Metabolomic profiles delineate potential role for sarcosine in prostate cancer progression

Sreekumar, Arun; Poisson, Laila; Rajendiran, Thekkelnaycke M.; Khan, Amjad P.; Cao, Qi; Yu, Jindan; Laxman, Bharathi; Mehra, Rohit; Lonigro, Robert J.; Li, Yong; Nyati, Mukesh K.; Ahsan, Aarif; Kalyana-Sundaram, Shanker; Han, Bo; Cao, Xuhong; Byun, Jaeman; Omenn, Gilbert S.; Ghosh, Debashis; Pennathur, Subramaniam; Alexander, Danny; Berger, Alvin; Shuster, Jeffrey R.; Wei, John T.; Varambally, Sooryanarayana; Beecher, Christopher W.W.; Chinnaiyan, Arul M.

doi:10.1038/nature07762

Cited by 1,932 publications

(1,764 citation statements)

References 19 publications

(28 reference statements)

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“…In this study, any of sarcosine algorithms was significantly higher in PCa than in NEM patients not only in all patients (Figures 1a and d) but also in patients with PSA o20 ng ml À1 (data not shown), supporting the report by Sreekumar et al 8 and simultaneously opposing the study by Jentzmik et al 9 As urinary creatinine concentration of patients with NEM did not differ from that of PCa patients in both groups ( Supplementary Figure 1), the creatinine normalization could not be the reason for this contradictory result. These inconsistent results might be explained by differences between the study populations or in pathological evaluation of specimens.…”

Section: Efforts To Solve Controversy In Sarcosine D-l Cao Et Alsupporting

confidence: 91%

“…25 Interestingly, a recent report in Nature by Sreekumar et al 8 demonstrated that sarcosine as one of metabolites offers a promising, non-invasive diagnostic and prognostic test for PCa. However, the first validation study 9 did not support that sarcosine has any advantage over serum PSA, %fPSA, Gleason score and tumor stage.…”

Section: Discussionmentioning

confidence: 99%

“…3,4 To the best of our knowledge, metabolomic analysis has already been used for identifying metabolic markers in tumors. [5][6][7] Notably, Sreekumar et al 8 demonstrated that sarcosine can be used as a biomarker for PCa and was non-invasively detected in urine, which led to great interest in the scientific community and among potential PCa patients. However, the first independent validation study 9 showed that sarcosine cannot be used as a biomarker to diagnose PCa and predict its aggression.…”

Section: Introductionmentioning

confidence: 99%

“…Following these observations, letters and replies [10][11][12][13][14][15][16] were published to discuss potential reasons for the contradictions between these two studies. 8,9 Although many possibilities (for example, the analytical method, the biomarker assay, the comparators and the study cohort) were discussed; no data from complete article has been reported.…”

Section: Introductionmentioning

confidence: 99%

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Efforts to resolve the contradictions in early diagnosis of prostate cancer: a comparison of different algorithms of sarcosine in urine

Cao

Zhu

et al. 2011

Prostate Cancer Prostatic Dis

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Controversial data on sarcosine as a promising biomarker for prostate cancer (PCa) detection are present. The objective was to clarify these discrepancies and reevaluate the potential value of sarcosine in PCa. Sarcosine algorithms (supernatant and sediment sarcosine/creatinine, supernatant and sediment log2 (sarcosine/alanine)) in urine samples from 71 untreated patients with PCa, 39 patients with no evidence of malignancy (NEM) and 20 healthy women and men were quantified by liquid chromatography/tandem mass spectrometry. Although any sarcosine algorithms were significantly higher in PCa patients than in NEM patients (all Po0.05), comparable sarcosine values were measured in healthy women and men. Additionally, neither biopsy Gleason score nor clinical T-stage were correlated with sarcosine algorithms (all P40.05), and receiver operating characteristic curve analysis indicated that the diagnostic power of any of sarcosine algorithms was nonsignificantly higher than that of serum and urine PSA, but nonsignificantly lower than prostate cancer antigen 3 (PCA3) and the percent-free PSA (%fPSA). Improved diagnostic performances were observed when any of sarcosine algorithms was combined with PCA3 or %fPSA. In conclusion, the predictive power of sarcosine in PCa is modest compared with PCA3 and %fPSA. Sarcosine, which awaits more validation before it reaches the clinic, could be included into the list of candidate PCa biomarkers.

