4.6 Review Book Chapter

Genomics of Immune Diseases and New Therapies

Journal

ANNUAL REVIEW OF IMMUNOLOGY, VOL 34
Volume 34, Issue -, Pages 121-149

Publisher

ANNUAL REVIEWS
DOI: 10.1146/annurev-immunol-041015-055620

Keywords

genomics; biochemical; mechanism; immune disorder; targeted therapy

Categories

Funding

  1. Intramural NIH HHS [Z01 AI000565-11] Funding Source: Medline

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Genomic DNA sequencing technologies have been one of the great advances of the 21st century, having decreased in cost by seven orders of magnitude and opening up new fields of investigation throughout research and clinical medicine. Genomics coupled with biochemical investigation has allowed the molecular definition of a growing number of new genetic diseases that reveal new concepts of immune regulation. Also, defining the genetic pathogenesis of these diseases has led to improved diagnosis, prognosis, genetic counseling, and, most importantly, new therapies. We highlight the investigational journey from patient phenotype to treatment using the newly defined XMEN disease, caused by the genetic loss of the MAGT1 magnesium transporter, as an example. This disease illustrates how genomics yields new fundamental immunoregulatory insights as well as how research genomics is integrated into clinical immunology. At the end, we discuss two other recently described diseases, CHAI/LATAIE (CTLA-4 deficiency) and PASLI (PI3K dysregulation), as additional examples of the journey from unknown immunological diseases to new precision medicine treatments using genomics. In almost all things, what they contain of useful or applicable nature is hardly perceived unless we are deprived of them, or they become deranged in some way. William Harvey (1657)

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