Combined impact of lipidomic and genetic aberrations on clinical outcomes in metastatic castration-resistant prostate cancer

Mak, Blossom; Lin, Huiming; Kwan, Edmond M.; Fettke, Heidi; Davis, Ian D.; Mahon, Kate; Stockler, Martin R.; Briscoe, Karen; Marx, Gavin; Zhang, Alison; Crumbaker, Megan; Tan, Winston; Huynh, Kevin; Meikle, Thomas G.; Mellett, Natalie A.; Hoy, Andrew J.; Du, Pan; Yu, Jianjun; Jia, Shidong; Joshua, Anthony M.; Waugh, David J.; Butler, Lisa M.; Kohli, Manish; Meikle, Peter J.; Azad, Arun; Horvath, Lisa G.

doi:10.1186/s12916-022-02298-0

Cited by 13 publications

(22 citation statements)

References 48 publications

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“…Of note, statins can also alter tryptophan metabolism [ 24 ], either directly through their effects on cholesterol metabolism or indirectly via other targets in cytokine‐producing immune cells. A recent report highlighted the importance of the potential association between elevated circulating sphingolipids with genetic aberrations in metastatic CRPC, such as AR , TP53 and RB1 , and that a biomarker signature combining lipid and genetic abnormalities may be predictive of worse prognosis [ 25 ].…”

Section: Discussionmentioning

confidence: 99%

Phase II proof‐of‐concept study of atorvastatin in castration‐resistant prostate cancer

et al. 2022

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To test for evidence of statin-mediated effects in patients with castration-resistant prostate cancer (CRPC) as post-diagnosis use of statins in patients with prostate cancer is associated with favourable survival outcome. Patients and MethodsThe SPECTRE trial was a 6-weeks-long proof-of-concept single-arm Phase II treatment trial, combining atorvastatin and androgen deprivation therapy in patients with CRPC (regardless of metastatic status), designed to test for evidence of statin-mediated effects in patients with CRPC. The primary study endpoint was the proportion of patients achieving a ≥50% drop from baseline in prostate-specific antigen (PSA) levels at any time over the 6-week period of atorvastatin medication (PSA response). Exploratory endpoints include PSA velocity and serum metabolites identified by mass spectrometry . ResultsAt the scheduled interim analysis, one of 12 patients experienced a ≥50% drop in PSA levels (primary endpoint), with ≥2 patients satisfying the primary endpoint required for further recruitment. All 12 patients experienced substantial falls in serum cholesterol levels following statin treatment. While all patients had comparable pre-study PSA velocities, six of 12 patients showed decreased PSA velocities after statin treatment, suggestive of disease stabilization. Unbiased metabolomics analysis on serial weekly blood samples identified tryptophan to be the dominant metabolite associated with patient response to statin. ConclusionsData from the SPECTRE study provide the first evidence of statin-mediated effects on CRPC and early sign of disease stabilization. Our data also highlight the possibility of altered tryptophan metabolism being associated with tumour response.

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Section: Discussionmentioning

confidence: 99%

Phase II proof‐of‐concept study of atorvastatin in castration‐resistant prostate cancer

et al. 2022

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“…Bibliometric analyses of clinical lipidomics publications in 2022 using Scopus search terms “lipidomics” AND “clinic*” on 15 th December 2022 …”

Section: In Review: Materials and Methodsmentioning

confidence: 99%

“…Bibliometric analyses of clinical lipidomics publications in 2022 according to separation techniques, detectors, and RPLC columns used …”

Section: In Review: Materials and Methodsmentioning

confidence: 99%

“…[170][171][172][173] Lipidomic analyses have revealed cancer-specific lipid dysregulations that could potentially serve as promising biomarkers for screening purposes, 174,175 as demonstrated by Lee et al in a plasma analysis of 140 human samples that could differentiate five cancers (liver, lung, gastric, colorectal, and thyroid). 176 It is therefore of no surprise with its known lipid dysregulation and urgency that oncology was the biggest application area in 2022, where the following cancers were studied: bladder, 177 brain, 155 breast, [178][179][180][181][182] colorectal, [183][184][185][186][187][188] endometrial, 189 gallbladder, 190 gastric, 191 kidney, 192 liver, [193][194][195][196][197] lungs, 156,[198][199][200] nasopharyngeal, 201 ovarian, 202 paediatric, 203 prostate, 204,205 and skin. 206 To maximize the survival rates of cancer patients, it is important to identify cancer at its early stages, where tumours can be surgically removed or treated with milder drug regimens.…”