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Section: Efforts To Solve Controversy In Sarcosine D-l Cao Et Alsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Efforts to resolve the contradictions in early diagnosis of prostate cancer: a comparison of different algorithms of sarcosine in urine

Cao

Zhu

et al. 2011

Prostate Cancer Prostatic Dis

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“…Overexpression of full length, transmembrane TMEFF2 in PCa cells impairs proliferation due to an interaction between the cytoplasmic domain of TMEFF2 and sarcosine dehydrogenase (SARDH). This interaction results in decreased levels of sarcosine (Chen et al, 2011a; Green et al, 2013), an amino acid associated with PCa progression (Sreekumar et al, 2009). Full length TMEFF2 also attenuates the migratory properties of PCa cells (Chen et al, 2014), indicating a tumour suppressor function.…”

Section: Introductionmentioning

confidence: 99%

TMEFF2 shedding is regulated by oxidative stress and mediated by ADAMs and transmembrane serine proteases implicated in prostate cancer

Gaweł-Bęben

Ali

Ellis

et al. 2017

Cell Biology International

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TMEFF2 is a type I transmembrane protein with two follistatin (FS) and one EGF‐like domain over‐expressed in prostate cancer; however its biological role in prostate cancer development and progression remains unclear, which may, at least in part, be explained by its proteolytic processing. The extracellular part of TMEFF2 (TMEFF2‐ECD) is cleaved by ADAM17 and the membrane‐retained fragment is further processed by the gamma‐secretase complex. TMEFF2 shedding is increased with cell crowding, a condition associated with the tumour microenvironment, which was mediated by oxidative stress signalling, requiring jun‐kinase (JNK) activation. Moreover, we have identified that TMEFF2 is also a novel substrate for other proteases implicated in prostate cancer, including two ADAMs (ADAM9 and ADAM12) and the type II transmembrane serine proteinases (TTSPs) matriptase‐1 and hepsin. Whereas cleavage by ADAM9 and ADAM12 generates previously identified TMEFF2‐ECD, proteolytic processing by matriptase‐1 and hepsin produced TMEFF2 fragments, composed of TMEFF2‐ECD or FS and/or EGF‐like domains as well as novel membrane retained fragments. Differential TMEFF2 processing from a single transmembrane protein may be a general mechanism to modulate transmembrane protein levels and domains, dependent on the repertoire of ADAMs or TTSPs expressed by the target cell.

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Sarcosine is a prostate epigenetic modifier that elicits aberrant methylation patterns through the SAMe‐Dnmts axis

et al. 2019

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DNA hypermethylation is one of the most common epigenetic modifications in prostate cancer ( PC a). Several studies have delineated sarcosine as a PC a oncometabolite that increases the migration of malignant prostate cells while decreasing their doubling time. Here, we show that incubation of prostate cells with sarcosine elicited the upregulation of sarcosine N‐demethylation enzymes, sarcosine dehydrogenase and pipecolic acid oxidase. This process was accompanied by a considerable increase in the production of the major methyl‐donor S ‐adenosylmethionine ( SAM e), together with an elevation of cellular methylation potential. Global DNA methylation analyses revealed increases in methylated CpG islands in distinct prostate cell lines incubated with sarcosine, but not in cells of nonprostate origin. This phenomenon was further associated with marked upregulation of DNA methyltransferases (Dnmts). Epigenetic changes were recapitulated through blunting of Dnmts using the hypomethylating agent 5‐azacytidine, which was able to inhibit sarcosine‐induced migration of prostate cells. Moreover, spatial mapping revealed concomitant increases in sarcosine, SAM e and Dnmt1 in histologically confirmed malignant prostate tissue, but not in adjacent or nonmalignant tissue, which is in line with the obtained in vitro data. In summary, we show here for the first time that sarcosine acts as an epigenetic modifier of prostate cells and that this may contribute to its oncometabolic role.

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Metabolomic profiles delineate potential role for sarcosine in prostate cancer progression

Cited by 1,932 publications

References 19 publications

Efforts to resolve the contradictions in early diagnosis of prostate cancer: a comparison of different algorithms of sarcosine in urine

Efforts to resolve the contradictions in early diagnosis of prostate cancer: a comparison of different algorithms of sarcosine in urine

TMEFF2 shedding is regulated by oxidative stress and mediated by ADAMs and transmembrane serine proteases implicated in prostate cancer

Sarcosine is a prostate epigenetic modifier that elicits aberrant methylation patterns through the SAMe‐Dnmts axis

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