Your search keyword '"Tsakiridis, Theodoros"' showing total 12 results

1. Prostate-Specific Membrane Antigen (PSMA) Expression Predicts Need for Early Treatment in Prostate Cancer Patients Managed with Active Surveillance.

Author

Ahmadi, Elham, Wang, Simon, Gouran-Savadkoohi, Mohammad, Douvi, Georgia, Isfahanian, Naghmeh, Tsakiridis, Nicole, Faught, Brent E., Cutz, Jean-Claude, Sur, Monalisa, Chawla, Satish, Pond, Gregory R., Steinberg, Gregory R., Brown, Ian, and Tsakiridis, Theodoros

Subjects

PROSTATE cancer patients, WATCHFUL waiting, FOLIC acid, CANCER treatment, GLEASON grading system, GLUCOSE transporters

Abstract

Metabolic dysregulation is an early event in carcinogenesis. Here, we examined the expression of enzymes involved in de novo lipogenesis (ATP-citrate lyase: ACLY), glucose uptake (Glucose Transporter 1: GLUT1), and folate–glutamate metabolism (Prostate-Specific Membrane Antigen: PSMA) as potential biomarkers of risk for early prostate cancer progression. Patients who were managed initially on active surveillance with a Gleason score of 6 or a low-volume Gleason score of 7 (3 + 4) were accrued from a prostate cancer diagnostic assessment program. Patients were asked to donate their baseline diagnostic biopsy tissues and permit access to their clinical data. PSMA, GLUT1, and ACLY expression were examined with immunohistochemistry (IHC) in baseline biopsies, quantitated by Histologic Score for expression in benign and malignant glands, and compared with patient time remaining on active surveillance (time-on-AS). All three markers showed trends for elevated expression in malignant compared to benign glands, which was statistically significant for ACLY. On univariate analysis, increased PSMA and GLUT1 expression in malignant glands was associated with shorter time-on-AS (HR: 5.06, [CI 95%: 1.83–13.94] and HR: 2.44, [CI 95%: 1.10–5.44], respectively). Malignant ACLY and benign gland PSMA and GLUT1 expression showed non-significant trends for such association. On multivariate analysis, overexpression of PSMA in malignant glands was an independent predictor of early PC progression (p = 0.006). This work suggests that the expression of metabolic enzymes determined by IHC on baseline diagnostic prostate biopsies may have value as biomarkers of risk for rapid PC progression. PSMA may be an independent predictor of risk for progression and should be investigated further in systematic studies. [ABSTRACT FROM AUTHOR]

Published

2023

2. The SGLT2 inhibitor canagliflozin suppresses growth and enhances prostate cancer response to radiotherapy.

Author

Ali, Amr, Mekhaeil, Bassem, Biziotis, Olga-Demetra, Tsakiridis, Evangelia E., Ahmadi, Elham, Wu, Jianhan, Wang, Simon, Singh, Kanwaldeep, Menjolian, Gabe, Farrell, Thomas, Mesci, Aruz, Liu, Stanley, Berg, Tobias, Bramson, Jonathan L., Steinberg, Gregory R., and Tsakiridis, Theodoros

Subjects

SODIUM-glucose cotransporter 2 inhibitors, DOSE-response relationship (Radiation), ANDROGEN receptors, CANCER radiotherapy, CANAGLIFLOZIN, PROSTATE cancer, AMP-activated protein kinases

Abstract

Radiotherapy is a non-invasive standard treatment for prostate cancer (PC). However, PC develops radio-resistance, highlighting a need for agents to improve radiotherapy response. Canagliflozin, an inhibitor of sodium-glucose co-transporter-2, is approved for use in diabetes and heart failure, but is also shown to inhibit PC growth. However, whether canagliflozin can improve radiotherapy response in PC remains unknown. Here, we show that well-tolerated doses of canagliflozin suppress proliferation and survival of androgen-sensitive and insensitive human PC cells and tumors and sensitize them to radiotherapy. Canagliflozin blocks mitochondrial respiration, promotes AMPK activity, inhibits the MAPK and mTOR-p70S6k/4EBP1 pathways, activates cell cycle checkpoints, and inhibits proliferation in part through HIF-1α suppression. Canagliflozin mediates transcriptional reprogramming of several metabolic and survival pathways known to be regulated by ETS and E2F family transcription factors. Genes downregulated by canagliflozin are associated with poor PC prognosis. This study lays the groundwork for clinical investigation of canagliflozin in PC prevention and treatment in combination with radiotherapy. The anti-diabetic drug canagliflozin promotes sensitivity to radiotherapy in prostate cancer by blocking mitochondrial respiration and repressing the mTORC1- HIF-1α pathway. [ABSTRACT FROM AUTHOR]

Published

2023

3. The Journey of Radiotherapy Dose Escalation in High Risk Prostate Cancer; Conventional Dose Escalation to Stereotactic Body Radiotherapy (SBRT) Boost Treatments.