Section: Oncologymentioning

confidence: 99%

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Chewing the fat: How lipidomics is changing our understanding of human health and disease in 2022

Géhin

Fowler

Trivedi

2023

Analytical Science Advances

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Lipids are biological molecules that play vital roles in all living organisms. They perform many cellular functions, such as 1) forming cellular and subcellular membranes, 2) storing and using energy, and 3) serving as chemical messengers during intra‐ and inter‐cellular signal transduction. The large‐scale study of the pathways and networks of cellular lipids in biological systems is called “lipidomics” and is one of the fastest‐growing omics technologies of the last two decades. With state‐of‐the‐art mass spectrometry instrumentation and sophisticated data handling, clinical studies show how human lipid composition changes in health and disease, thereby making it a valuable medium to collect for clinical applications, such as disease diagnostics, therapeutic decision‐making, and drug development. This review gives a comprehensive overview of current workflows used in clinical research, from sample collection and preparation to data and clinical interpretations. This is followed by an appraisal of applications in 2022 and a perspective on the exciting future of clinical lipidomics.

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“…However, atrial fibrillation, frequent premature ventricular contractions, interrupted QTc, and refractory hypokalaemia was reported in an elderly patient with metastatic castra-tion-resistant prostate cancer who received abiraterone [74]. A most recent cell-free DNA sequencing and lipid profile analysis on 106 patients with metastatic castration-resistant prostate cancer who received different chemotherapeutics (e.g., abiraterone acetate and enzalutamide) showed aberrations in the androgen receptor, TP53, RB1, PI3K, and aggressive-variant prostate cancer along with lipid abnormalities [75] are well-known pieces of evidence to be risk factors for cardiovascular disorders [76]. Furthermore, a case report showed that the administration of abiraterone acetate to a 70-year-old male resulted in cardiovascular dysfunction and syncope [77] Similarly, ventricular repolarization is reported as a possible adverse effect of enzalutamide therapy in male patients with hypogonadism [88].…”

Section: Cardiotoxicity Of Second-generation Anti-androgensmentioning

confidence: 99%

Drug Resistance and Cardiovascular Safety of Second-Generation Anti-Androgens in Patients with Advanced Prostate Cancer

Raberi

Shariati

Abbasnezhad

et al. 2023

GMJ

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Prostate cancer is recognized as one of the most common cancers affecting the male population. The prostate is revealed to be a hormone-dependent tissue as testosterone and dihydrotestosterone could bind to the androgen receptor, activate it, and initiate the nuclear translocation of this receptor which is followed by subsequent signaling cascades. Regarding this androgen dependency of the prostate, it is believed that androgen deprivation therapies are able to confront aggressive prostate cancer as first-line treatment. However, prostate cancer could overcome hormone deprivation strategies through a number of cellular mechanisms, such as intratumoral androgen production and the production of ligand-independent androgen receptor splice variants, which are known clinically as castration-resistant prostate cancer. Due to the limited efficacy of first-generation antiandrogens in complete blockage of androgen receptor activity, recently, four second-generation anti-androgens, including abiraterone acetate, enzalutamide, apalutamide, and darolutamide approved by the Food and Drug Administration, and considered standard of care for patients with advanced prostate cancer. Nevertheless, prostate cancer cells may acquire drug-resistance mechanisms to overcome these novel chemotherapeutics. Furthermore, potential adverse effects on nontargeted organs such as the cardiovascular system, are possible. Hence, the current study aimed to review the efficacy and cardio-safety of these novel therapeutical strategies.

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Combined impact of lipidomic and genetic aberrations on clinical outcomes in metastatic castration-resistant prostate cancer

Cited by 13 publications

References 48 publications

Phase II proof‐of‐concept study of atorvastatin in castration‐resistant prostate cancer

Phase II proof‐of‐concept study of atorvastatin in castration‐resistant prostate cancer

Chewing the fat: How lipidomics is changing our understanding of human health and disease in 2022

Drug Resistance and Cardiovascular Safety of Second-Generation Anti-Androgens in Patients with Advanced Prostate Cancer

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