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Clinical Cytogenetics: Current Practices and Beyond. | LitMetric

Clinical Cytogenetics: Current Practices and Beyond.

J Appl Lab Med

The Steve and Cindy Rasmussen Institute for Genomic Medicine, Nationwide Children's Hospital, Columbus, OH, United States.

Published: January 2024

AI Article Synopsis

  • The field of cytogenetics has evolved significantly with advancements in technology, transitioning from older methods like banding to more modern techniques such as FISH and chromosomal microarrays.
  • This review highlights key discoveries in clinical cytogenetics, discussing current testing methods, their applications, and limitations, as well as potential future technologies.
  • Traditional cytogenetic methods remain essential for testing, offering quick results for known genetic conditions, while newer high-throughput technologies improve the analysis of more complex cases.

Article Abstract

Background: Throughout history, the field of cytogenetics has witnessed significant changes due to the constant evolution of technologies used to assess chromosome number and structure. Similar to the evolution of single nucleotide variant detection from Sanger sequencing to next-generation sequencing, the identification of chromosome alterations has progressed from banding to fluorescence in situ hybridization (FISH) to chromosomal microarrays. More recently, emerging technologies such as optical genome mapping and genome sequencing have made noteworthy contributions to clinical laboratory testing in the field of cytogenetics.

Content: In this review, we journey through some of the most pivotal discoveries that have shaped the development of clinical cytogenetics testing. We also explore the current test offerings, their uses and limitations, and future directions in technology advancements.

Summary: Cytogenetics methods, including banding and targeted assessments like FISH, continue to hold crucial roles in cytogenetic testing. These methods offer a rapid turnaround time, especially for conditions with a known etiology involving recognized cytogenetic aberrations. Additionally, laboratories have the flexibility to now employ higher-throughput methodologies to enhance resolution for cases with greater complexity.

Download full-text PDF

Source
http://dx.doi.org/10.1093/jalm/jfad086DOI Listing

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