AI Article Synopsis

  • - Transporter research usually focuses on well-known substrates, which limits understanding of how transporters work for less common micromolecules like micronutrients and d-serine, a potential kidney function biomarker.
  • - The study identifies two renal transport systems for d-serine: ASCT2, a previously unrecognized small amino acid transporter, and sodium-coupled monocarboxylate transporters (SMCTs), which reveals d-serine’s role as a non-canonical substrate.
  • - The findings show that ASCT2 is primarily responsible for d-serine transport, especially in pathological conditions, and highlight the need for broader research into the transport systems of trace micromolecules in health and disease contexts.

Article Abstract

Transporter research primarily relies on the canonical substrates of well-established transporters. This approach has limitations when studying transporters for the low-abundant micromolecules, such as micronutrients, and may not reveal physiological functions of the transporters. While d-serine, a trace enantiomer of serine in the circulation, was discovered as an emerging biomarker of kidney function, its transport mechanisms in the periphery remain unknown. Here, using a multi-hierarchical approach from body fluids to molecules, combining multi-omics, cell-free synthetic biochemistry, and ex vivo transport analyses, we have identified two types of renal d-serine transport systems. We revealed that the small amino acid transporter ASCT2 serves as a d-serine transporter previously uncharacterized in the kidney and discovered d-serine as a non-canonical substrate of the sodium-coupled monocarboxylate transporters (SMCTs). These two systems are physiologically complementary, but ASCT2 dominates the role in the pathological condition. Our findings not only shed light on renal d-serine transport, but also clarify the importance of non-canonical substrate transport. This study provides a framework for investigating multiple transport systems of various trace micromolecules under physiological conditions and in multifactorial diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11037918PMC
http://dx.doi.org/10.7554/eLife.92615DOI Listing

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