2006
DOI: 10.1016/j.parkreldis.2006.04.001
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LRRK2 G2019S mutation and Parkinson's disease: A clinical, neuropsychological and neuropsychiatric study in a large Italian sample

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Cited by 101 publications
(88 citation statements)
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“…Even when confined to LRRK2 G2019S, penetrance estimates vary widely (24%-100%). 8 Penetrance estimates may differ based on ethnic group, sex, and the presence of genetic or environmental modifiers of age at onset. How probands and family members are ascertained and the statistical methodologies used may also help explain this range in estimates; for example, 8 young-onset and familial cases, both of whom are more likely to harbor genetic mutations, are more likely to be seen at an academic center.…”
mentioning
confidence: 99%
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“…Even when confined to LRRK2 G2019S, penetrance estimates vary widely (24%-100%). 8 Penetrance estimates may differ based on ethnic group, sex, and the presence of genetic or environmental modifiers of age at onset. How probands and family members are ascertained and the statistical methodologies used may also help explain this range in estimates; for example, 8 young-onset and familial cases, both of whom are more likely to harbor genetic mutations, are more likely to be seen at an academic center.…”
mentioning
confidence: 99%
“…8 Penetrance estimates may differ based on ethnic group, sex, and the presence of genetic or environmental modifiers of age at onset. How probands and family members are ascertained and the statistical methodologies used may also help explain this range in estimates; for example, 8 young-onset and familial cases, both of whom are more likely to harbor genetic mutations, are more likely to be seen at an academic center. Here, we estimate penetrance of LRRK2 G2019S in a genetically homogenous AJ cohort, using the same validated family history interview (FHI) at 3 academic centers specialized in the care of PD.…”
mentioning
confidence: 99%
“…LRRK2 is a complex 286-kDa protein that consists of multiple domains, including (in order, from the amino to carboxyl terminus) armadillo, ankyrin, and the namesake leucine-rich repeats (LRRs), followed by an ROC (Ras of complex proteins) GTPase domain, a COR (C-terminal of ROC) dimerization domain, a kinase domain, and a predicted C-terminal WD40 repeat domain (4-6). Several single-nucleotide alterations have been identified in LRRK2, but only five missense mutations within the ROC, COR, and kinase domains clearly segregate with PD in large family studies (7,8). It has recently been shown that the WD40 domain is required to stabilize the LRRK2 dimer and to execute LRRK2-associated kinase activity as well as neurotoxicity (9, 10), but the role of this domain within LRRK2 physiological and pathological function has not yet been completely defined.…”
mentioning
confidence: 99%
“…Frequencies ranged from the no cases to 35.7% in sporadic and 42% in familial North-African Arab patients (Brás et al 2005;Lesage et al 2005Lesage et al , 2006Lesage et al , 2008Clark et al 2006;Deng et al 2006;Gaig et al 2006;Goldwurm et al 2006;Infante et al 2006;Ozelius et al 2006;Marongiu et al 2006;Mata et al 2006Mata et al , 2009bCivitelli et al 2007;Cossu et al 2007;Ferreira et al 2007;González-Fernández et al 2007;Ishihara et al 2007;Orr-Urtreger et al 2007;Perez-Pastene et al 2007;Squillaro et al 2007;Hulihan et al 2008;Munhoz et al 2008;Pimentel et al 2008;Correia Guedes et al 2009;De Rosa et al 2009;Floris et al 2009;Gorostidi et al 2009). …”
Section: Discussionmentioning
confidence: 99%