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1. The Study of a 231 French Patient Cohort Significantly Extends the Mutational Spectrum of the Two Major Usher Genes MYO7A and USH2A .

2. Whole USH2A Gene Sequencing Identifies Several New Deep Intronic Mutations.

3. Enrichment of LOVD-USHbases with 152 USH2A genotypes defines an extensive mutational spectrum and highlights missense hotspots.

4. Non-USH2A mutations in USH2 patients.

5. Usher syndrome type 2 caused by activation of an USH2A pseudoexon: implications for diagnosis and therapy.

6. The USH2A c.2299delG mutation: dating its common origin in a Southern European population.

7. Molecular and in silico analyses of the full-length isoform of usherin identify new pathogenic alleles in Usher type II patients.

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