<p>Rare and undiagnosed diseases pose diagnostic challenges due to phenotypic and genetic heterogeneity and the limitations of conventional molecular testing. As part of the RareBoost project, we implemented an integrated, stepwise genomic strategy in a cohort of 134 patients from 120 families with previously inconclusive genetic testing. Our strategy combined systematic exome sequencing with subsequent genome sequencing when indicated, followed by targeted RNA-sequencing, and complemented with comprehensive phenotyping and follow-up segregation analysis. Definitive molecular diagnoses (pathogenic/likely pathogenic variants) were achieved in 25.0% of families, and an additional 25.8% harbored clinically relevant variants of uncertain significance with phenotypic correlation. This approach identified non-coding and structural variants while resolving cases through systematic reanalysis of previously negative data. Collectively, our findings demonstrate that integrated genomic and transcriptomic analyses with reanalysis of existing data enhance diagnostic yield in complex rare disease cohorts and provide a scalable framework for implementing genomic medicine in clinical practice.</p>

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Integrative and systematic genomic approaches to improve diagnosis in rare and undiagnosed diseases: results from the RareBoost project

  • Ayca Yigit,
  • Mert Pekerbas,
  • Baris Salman,
  • Kutay Bulut,
  • Emre Ozzeybek,
  • Mehmet Mert Topaloglu,
  • Burcu Akman,
  • Ravza Nur Yildirim,
  • Sinem Aktug,
  • Tugce Batur,
  • Ahmet Okay Caglayan,
  • Aliye Kubra Unal,
  • Inci Yaprak,
  • Beste Ozkalay,
  • Caglar Celebi,
  • Evin Iscan,
  • Miray Sevinin,
  • Mehmet Baysan,
  • Nese Atabey,
  • Sanem Tercan Avci,
  • Yavuz Oktay,
  • Ayse Ipek Polat,
  • Ayse Semra Hiz,
  • Uluc Yis,
  • Huseyin Bahadır Senol,
  • Mustafa Halk,
  • Elif Naz Kadem,
  • Dilek Sonmezoglu,
  • Asude Durmaz,
  • Ayca Aykut,
  • Haluk Akin,
  • Pinar Gencpinar,
  • Safa Mete Dagdas,
  • Mehmet Semiz,
  • Ozlem Giray,
  • Semra Gursoy,
  • Seda Gunes,
  • Ozlem Akgun Dogan,
  • Bulent Kara,
  • Esra Isik,
  • Tahir Atik,
  • Merve Bilen,
  • Nur Arslan,
  • Pelin Teke,
  • Abdurrahman Akgun,
  • Arzu Akyay,
  • Aslihan Uzun,
  • Aydan Mengubas Erbas,
  • Berk Ozyilmaz,
  • Fatma Silan,
  • Gokhan Ozan Cetin,
  • Ilknur Surucu Kara,
  • Korcan Demir,
  • Ozlem Unal Uzun,
  • Sevil Yildiz,
  • Tolga Polat,
  • Sezgin Sahin,
  • Ercan Mihci,
  • Gonca Kilic Yildirim,
  • Fehime Erdem,
  • Ugur Ozbek

摘要

Rare and undiagnosed diseases pose diagnostic challenges due to phenotypic and genetic heterogeneity and the limitations of conventional molecular testing. As part of the RareBoost project, we implemented an integrated, stepwise genomic strategy in a cohort of 134 patients from 120 families with previously inconclusive genetic testing. Our strategy combined systematic exome sequencing with subsequent genome sequencing when indicated, followed by targeted RNA-sequencing, and complemented with comprehensive phenotyping and follow-up segregation analysis. Definitive molecular diagnoses (pathogenic/likely pathogenic variants) were achieved in 25.0% of families, and an additional 25.8% harbored clinically relevant variants of uncertain significance with phenotypic correlation. This approach identified non-coding and structural variants while resolving cases through systematic reanalysis of previously negative data. Collectively, our findings demonstrate that integrated genomic and transcriptomic analyses with reanalysis of existing data enhance diagnostic yield in complex rare disease cohorts and provide a scalable framework for implementing genomic medicine in clinical practice.