Challenges in Clinicogenetic Correlations: One Phenotype - Many Genes

Rahul Gannamani; Sterre van der Veen; Martje van Egmond; Tom J de Koning; Marina A J Tijssen

doi:10.1002/mdc3.13163

Challenges in Clinicogenetic Correlations: One Phenotype - Many Genes

Mov Disord Clin Pract. 2021 Mar 2;8(3):311-321. doi: 10.1002/mdc3.13163. eCollection 2021 Apr.

Authors

Rahul Gannamani^{1

2

3}, Sterre van der Veen^{1

3}, Martje van Egmond^{1

3}, Tom J de Koning^{2

3

4}, Marina A J Tijssen^{1

3}

Affiliations

¹ Department of Neurology University of Groningen, University Medical Centre Groningen Groningen The Netherlands.
² Department of Genetics University of Groningen, University Medical Centre Groningen Groningen The Netherlands.
³ Expertise Centre Movement Disorders Groningen University Medical Centre Groningen Groningen The Netherlands.
⁴ Pediatrics, Department of Clinical Sciences Lund University Lund Sweden.

Abstract

Background: In the field of movement disorders, what you see (phenotype) is seldom what you get (genotype). Whereas 1 phenotype was previously associated to 1 gene, the advent of next-generation sequencing (NGS) has facilitated an exponential increase in disease-causing genes and genotype-phenotype correlations, and the "one-phenotype-many-genes" paradigm has become prominent.

Objectives: To highlight the "one-phenotype-many-genes" paradigm by discussing the main challenges, perspectives on how to address them, and future directions.

Methods: We performed a scoping review of the various aspects involved in identifying the underlying molecular cause of a movement disorder phenotype.

Results: The notable challenges are (1) the lack of gold standards, overlap in clinical spectrum of different movement disorders, and variability in the interpretation of classification systems; (2) selecting which patients benefit from genetic tests and the choice of genetic testing; (3) problems in the variant interpretation guidelines; (4) the filtering of variants associated with disease; and (5) the lack of standardized, complete, and up-to-date gene lists. Perspectives to address these include (1) deep phenotyping and genotype-phenotype integration, (2) adherence to phenotype-specific diagnostic algorithms, (3) implementation of current and complementary bioinformatic tools, (4) a clinical-molecular diagnosis through close collaboration between clinicians and genetic laboratories, and (5) ongoing curation of gene lists and periodic reanalysis of genetic sequencing data.

Conclusions: Despite the rapidly emerging possibilities of NGS, there are still many steps to take to improve the genetic diagnostic yield. Future directions, including post-NGS phenotyping and cohort analyses enriched by genotype-phenotype integration and gene networks, ought to be pursued to accelerate identification of disease-causing genes and further improve our understanding of disease biology.

Keywords: genetics; genotype; movement disorder; neurogenetics; phenotype.

Publication types

Review