Atorvastatin / Histones Cancer Research Results

ATV, Atorvastatin: Click to Expand ⟱
Features: Statin
Atorvastatin is a statin, i.e., an inhibitor of HMG-CoA reductase, the rate-limiting enzyme of the mevalonate pathway. Clinically it is prescribed to lower LDL cholesterol and cardiovascular risk.

Atorvastatin — a synthetic small-molecule statin that competitively inhibits HMG-CoA reductase (HMGCR), the rate-limiting enzyme of the mevalonate (MVA) pathway. It is a clinically approved oral lipid-lowering drug (LDL-C reduction; ASCVD risk reduction) with extensive hepatic first-pass handling and pleiotropic vascular/anti-inflammatory effects. Classification: small-molecule drug; HMG-CoA reductase inhibitor (statin). Standard abbreviation(s): ATV; (brand: Lipitor). In oncology research, its main leverage is MVA-pathway suppression leading to reduced isoprenoid supply (FPP/GGPP) and impaired prenylation-dependent signaling (Ras/Rho family), with context-dependent chemosensitization/radiosensitization reported in preclinical and limited clinical settings.

Primary mechanisms (ranked):

  1. HMGCR inhibition → ↓ mevalonate flux → ↓ FPP/GGPP isoprenoids → impaired protein prenylation (Ras/Rho/Rac signaling dependence)
  2. ↓ prenylation/↓ lipid-raft cholesterol support → attenuation of growth, survival, EMT/migration programs (context-dependent)
  3. Compensatory sterol-feedback rewiring (SREBP2-driven upregulation of MVA genes; “restore-the-pathway” resistance axis)
  4. Immuno-inflammatory modulation (often ↓ NF-κB–linked cytokine programs; tumor-context dependent)
  5. Cell-stress outputs (apoptosis/autophagy modulation; mitochondrial stress/ROS changes in some models)
  6. Therapy interaction phenotypes (chemosensitization and radiosensitization in selected contexts; not universal)

Bioavailability / PK relevance: Oral dosing with high hepatic extraction; exposure is strongly interaction-sensitive because atorvastatin is a CYP3A4 substrate and also uses hepatic transport (e.g., OATP1B1/1B3). Clinically meaningful systemic levels are achievable, but many anticancer in-vitro concentrations may exceed typical free plasma exposures; tumor delivery and intracellular “on-pathway” inhibition are therefore context- and dosing-dependent.

In-vitro vs systemic exposure relevance: Antiproliferative/EMT and apoptosis effects in cell culture are frequently reported at micromolar concentrations, which may be higher than unbound systemic exposures in humans; the most translatable mechanism is on-target MVA suppression with downstream prenylation stress, especially where tumors are MVA-addicted or combined with agents that block feedback/compensation.

Clinical evidence status: Approved drug for dyslipidemia/ASCVD prevention. In cancer: extensive preclinical literature plus observational associations; limited interventional oncology studies exist (including biomarker-focused trials and combination/adjunct concepts). Overall status: repurposing candidate with context-dependent signals; not an established anticancer therapy.

Across preclinical and observational contexts, atorvastatin tends to:
-DOWNREGULATE proliferative and survival signaling (via impaired prenylation)
-REDUCE inflammatory signaling (NF-κB–linked effects)
-MODULATE immune and stromal interactions
-SENSITIZE some tumors to chemotherapy or radiation (context-dependent)
-Epidemiologic studies suggest statin use is associated with reduced incidence or improved outcomes in some cancers (e.g., colorectal, prostate, breast).