Author

Mesci, Aruz, Isfahanian, Naghmeh, Dayes, Ian, Lukka, Himu, and Tsakiridis, Theodoros

Subjects

STEREOTACTIC radiotherapy, PROSTATE cancer treatment, RADIATION dosimetry, CANCER relapse, TREATMENT effectiveness

Abstract

High risk prostate cancer (HR-PrCa) is a subset of localized PrCa with significant potential for morbidity and mortality associated with disease recurrence and metastasis. Radiotherapy combined with Androgen Deprivation Therapy has been the standard of care for many years in HR-PrCa. In recent years, dose escalation, hypo-fractionation and high precision delivery with immobilization and image-guidance have substantially changed the face of modern PrCa radiotherapy, improving treatment convenience and outcomes. Ultra-hypo-fractionated radiotherapy delivered with high precision in the form of stereotactic body radiation therapy (SBRT) combines delivery of high biologically equivalent dose radiotherapy with the convenience of a shorter treatment schedule, as well as the promise of similar efficacy and reduced toxicity compared to conventional radiotherapy. However, rigorous investigation of SBRT in HR-PrCa remains limited. Here, we review the changes in HR-PrCa radiotherapy through dose escalation, hypo- and ultra-hypo-fractionated radiotherapy boost treatments, and the radiobiological basis of these treatments. We focus on completed and on-going trials in this disease utilizing SBRT as a sole radiation modality or as boost therapy following pelvic radiation. [ABSTRACT FROM AUTHOR]

Published

2022

4. 18F-DCFPyL (PSMA) PET as a Radiotherapy Response Assessment Tool in Metastatic Prostate Cancer.

Author

Gouran-savadkoohi, Mohammad, Tsakiridis, Theodoros, Ahmadi, Elham, and Mesci, Aruz

Subjects

*CASTRATION-resistant prostate cancer, *ANDROGEN receptors, *POSITRON emission tomography, *ANDROGEN deprivation therapy, *PROSTATE tumors, *PROSTATE cancer

Abstract

Introduction: Prostate Specific Membrane Antigen (PSMA) - positron emission tomography (PET) guides metastasis - directed radiotherapy (MDRT) in prostate cancer (PrCa). However, its value as a treatment response assessment tool after MDRT remains unclear. Importantly, there is limited understanding of the potential of radiotherapy (RT) to alter PSMA gene (folate hydrolase 1; FOLH1) expression. Methods: We reviewed a series of 11 men with oligo - metastatic PrCa (25 metastasis sites) treated with MDRT before re - staging with 18F - DCFPyL (PSMA) PET upon secondary recurrence. Acute effects of RT on PSMA protein and mRNA levels were examined with qPCR and immunoblotting in human wild - type androgen - sensitive (LNCap), castrate - resistant (22RV1) and castrate - resistant neuroendocrine (PC3 and DU145) PrCa cell lines. Xenograft tumors were analyzed with immunohistochemistry. Further, we examined PSMA expression in untreated and irradiated radio - resistant (RR) 22RV1 (22RV1 - RR) and DU145 (DU145 - RR) cells and xenografts selected for survival after high - dose R. Results: The majority of MDRT - treated lesions showed lack of PSMA - PET/CT avidity, suggesting treatment response even after low biological effective dose (BED) MDRT. We observed similar high degree of heterogeneity of PSMA expression in both human specimens and in xenograft tumors. PSMA was highly expressed in LNCap and 22RV1 cells and tumors but not in the neuroendocrine PC3 and DU145 models. Single fraction RT caused detectable reduction in PSMA protein but not in mRNA levels in LNCap cells and did not significantly alter PSMA protein or mRNA levels in tissue culture or xenografts of the other cell lines. However, radio - resistant 22RV1 - RR cells and tumors demonstrated marked decrease of PSMA transcript and protein expression over their parental counterparts. Conclusions: PSMA - PET may be a promising tool to assess RT response in oligo - metastatic PrCa. However, future systematic investigation of this concept should recognize the high degree of heterogeneity of PSMA expression within prostate tumors and the risk for loss of PSMA expression in tumor surviving curative courses of RT. [ABSTRACT FROM AUTHOR]

Published

2024

5. Radiographic and metabolic evolution of prostate cancer lung metastasis detected by prostate-specific membrane antigen and fluoro-2-deoxy-D-glucose positron emission tomography/computed tomography.

