Statins and endocrine resistance in breast cancer

Hyder, Tara; Martí, Juan; Nasrazadani, Azadeh; Brufsky, Adam

doi:10.20517/cdr.2020.112

Cited by 10 publications

(10 citation statements)

References 51 publications

(68 reference statements)

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“…Active GTP-loaded Rab promotes GLUT4 translocation to the plasma membrane. Active AMPK can also mediate the emergence of more active GTP-loaded Rab [43,47,48]. The prenylation of small GTPases may be depleted over time via the inhibition of the mevalonate pathway and even by an increase in HMGCR expression, as we showed recently by Grunwald et al in 2020 under statin treatment [26].…”

Section: Discussionmentioning

confidence: 63%

“…However, this is different for muscle, which may switch to an alternative pathway for GLUT4 translocation [43]. Statins inhibit the formation of isoprenoids and thus farnesyl and geranylgeranyl pyrophosphates, from the mevalonate pathway and required for small GTPase prenylation, are reduced [43,47]. RabGTPases are hydrophobically prenylated by Rab geranylgeranyl transferase to bind to their target membrane structures, such as GLUT4 vesicles, and to direct the translocation of GLUT4 [48,49].…”

Section: Discussionmentioning

confidence: 99%

“…Muscle cryosection GLUT4 immunostaining was performed as previously described [47]. Briefly, after fixation and permeabilization, sections were stained with rabbit GLUT4 antiserum followed by incubation with biotin-conjugated Fab2 and streptavidin-Cy3 (Table 2).…”

Section: Immunofluorescencementioning

confidence: 99%

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Statins Aggravate the Risk of Insulin Resistance in Human Muscle

Grunwald

Haafke

Grieben

et al. 2022

IJMS

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Beside their beneficial effects on cardiovascular events, statins are thought to contribute to insulin resistance and type-2 diabetes. It is not known whether these effects are long-term events from statin-treatment or already triggered with the first statin-intake. Skeletal muscle is considered the main site for insulin-stimulated glucose uptake and therefore, a primary target for insulin resistance in the human body. We analyzed localization and expression of proteins related to GLUT4 mediated glucose uptake via AMPKα or AKT in human skeletal muscle tissue from patients with statin-intake >6 months and in primary human myotubes after 96 h statin treatment. The ratio for AMPKα activity significantly increased in human skeletal muscle cells treated with statins for long- and short-term. Furthermore, the insulin-stimulated counterpart, AKT, significantly decreased in activity and protein level, while GSK3ß and mTOR protein expression reduced in statin-treated primary human myotubes, only. However, GLUT4 was normally distributed whereas CAV3 was internalized from plasma membrane around the nucleus in statin-treated primary human myotubes. Statin-treatment activates AMPKα-dependent glucose uptake and remains active after long-term statin treatment. Permanent blocking of its insulin-dependent counterpart AKT activation may lead to metabolic inflexibility and insulin resistance in the long run and may be a direct consequence of statin-treatment.

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Section: Discussionmentioning

confidence: 63%

Section: Discussionmentioning

confidence: 99%

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Statins Aggravate the Risk of Insulin Resistance in Human Muscle

Grunwald

Haafke

Grieben

et al. 2022

IJMS

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“…The output of this biological process is the generation of the 3-hydroxy-3-methyl-glutaryl-CoA reductase (HMGCR) that has been associated with cancer growth leading to poorer prognosis. [ 122 ] Hence, statins, the HMGCR inhibitors, are currently of increasing translational interest for inhibiting tumor growth and angiogenesis.…”

Section: Emerging Therapies and Clinical Trials For Mbcmentioning

confidence: 99%

The Present and Future of Clinical Management in Metastatic Breast Cancer

Lin

Laliotis

2022

JCM

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Regardless of the advances in our ability to detect early and treat breast cancer, it is still one of the common types of malignancy worldwide, with the majority of patients decease upon metastatic disease. Nevertheless, due to these advances, we have extensively characterized the drivers and molecular profiling of breast cancer and further dividing it into subtypes. These subgroups are based on immunohistological markers (Estrogen Receptor-ER; Progesterone Receptor-PR and Human Epidermal Growth Factor Receptor 2-HER-2) and transcriptomic signatures with distinct therapeutic approaches and regiments. These therapeutic approaches include targeted therapy (HER-2+), endocrine therapy (HR+) or chemotherapy (TNBC) with optional combination radiotherapy, depending on clinical stage. Technological and scientific advances in the identification of molecular pathways that contribute to therapy-resistance and establishment of metastatic disease, have provided the rationale for revolutionary targeted approaches against Cyclin-Dependent Kinases 4/6 (CDK4/6), PI3 Kinase (PI3K), Poly ADP Ribose Polymerase (PARP) and Programmed Death-Ligand 1 (PD-L1), among others. In this review, we focus on the comprehensive overview of epidemiology and current standard of care treatment of metastatic breast cancer, along with ongoing clinical trials. Towards this goal, we utilized available literature from PubMed and ongoing clinical trial information from clinicaltrials.gov to reflect the up to date and future treatment options for metastatic breast cancer.

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“…Activation of the PIK3 leads to recruitment of the AKT kinase and subsequently intracellular cascade of phosphorylation of mTOR, a potent driver of cancer cell progression and survival [119]. PI3K mutation and AKT activation are also paramount in endocrine therapy resistance [120]. To this extent, several ongoing clinical trials are investigating the efficacy and safety of PI3K/AKT/mTOR inhibitors, in combination with estrogen therapy and standard-of-care chemotherapy.…”

Section: Emerging Therapies and Clinical Trials For Mbcmentioning

confidence: 99%

The Present and Future of Clinical Management in Metastatic Breast Cancer

Lin¹,

Laliotis²

2022

Preprint

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Regardless of the advances in our ability to detect early and treat breast cancer, it is still one of the common types of malignancy worldwide, with the majority of patients decease upon metastatic disease. Nevertheless, due to these advances, we have extensively characterized the drivers and molecular profiling of breast cancer and further dividing it into subtypes. These subgroups are based on immunohistological markers (Estrogen Receptor-ER, Progesterone Receptor-PR and Human Epidermal Growth Factor Receptor 2-HER-2) and transcriptomic signatures, with distinct therapeutic approaches and regiments. These therapeutic approaches include targeted therapy (HER-2+), endocrine therapy (HR+) or chemotherapy (TNBC) with optional combination radiotherapy, depending on clinical stage. Technological and scientific advances in the identification of molecular pathways that contribute to therapy-resistance and establishment of metastatic disease, have provided the rationale for revolutionary targeted approaches against Cyclin-Dependent Kinases 4/6 (CDK4/6), PI3 Kinase (PI3K), Poly ADP Ribose Polymerase (PARP) and Programmed Death-Ligand 1 (PD-L1), among others. In this review, we focus on the comprehensive overview of epidemiology and current standard of care treatment of metastatic breast cancer, along with ongoing clinical trials. Towards this goal, we utilized available literature from PubMed and ongoing clinical trial information from clinicaltrials.gov to reflect the up to date and future treatment options for metastatic breast cancer.

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Statins and endocrine resistance in breast cancer

Cited by 10 publications

References 51 publications

Statins Aggravate the Risk of Insulin Resistance in Human Muscle

Statins Aggravate the Risk of Insulin Resistance in Human Muscle

The Present and Future of Clinical Management in Metastatic Breast Cancer

The Present and Future of Clinical Management in Metastatic Breast Cancer

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