AI Article Synopsis

  • Mucin-1 kidney disease, also known as MCKD1, is an autosomal dominant kidney disease caused by a mutation in the MUC1 gene that is challenging to diagnose due to variable symptoms and age of onset.
  • The mutation's specific location in a high GC content region has made traditional next-generation sequencing ineffective for detection.
  • To address this, researchers developed a mass spectrometry-based probe extension assay, which successfully identified the mutation with 100% sensitivity and specificity, validating it as a reliable diagnostic tool.

Article Abstract

Mucin-1 kidney disease, previously described as medullary cystic kidney disease type 1 (MCKD1, OMIM 174000), is an autosomal dominant tubulointerstitial kidney disease recently shown to be caused by a single-base insertion within the variable number tandem repeat region of the MUC1 gene. Because of variable age of disease onset and often subtle signs and symptoms, clinical diagnosis of mucin-1 kidney disease and differentiation from other forms of hereditary kidney disease have been difficult. The causal insertion resides in a variable number tandem repeat region with high GC content, which has made detection by standard next-generation sequencing impossible to date. The inherently difficult nature of this mutation required an alternative method for routine detection and clinical diagnosis of the disease. We therefore developed and validated a mass spectrometry-based probe extension assay with a series of internal controls to detect the insertion event using 24 previously characterized positive samples from patients with mucin-1 kidney disease and 24 control samples known to be wild type for the variant. Validation results indicate an accurate and reliable test for clinically establishing the molecular diagnosis of mucin-1 kidney disease with 100% sensitivity and specificity across 275 tests called.

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http://dx.doi.org/10.1016/j.jmoldx.2016.03.003DOI Listing

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