Author

Tsakiridis, Theodoros, Bonert, Michael, Zukotynski, Katherine, and Anagnostopoulos, Alexander

Subjects

*POSITRON emission tomography computed tomography, *COMPUTED tomography, *PROSTATE-specific membrane antigen, *METASTASIS, *LUNG cancer, *PROSTATE cancer, *CASTRATION-resistant prostate cancer

Abstract

We describe the case of a 75-year-old patient who progressed over a 12-year period from localized to symptomatic metastatic prostate cancer (PrCa) with lung as the sole organ of involvement. In this case, the specific sequence of positron emission tomography (PET)-based next-generation imaging with 18F-sodium fluoride-, 18F-fluoro-2-deoxy-D-glucose-, and 18F-DCFPyL PET/computed tomography and biopsies allowed illustration of the pathway of disease progression from nonglycolytic hormone-sensitive PrCa to glycolytic castrate-resistant PrCa without neuroendocrine features. The observations provide a unique insight into the timelines of anatomical and metabolic progression of metastatic PrCa. They highlight the value of close radiographic surveillance of metastatic PrCa with modern imaging to guide early treatment interventions. [ABSTRACT FROM AUTHOR]

Published

2020

6. The diabetes medication Canagliflozin reduces cancer cell proliferation by inhibiting mitochondrial complex-I supported respiration.

Author

Villani, Linda A., Smith, Brennan K., Marcinko, Katarina, Ford, Rebecca J., Broadfield, Lindsay A., Green, Alex E., Houde, Vanessa P., Muti, Paola, Tsakiridis, Theodoros, and Steinberg, Gregory R.

Abstract

Objective The sodium-glucose transporter 2 (SGLT2) inhibitors Canagliflozin and Dapagliflozin are recently approved medications for type 2 diabetes. Recent studies indicate that SGLT2 inhibitors may inhibit the growth of some cancer cells but the mechanism(s) remain unclear. Methods Cellular proliferation and clonogenic survival were used to assess the sensitivity of prostate and lung cancer cell growth to the SGLT2 inhibitors. Oxygen consumption, extracellular acidification rate, cellular ATP, glucose uptake, lipogenesis, and phosphorylation of AMP-activated protein kinase (AMPK), acetyl-CoA carboxylase, and the p70S6 kinase were assessed. Overexpression of a protein that maintains complex-I supported mitochondrial respiration (NDI1) was used to establish the importance of this pathway for mediating the anti-proliferative effects of Canagliflozin. Results Clinically achievable concentrations of Canagliflozin, but not Dapagliflozin, inhibit cellular proliferation and clonogenic survival of prostate and lung cancer cells alone and in combination with ionizing radiation and the chemotherapy Docetaxel. Canagliflozin reduced glucose uptake, mitochondrial complex-I supported respiration, ATP, and lipogenesis while increasing the activating phosphorylation of AMPK. The overexpression of NDI1 blocked the anti-proliferative effects of Canagliflozin indicating reductions in mitochondrial respiration are critical for anti-proliferative actions. Conclusion These data indicate that like the biguanide metformin, Canagliflozin not only lowers blood glucose but also inhibits complex-I supported respiration and cellular proliferation in prostate and lung cancer cells. These observations support the initiation of studies evaluating the clinical efficacy of Canagliflozin on limiting tumorigenesis in pre-clinical animal models as well epidemiological studies on cancer incidence relative to other glucose lowering therapies in clinical populations. [ABSTRACT FROM AUTHOR]

Published

2016

7. 23 Stereotactic Body Versus Conventional Fractionation External Beam Radiotherapy (EBRT) Boost for High-Risk Prostate Cancer (HR-PC); Early Results of PBS: A Phase II Randomized Trial (NCT03380806).

Author

Gouveia, Andre, Mesci, Aruz, Isfahanian, Naghmeh, Dayes, Ian, Schnarr, Kara Lynne, Quan, Kimmen, Maharaj, Lindsay, Cuthbert, David, Hallock, Abhiram, Douvi, Georgia, Lukka, Himu, Goldberg, Mira, Wright, Jim, Swaminath, Anand, Chow, Tom, Diamond, Kevin, Ewusie, Joycelyne, Hajdok, George, and Tsakiridis, Theodoros

Subjects

*EXTERNAL beam radiotherapy, *PROSTATE cancer

Published

2024

8. 124 Phase II Randomized Trial of Optimal Recurrence-Directed Therapy (RDT) Without or with Androgen-Deprivation Therapy (ADT) in Radio-Recurrent Oligo-Metastatic Hormone/Castrate Sensitive Prostate Cancer (romCSPC): The OCOG-Rational-PCS Trial.

