiselevated Abeta42 levels and Abeta42/40 ratio were observedJapanTabira et al., 2002 [64]
10p.Arg352CysHL-VI (b)56–62 years, EOAD, psychiatric, behavioral symptomsCysteine could result intramolecular disulfide boundChinaJiang et al., 2015 [66]
11p.Gly378GluTM-VII37 years, EOAD, familiar positiveAbeta42/Abeta40 ratio increased (3.2 *)JapanIkeda et al., 1996 [59]
p.Leu381ValTM-VII30s years, AD and spastic paraparesisAbeta42/Abeta40 ratio increased (1.9 *)JapanIkeuchi et al., 2008 [65]
p.Gly384AlaTM-VII31–37 years, EOAD, senile plaques and tangles inside proband’s brainBeta40 and the Abeta42/Abeta40 ratio decreased and increased significantly. Abeta42/total Abeta ratio increased (3.8 *)JapanKamimura et al. 1998 [61]
p.Leu392ValTM-VII42 years, EOADAbeta42/Abeta40 ratio (2.4*). An increase in the Abeta42/Abeta40 ratio (2.9 *)JapanIkeuchi et al. 2008 [65]
p.Asn405SerHL-VIIEOAD, the patient has several senile plaques and tangles in the brainIt caused disturbances in the motor neuronal systems, leading to spastic paraparesisJapanYasuda et al., 2000 [46]
p.Gly417AlaHL-VIII37 years; EOAD, parkinsonism, positive familiarPathogenic mechanismKoreaThis study
12p.Ala431ValHL-VIII16 months, t-tau and phospho-Tau levels increased in the CSF, and metabolic deficits were detected in several parts of the brainPossibly pathogenicJapanMatsushita et al., 2002 [45]
p.Ala434ThrHL-VIII38 years, EOAD,
Hallucinations, delusions		Threonine might result extramolecular or intramolecular hydrogen boundChinaJiao et al., 2014 [31]
p.Thr440delHL-VIII52 years, strong familiar history, EOAD and parkinsonismProbably pathogenic, may alter the normal amyloid productionJapanIshikawa et al., 2005 [42]
PSEN24p.Arg62CysN-term49 years, EOADPossibly pathogenic, may alter the normal amyloid production.KoreaThis study
40–65 years, EOADIranAkbari et al., 2013 [34]
5p.Asn141TyrTM-II43–49 years, EOADNo functional dataChinaNiu et al., 2014 [39]
6p.His169AsnTM-III50 years; de novoIt may result in major helix torsion due to histidine to asparagine substitutionKoreaThis study
62 years; AD, de novoChinaShi Z et al., 2015 [40]
68 years; FTD, progressive nonfluent aphasia, Familial
63 years/Familial, LOADChinaMa et al., 2018 [41]
7p.Val214LeuTM-IV56–70 years; ADThe extra CH3 group in leucine could result extra stress in the TM-IV regionKoreaThis study
Abbreviation: APP, amyloid precursor protein; PSEN1, presenilin-1; PSEN2, presenilin-2; AD, Alzheimer’s disease; EOAD, early-onset Alzheimer’s disease; LOAD, late-onset Alzheimer’s disease; MCI, mild cognitive impairment; DLB, dementia with Lewy bodies; FTD, frontotemporal dementia; HEK293, human embryonic kidney 293; CHO, Chinese hamster ovary; COS-1, cercopithecus aethiops kidney; TM, transmembrane domain; * multiplication sign.

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MDPI and ACS Style

Giau, V.V.; Bagyinszky, E.; Youn, Y.C.; An, S.S.A.; Kim, S. APP, PSEN1, and PSEN2 Mutations in Asian Patients with Early-Onset Alzheimer Disease. Int. J. Mol. Sci. 2019, 20, 4757. https://doi.org/10.3390/ijms20194757

AMA Style

Giau VV, Bagyinszky E, Youn YC, An SSA, Kim S. APP, PSEN1, and PSEN2 Mutations in Asian Patients with Early-Onset Alzheimer Disease. International Journal of Molecular Sciences. 2019; 20(19):4757. https://doi.org/10.3390/ijms20194757

Chicago/Turabian Style

Giau, Vo Van, Eva Bagyinszky, Young Chul Youn, Seong Soo A. An, and SangYun Kim. 2019. "APP, PSEN1, and PSEN2 Mutations in Asian Patients with Early-Onset Alzheimer Disease" International Journal of Molecular Sciences 20, no. 19: 4757. https://doi.org/10.3390/ijms20194757

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