4.7 Article

Metabolomic Analysis Reveals a Unique Urinary Pattern in Normozoospermic Infertile Men

Journal

JOURNAL OF PROTEOME RESEARCH
Volume 13, Issue 6, Pages 3088-3099

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/pr5003142

Keywords

biomarkers; male infertility; metabolomics; multivariate analysis; normozoospermic infertility; urine

Funding

  1. Chinese Academy of Sciences (CAS) Knowledge Innovation Programs [KZCX2-EW-QN408]
  2. NSFC foundation [21177123, 21307126]
  3. NSFC-RC International Exchange Programme
  4. Natural Environment Research Council [ceh010010] Funding Source: researchfish

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Normozoospermic infertility has become a common and important health problem worldwide. We designed this metabolomic case-control study to investigate the possible mechanism and urinary biomarkers of normozoospermic infertility. Normozoospermic infertile cases (n = 71) and fertile controls (n = 47) were recruited. A urinary metabolome pattern could discriminate normozoospermic infertile cases from fertile controls. A total of 37 potential biomarkers were identified; these have functionally important roles in energy production, antioxidation, and hormone regulation in spermatogenesis. This gave rise to a combined biomarker pattern of leukotriene E-4, 3-hydroxypalmitoylcarnitine, aspartate, xanthosine, and methoxytryptophan pointing to a diagnostic capability (AUC = 0.901, sensitivity = 85.7%, and specificity = 86.8%) in a ROC model; these markers may highlight keynote events of normozoospermic infertility. Stalled medium- and long-chain fatty acid metabolism with improved ketone body metabolism, plus decreased levels of malate and aspartate could result in citrate cycle alterations via a malate-aspartate shuttle in ATP generation in spermatogenesis. Inhibitory alterations in the normal hormone-secreting activity in spermatogenesis were suggested in normozoospermic infertility. Folate deficiency and oxidative stress may jointly impact infertile patients. The disruption of eicosanoid metabolism and xanthine oxidase system, which were tightly associated with energy metabolism and oxidative stress, was also a potential underlying mechanism. In addition, depression might be associated with normozoospermic infertility via neural activity-related metabolites. This study suggests that the urinary metabolome can be used to differentiate normozoospermic infertile men from fertile individuals. Potential metabolic biomarkers derived from these analyses might be used to diagnose what remains a somewhat idiopathic condition and provide functional insights into its pathogenesis.

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