Beta-interferon, retinoids and tamoxifen in metastatic breast cancer: Long-term follow-up of a phase II study

Recchia, F.; Sica, Gigliola; Candeloro, Giampiero; Necozione, Stefano; Bisegna, R.; Bratta, Massimo; Rea, Silvio

doi:10.3892/or_00000317

Cited by 22 publications

(14 citation statements)

References 30 publications

(42 reference statements)

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“…Within the CTRA alterations, down-regulation of pro-inflammatory genes is notable because chronic inflammation is implicated in breast cancer progression and recurrence (Cole, 2009; Pierce et al, 2009). Further, enhanced expression of type I interferon-related genes - also encompassed in the CTRA composite - is associated with reduced breast cancer progression (Andersen et al, 2010; Recchia et al, 2009; Seth et al, 2003). It is plausible that other psychosocial interventions known to have positive effects on breast cancer disease recurrence may operate via similar mechanisms, though this requires empirical testing.…”

Section: Discussionmentioning

confidence: 99%

Stress management, leukocyte transcriptional changes and breast cancer recurrence in a randomized trial: An exploratory analysis

Antoni

Bouchard

Jacobs

et al. 2016

Psychoneuroendocrinology

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Purpose Cognitive behavioral stress management (CBSM) is an empirically-validated group-based psychosocial intervention. CBSM is related to decreased self-reported indicators of psychological adversity during breast cancer treatment and greater disease-free survival (DFS) vs. a control condition. This study examined relationships between CBSM, DFS, and a potential biobehavioral pathway linking these variables in breast cancer patients through a gene expression composite representing the leukocyte conserved transcriptional response to adversity (CTRA). Design Women with stage 0-IIIb breast cancer completed questionnaires and provided blood samples post-surgery. Participants were randomized to 10-week group-based CBSM or a psychoeducation control group and followed at 6 months, 12 months, and median 11 years. In total, 51 participants provided blood data for longitudinal analyses (CBSM n = 28; Control n = 23). Mixed model analyses examined CBSM effects on 6–12 month changes in CTRA expression (53 indicator genes representing pro-inflammatory, anti-viral and antibody production signaling). Cox regression models assessed the relationship between 6–12 month changes in CTRA expression and 11-year DFS. Results Patients randomized to CBSM showed attenuated 6–12 month change in CTRA gene expression, whereas patients randomized to control showed increased CTRA expression (p = 0.010). Average DFS was 5.92 years (SD = 3.90). Greater 6–12 month CTRA increases predicted shorter 11-year DFS controlling for covariates (p = 0.023). Conclusions CBSM attenuated CTRA gene expression during the initial year of breast cancer treatment. In turn, greater increases in CTRA gene expression predicted shorter long-term DFS. These findings identify a biobehavioral oncology pathway to examine in future work.

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Section: Discussionmentioning

confidence: 99%

Stress management, leukocyte transcriptional changes and breast cancer recurrence in a randomized trial: An exploratory analysis

Antoni

Bouchard

Jacobs

et al. 2016

Psychoneuroendocrinology

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“…Isotretinoin, alitretinoin and retinyl palmitate were also tested as therapies in late-stage post-menopausal breast cancer patients (Table 2). No potentiation in the effect of tamoxifen or a difference in survival was detected [75], although a clinical response was seen in 55% of the patients treated with retinyl palmitate [76]. Clinical benefit with bexarotene was documented in 20% of patients with hormone-refractory metastatic breast cancers, with lower toxicity than seen with retinoids [77].…”

Section: Medical Use Of Retinoids and Rexinoidsmentioning

confidence: 99%

Retinoids and rexinoids in cancer prevention: from laboratory to clinic

Uray

Dmitrovsky

Brown

2016

Seminars in Oncology

131

102

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Early in the age of modern medicine the consequences of vitamin A deficiency drew attention to the fundamental link between retinoid-dependent homeostatic regulation and malignant hyperproliferative diseases. The term retinoid includes a handful of endogenous and a large group of synthetic derivatives of vitamin A. These multifunctional lipid-soluble compounds directly regulate target genes of specific biological functions and critical signaling pathways to orchestrate complex functions from vision to development, metabolism and inflammation. Many of the retinoid activities on the cellular level have been well characterized and translated to the regulation of processes like differentiation and cell death, which play critical roles in the outcome of malignant transformation of tissues. In fact, retinoid-based differentiation therapy of acute promyelocytic leukemia was one of the first successful examples of molecularly targeted treatment strategies. The selectivity, high receptor binding affinity and the ability of retinoids to directly modulate gene expression programs present a distinct pharmacological opportunity for cancer treatment and prevention. However, to fully exploit their potential, the adverse effects of retinoids must be averted. In this review we provide an overview of the biology of retinoid (activated by nuclear retinoic acid receptors, RARs) and rexinoid (engaged by nuclear retinoid X receptors, RXRs) action concluded from a long line of preclinical studies, in relation to normal and transformed states of cells. We will also discuss the past and current uses of retinoids in the treatment of malignancies, the potential of rexinoids in the cancer prevention setting, both as single agents and in combinations.

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“…The combination of TAM with 13-cis-retinoic acid did not enhance the effects of the retinoid on patients with advanced breast cancer [26]. In a pilot phase II study, the combination of interferon, retinyl palmitate and TAM was studied as a salvage therapy in stage IV breast carcinoma patients [73]. Among 65 evaluable patients, 36 achieved a clinical response; toxicity was moderate and mainly hepatic [73].…”

Section: The Retinoid-antiestrogen Combined Effects and Their Therapementioning

confidence: 99%

Interplay between estrogen and retinoid signaling in breast cancer – Current and future perspectives

Ribeiro¹,

Santos²,

Custódio³

2014

Cancer Letters

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Beta-interferon, retinoids and tamoxifen in metastatic breast cancer: Long-term follow-up of a phase II study

Cited by 22 publications

References 30 publications

Stress management, leukocyte transcriptional changes and breast cancer recurrence in a randomized trial: An exploratory analysis

Stress management, leukocyte transcriptional changes and breast cancer recurrence in a randomized trial: An exploratory analysis

Retinoids and rexinoids in cancer prevention: from laboratory to clinic

Interplay between estrogen and retinoid signaling in breast cancer – Current and future perspectives

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