Screening for PS1 mutations in a referral-based series of AD cases: 21 novel mutations

E. A. Rogaeva; K. C. Fafel; Y. Q. Song; H. Medeiros; C. Sato; Y. Liang; E. Richard; E. I. Rogaev; P. Frommelt; A. D. Sadovnick; W. Meschino; K. Rockwood; M. A. Boss; R. Mayeux; P. St George-Hyslop

Screening for PS1 mutations in a referral-based series of AD cases: 21 novel mutations

E. A. Rogaeva, K. C. Fafel, Y. Q. Song, H. Medeiros, C. Sato, Y. Liang, E. Richard, E. I. Rogaev, P. Frommelt, A. D. Sadovnick, W. Meschino, K. Rockwood, M. A. Boss, R. Mayeux, P. St George-Hyslop

Other Departments

Research output: Contribution to journal › Article › Academic › peer-review

195 Citations (Scopus)

Abstract

Mutations in the presenilin-1 gene (PS1) account for a majority of patients with early-onset familial AD. However, the clinical indications and algorithms for genetic testing in dementia are still evolving. The entire open reading frame of the PS1 gene was sequenced in a series of 414 consecutive patients referred for diagnostic testing, including 372 patients with AD and 42 asymptomatic persons with a strong family history of AD. Forty-eight independent patients screened had a PS1 mutation including 21 novel mutations. In addition, 3% of subjects (11/413) had a known polymorphism, the Glu318Gly substitution. The majority of the mutations were missense substitutions but there were three insertions and Delta exon 10 mutation. With six exceptions (codons 35, 178, 352, 354, 358, and 365) most of the mutations occurred at residues conserved in the homologous PS2 gene or in PS1 of other species. Eleven percent of a referral-based series of patients with AD can be explained by coding sequence mutations in the PS1 gene. The high frequency of PS1 mutations in this study indicates that screening for PS1 mutations in AD is likely to be successful, especially when directed at patients with a positive family history with onset before 60 years (90% of those with PS1 mutations were affected by age 60 years). This will also have significance for the secondary identification of at-risk relatives who might be candidates for future prophylactic therapies for AD

Original language	English
Pages (from-to)	621-625
Journal	Neurology
Volume	57
Issue number	4
Publication status	Published - 2001

Cite this

@article{4b87a76bde3b4cb9ac73dfa7b80bb36a,

title = "Screening for PS1 mutations in a referral-based series of AD cases: 21 novel mutations",

abstract = "Mutations in the presenilin-1 gene (PS1) account for a majority of patients with early-onset familial AD. However, the clinical indications and algorithms for genetic testing in dementia are still evolving. The entire open reading frame of the PS1 gene was sequenced in a series of 414 consecutive patients referred for diagnostic testing, including 372 patients with AD and 42 asymptomatic persons with a strong family history of AD. Forty-eight independent patients screened had a PS1 mutation including 21 novel mutations. In addition, 3% of subjects (11/413) had a known polymorphism, the Glu318Gly substitution. The majority of the mutations were missense substitutions but there were three insertions and Delta exon 10 mutation. With six exceptions (codons 35, 178, 352, 354, 358, and 365) most of the mutations occurred at residues conserved in the homologous PS2 gene or in PS1 of other species. Eleven percent of a referral-based series of patients with AD can be explained by coding sequence mutations in the PS1 gene. The high frequency of PS1 mutations in this study indicates that screening for PS1 mutations in AD is likely to be successful, especially when directed at patients with a positive family history with onset before 60 years (90% of those with PS1 mutations were affected by age 60 years). This will also have significance for the secondary identification of at-risk relatives who might be candidates for future prophylactic therapies for AD",

author = "Rogaeva, {E. A.} and Fafel, {K. C.} and Song, {Y. Q.} and H. Medeiros and C. Sato and Y. Liang and E. Richard and Rogaev, {E. I.} and P. Frommelt and Sadovnick, {A. D.} and W. Meschino and K. Rockwood and Boss, {M. A.} and R. Mayeux and {St George-Hyslop}, P.",

year = "2001",

language = "English",

volume = "57",

pages = "621--625",

journal = "Neurology",

issn = "0028-3878",

publisher = "American Academy of Neurology",

number = "4",

}

TY - JOUR

T1 - Screening for PS1 mutations in a referral-based series of AD cases: 21 novel mutations

AU - Rogaeva, E. A.

AU - Fafel, K. C.

AU - Song, Y. Q.

AU - Medeiros, H.

AU - Sato, C.

AU - Liang, Y.

AU - Richard, E.

AU - Rogaev, E. I.

AU - Frommelt, P.

AU - Sadovnick, A. D.

AU - Meschino, W.

AU - Rockwood, K.

AU - Boss, M. A.

AU - Mayeux, R.

AU - St George-Hyslop, P.

PY - 2001

Y1 - 2001

N2 - Mutations in the presenilin-1 gene (PS1) account for a majority of patients with early-onset familial AD. However, the clinical indications and algorithms for genetic testing in dementia are still evolving. The entire open reading frame of the PS1 gene was sequenced in a series of 414 consecutive patients referred for diagnostic testing, including 372 patients with AD and 42 asymptomatic persons with a strong family history of AD. Forty-eight independent patients screened had a PS1 mutation including 21 novel mutations. In addition, 3% of subjects (11/413) had a known polymorphism, the Glu318Gly substitution. The majority of the mutations were missense substitutions but there were three insertions and Delta exon 10 mutation. With six exceptions (codons 35, 178, 352, 354, 358, and 365) most of the mutations occurred at residues conserved in the homologous PS2 gene or in PS1 of other species. Eleven percent of a referral-based series of patients with AD can be explained by coding sequence mutations in the PS1 gene. The high frequency of PS1 mutations in this study indicates that screening for PS1 mutations in AD is likely to be successful, especially when directed at patients with a positive family history with onset before 60 years (90% of those with PS1 mutations were affected by age 60 years). This will also have significance for the secondary identification of at-risk relatives who might be candidates for future prophylactic therapies for AD

AB - Mutations in the presenilin-1 gene (PS1) account for a majority of patients with early-onset familial AD. However, the clinical indications and algorithms for genetic testing in dementia are still evolving. The entire open reading frame of the PS1 gene was sequenced in a series of 414 consecutive patients referred for diagnostic testing, including 372 patients with AD and 42 asymptomatic persons with a strong family history of AD. Forty-eight independent patients screened had a PS1 mutation including 21 novel mutations. In addition, 3% of subjects (11/413) had a known polymorphism, the Glu318Gly substitution. The majority of the mutations were missense substitutions but there were three insertions and Delta exon 10 mutation. With six exceptions (codons 35, 178, 352, 354, 358, and 365) most of the mutations occurred at residues conserved in the homologous PS2 gene or in PS1 of other species. Eleven percent of a referral-based series of patients with AD can be explained by coding sequence mutations in the PS1 gene. The high frequency of PS1 mutations in this study indicates that screening for PS1 mutations in AD is likely to be successful, especially when directed at patients with a positive family history with onset before 60 years (90% of those with PS1 mutations were affected by age 60 years). This will also have significance for the secondary identification of at-risk relatives who might be candidates for future prophylactic therapies for AD

M3 - Article

C2 - 11524469

SN - 0028-3878

VL - 57

SP - 621

EP - 625

JO - Neurology

JF - Neurology

IS - 4

ER -