2008
DOI: 10.1016/j.ymgme.2007.08.124
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CLN2/TPP1 deficiency: The novel mutation IVS7-10A>G causes intron retention and is associated with a mild disease phenotype

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Cited by 31 publications
(24 citation statements)
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“…Table 1 lists the mutations found in this South American cohort, including those published in earlier works by our group (Kohan et al, 2008; Kohan et al, 2009) or other authors (Sleat et al, 1999; Bessa et al, 2008; Kousi et al, 2012). We have added to the mutational spectrum those of 18 additional subjects, identifying four novel mutations.…”
Section: Discussionmentioning
confidence: 99%
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“…Table 1 lists the mutations found in this South American cohort, including those published in earlier works by our group (Kohan et al, 2008; Kohan et al, 2009) or other authors (Sleat et al, 1999; Bessa et al, 2008; Kousi et al, 2012). We have added to the mutational spectrum those of 18 additional subjects, identifying four novel mutations.…”
Section: Discussionmentioning
confidence: 99%
“…The presence of novel splice sites that compete with the wild-type sites would allow the alternative existence of normal and mutated mRNAs, which may in turn be related to some residual enzyme activity that ameliorates the pathological phenotype. In fact, the I7 c.887-10A>G mutation was extensively studied byBessa et al (2008). They found this intronic mutation in homozygous condition in one Portuguese patient exhibiting a protracted phenotype and residual TPP1 activity.…”
Section: Discussionmentioning
confidence: 99%
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“…4 Nonclassic presentations (ie, juvenile, adult, or infantile onset) exist as well. 3,[5][6][7][8] On conventional MR imaging, a marked supratentorial and infratentorial atrophy with ventriculomegaly is the typical finding. In addition, a progressive-but-mild increase of WM signal intensity on T2WI and increased ADC values are observed.…”
mentioning
confidence: 99%
“…It is now recognized that mutations in all genes are distributed across many countries, albeit with higher incidence in some ethnic groups due to founder effects. Among the many recognized variants of NCL human forms (recent reviews in [3,6,11]), eight causal genes have been identified: CLN10/CTSD [12][13][14], CLN1/PPT1 [3,6,[15][16][17][18], CLN2/TPP1 [6,[18][19][20][21], CLN3 [22][23][24][25], CLN5 [26][27][28][29][30], CLN6 [31][32][33][34], CLN7/ MFSD8 [35][36][37][38][39], CLN8 [40][41][42]. The genes CLCN6 [43], and CLCN7 [44], and possibly SGSH [45], may also contribute to rare forms of NCL.…”
Section: Introductionmentioning
confidence: 99%