Abstract
Male hypogonadism associated with insulin resistance (IR) very often leads to metabolic syndrome, at variance with hypogonadism in its first stadium of insulin sensitivity (IS). A plasma metabolomic investigation of these patients can provide useful information in comparison with the values of IS patients. To this aim plasma from insulin-resistant males with hypogonadism were analysed by using ultra high-performance liquid chromatography (UHPLC) and high-resolution mass spectrometry (HRMS). Thus, metabolites were compared to the controls through multivariate statistical analysis and grouped by metabolic pathways. Metabolite database searches and pathway analyses identified imbalances in 18–20 metabolic pathways. Glucose metabolism (e.g., glycolysis and the Krebs cycle) is fuelled by amino acids degradation, in particular of branched amino acids, in individuals with lean body mass. Gluconeogenesis is strongly activated. Some crucial pathways such as glycerol are skewed. Mitochondrial electron transport is affected with a reduction in ATP production. Beta-oxidation of short and medium chain fatty acids did not represent an energy source in hypogonadism, at variance with long and branched fatty acids, justifying the increase in fat mass. Carnosine and β-alanine are strongly reduced resulting in increased fatigue and mental confusion. A comparison of IR with IS male hypogonadism will contribute to a better understanding of how these two hormones work in synergy or antagonise each other in humans. It could also help to select patients who will respond to hormone treatment, and provide accurate biomarkers to measure the response to treatment eventually leading to better strategies in preventing systemic complications in patients not fit for hormone replacement therapy.
Highlights
Male hypogonadism is a disorder characterised by low levels of the hormone testosterone, which can arise from various testicular and central causes[1]
Metabolic profiling of plasma using highresolution mass spectrometry (HRMS) To explore the metabolic differences between the two participant groups, 15 control subjects and 15 insulin resistance (IR) hypogonadal patients were analysed, and multivariate statistical analyses were employed on the HPLC-MS data set
To identify which metabolic pathways were mostly affected in IR male hypogonadism, we performed an overview of pathways analysis according to p-values from their enrichment and impact values
Summary
Male hypogonadism is a disorder characterised by low levels of the hormone testosterone, which can arise from various testicular (primary) and central (secondary) causes[1]. It can present symptoms and signs related to the sexual sphere, such as reduced libido, erectile dysfunction, decreased volume of ejaculate, and infertility, as well as involving the whole organism, such as reduced muscle strength, reduced bone strength, anaemia, and low mood (sadness, sense of hopelessness, profound sense of fault, etc.)[2]. A metabolic investigation of plasma from hypogonadic men before and after testosterone treatment could shed light on the molecular mechanisms of this condition, as well as on related biochemical pathways accounting for the overall benefit in insulin sensitivity observed in clinical trials
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
