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The Emerging Clinical Role of Spermine in Prostate Cancer

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MDPI
DOI: 10.3390/ijms22094382

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prostate cancer; spermine; polyamine; cancer metabolism; biomarker

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Decreased levels of spermine in prostate cancer compared to benign tissue may serve as an indicator of malignant transformation, with potential applications in therapy and chemoprevention. Ongoing research suggests a complex relationship between spermine metabolism and prostate cancer pathophysiology, offering new opportunities for diagnostic and therapeutic interventions.
Spermine, a member of polyamines, exists in all organisms and is essential for normal cell growth and function. It is highly expressed in the prostate compared with other organs and is detectable in urine, tissue, expressed prostatic secretions, and erythrocyte. A significant reduction of spermine level was observed in prostate cancer (PCa) tissue compared with benign prostate tissue, and the level of urinary spermine was also significantly lower in men with PCa. Decreased spermine level may be used as an indicator of malignant phenotype transformation from normal to malignant tissue in prostate. Studies targeting polyamines and key rate-limiting enzymes associated with spermine metabolism as a tool for PCa therapy and chemoprevention have been conducted with various polyamine biosynthesis inhibitors and polyamine analogues. The mechanism between spermine and PCa development are possibly related to the regulation of polyamine metabolism, cancer-driving pathways, oxidative stress, anticancer immunosurveillance, and apoptosis regulation. Although the specific mechanism of spermine in PCa development is still unclear, ongoing research in spermine metabolism and its association with PCa pathophysiology opens up new opportunities in the diagnostic and therapeutic roles of spermine in PCa management.

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