Author

Gouveia, Andre, Vavassis, Peter, Mesci, Aruz, Hotte, Sebastien, Berlin, Alejandro, Zukotynski, Katherine, Morgan, Scott, Dayes, Ian, Perlis, Nathan, Wright, Jim, Pond, Gregory, Niazi, Tamim, and Tsakiridis, Theodoros

Subjects

*PROSTATE cancer, *HORMONES

Published

2024

9. The Diabetes Drug Canagliflozin Enhances the Response of Prostate Cancer to Radiotherapy

Author

Mekhaeil, Bassem, Tsakiridis, Theodoros, and Health Sciences

Subjects

Radiation, Metabolism, Prostate Cancer, Canagliflozin

Abstract

Canagliflozin (CANA) is a sodium-glucose co-transporter 2 (SGLT2) inhibitor used for the treatment of type II diabetes. There is recent evidence suggesting that Canagliflozin has antiproliferative effects against malignant tumours. Canagliflozin is able to inhibit cell growth and cancer progression by inhibiting mitochondrial complex I leading to a reduction in cellular ATP levels. This alteration in the energy status of the cell leads to AMP-activated kinase (AMPK) activation, which in turn downregulates protein synthesis, lipogenesis and induces cell cycle arrest. The aim of this thesis is to explore whether Canagliflozin can be combined with radiation to enhance the outcome of radiation therapy in the treatment of prostate cancer and to further our knowledge on the cellular pathways impacted by Canagliflozin. Proliferation and clonogenic survival assays were used to establish the antiproliferative effect of Canagliflozin in vitro alone and when combined with radiation. Prostate cancer cell lines with different mutation profiles were used to assess the effectiveness of the drug under different radiation doses. A xenograft model was then used to test Canagliflozin’s effects in vivo. PC-3 cells were injected in the flank of balb/c nude mice. Mice were treated with Canagliflozin, radiation or a combined treatment and tumour growth was monitored. Furthermore, a western blot analysis of cells treated with Canagliflozin and radiation was performed to deepen our understanding of the cellular pathways affected by Canagliflozin. Our results show that Canagliflozin has an additive effect when combined with radiation. Canagliflozin was able to effectively downregulate the mTOR pathway, blocking mitosis and leading to cell cycle arrest. These findings provide evidence that Canagliflozin could be used as an adjunct to radiation therapy in clinical settings. Thesis Master of Science in Medical Sciences (MSMS) Radiation therapy is a key therapy for prostate cancer. Although it is very effective at treating early stages of prostate cancer, prostate cancer cells develop resistance to radiation therapy rendering it less effective. One way to overcome this obstacle is by delivering higher doses of radiotherapy. However, this leads to increased side effects caused by radiation on normal tissues surrounding the prostate. An additional potential solution to this problem is administering a drug that can make cancer cells more sensitive to radiotherapy. This way we can deliver lower doses of radiation to avoid side effects while treating the disease. This study focuses on using a drug called Canagliflozin in combination with radiation in order to improve the outcomes of radiotherapy in prostate cancer.

Published

2020

10. 206: A Randomized Phase Ii Trial of Prostate Boost Irradiation with Stereotactic Body Radiotherapy (SBRT) in High-Risk Prostate Cancer. The Pbs Trial.

Author

Douvi, Georgia, Isfahanian, Naghmeh, Lukka, Himanshu, IanDayes, Quan, Kimmen, Schnarr, Kara Lynne, Goldberg, Mira, Wright, Jim, Hallock, Abhirami, Ishkanian, Adrian, Cuthbert, David, Swaminath, Anand, Chow, Tom, Diamond, Kevin, Cutz, Jean-Claude, Kavsak, Peter, Thabane, Lehana, and Tsakiridis, Theodoros

Subjects

*STEREOTACTIC radiotherapy, *PROSTATE cancer, *PROSTATE, *IRRADIATION

Published

2020

11. 18: PSMA-PET-Based Response Assessment of Metastatic Prostate Cancer Response to Radiotherapy: A Case Series.

Author

Mesci, Aruz, Gouran-Savadkoohi, Mohammad, Greenspoon, Jeffrey, Kapoor, Anil, Lukka, Himanshu, and Tsakiridis, Theodoros

Subjects

*CANCER radiotherapy, *METASTASIS, *PROSTATE cancer

Published

2021

12. 151: Prostate SBRT Boost Radiotherapy (PBS Trial): A Randomized Phase II Trial of SBRT Versus Conventionally-Fractionated Radiotherapy Boost Following Pelvic Radiotherapy in High-Risk Prostate Cancer.

Author

Mesci, Aruz, Isfahanian, Naghmeh, Douvi, Georgia, Gouran-Savadkoohi, Mohammad, Dayes, Ian, Lukka, Himanshu, Quan, Kimmen, Schnarr, Kara, Goldberg, Mira, Hallock, Abhirami, Chow, Tom, Diamond, Kevin, Jakubovic, Raphael, Thabane, Lahane, and Tsakiridis, Theodoros

Subjects

*PROSTATE cancer, *PROSTATE, *RADIOTHERAPY

Published

2021