Atorvastatin — cancer-relevant mechanistic axes (ranked)

Rank Pathway / Axis Cancer Cells Normal Cells TSF Primary Effect Notes / Interpretation
1 Mevalonate pathway suppression HMGCR ↓ → MVA flux ↓ HMGCR ↓ (hepatic target) P/R Depletes sterols + isoprenoids upstream On-target mechanism; anticancer relevance rises in MVA-addicted tumors and when combined with strategies that prevent compensation.
2 Protein prenylation stress Ras/Rho/Rac prenylation ↓ → signaling output ↓ Variable; typically tolerated at clinical doses R Disrupts membrane localization of key GTPases Central downstream effector of anticancer activity; impacts proliferation, migration, cytoskeletal dynamics, and survival programs.
3 SREBP2 feedback and “restore-the-pathway” resistance SREBP2 ↑ (often) → HMGCR/MVA genes ↑ (adaptive) SREBP2 ↑ (homeostatic lipid control) G Adaptive rewiring that can blunt efficacy Common translational constraint: tumors may upregulate MVA pathway, increase uptake, or rewire metabolism to bypass blockade.
4 Growth and survival signaling PI3K–AKT ↔/↓, MAPK ↔/↓ (model-dependent) Endothelial survival ↔/↑ (context-dependent) R/G Downshifts pro-survival signaling tone Often secondary to prenylation/lipid-raft disruption; direction depends on oncogenic wiring and dose.
5 Migration, invasion, EMT EMT ↓, motility ↓ (often) Wound/repair migration ↔ G Anti-migratory / anti-invasive phenotype Mechanistically linked to Rho-family prenylation and cytoskeletal/ECM programs; may be clinically relevant in select settings.
6 Inflammation and NF-κB-linked cytokine programs IL-6/IL-8/TNF-α ↓ (often) Vascular inflammation ↓ R/G Anti-inflammatory immunometabolic shift Pleiotropic statin effects; may affect tumor microenvironment and therapy tolerance, but tumor-immune direction can be context-dependent.
7 ROS and mitochondrial stress ROS ↑ (sometimes; dose-dependent) Oxidative injury ↔/↓ in vascular contexts P/R Stress signaling that can promote apoptosis or sensitize to therapy Reported in subsets of models; not universally primary. Separate “cancer cell ROS ↑” from “vascular protective” pleiotropy.
8 Cell death programs Apoptosis ↑; autophagy ↔/↑ (model-dependent) Generally cytoprotective at therapeutic dosing R/G Stress-induced cell fate shift Often downstream of prenylation deficit + metabolic stress; strong effects often require higher concentrations or combinations.
9 Drug transport and resistance P-gp ↓ (reported); efflux ↔/↓ (context-dependent) Transporter effects ↔ R/G Potential bioenhancement / chemosensitization May contribute to combination effects, but clinical relevance is uncertain and interaction risk must be managed.
10 Radiosensitization and chemosensitization RadioS ↑; ChemoSen ↑ (subset) Normal tissue injury ↔/↓ (some contexts) G Adjunct therapy leverage (context-dependent) Signals exist in preclinical and limited clinical/biomarker work; not a class-wide guarantee and may depend on tumor MVA reliance.
11 Clinical Translation Constraint Free exposure may be below many in-vitro “kill” concentrations; adaptive SREBP2 feedback; tumor heterogeneity Myopathy/rhabdomyolysis risk ↑ with interacting drugs; hepatic enzyme elevations; pregnancy contraindication Defines practical therapeutic window Major constraints: CYP3A4/transport interactions (e.g., strong inhibitors; grapefruit), muscle toxicity risk, and uncertain tumor delivery/on-target engagement at tolerated doses.

TSF legend: P: 0–30 min   R: 30 min–3 hr   G: >3 hr
Histones, Histones: Click to Expand ⟱
Source:
Type:
Histones play a crucial role in regulating gene expression, and this regulatory mechanism is central to many aspects of brain development, function, and plasticity.

-Histone Acetylation: Often associated with active gene transcription. Enzymes known as histone acetyltransferases (HATs) add acetyl groups that reduce the positive charge on histones, weakening their interaction with the negatively charged DNA and thereby promoting gene expression.
-Histone Methylation: Depending on the specific amino acid residue and the number of methyl groups added, histone methylation can either activate or repress transcription. For instance, methylation on lysine 4 of histone H3 (H3K4me) is commonly linked to gene activation, whereas methylation on lysine 9 (H3K9me) is typically associated with gene repression.
Scientific Papers found: Click to Expand⟱
4981- ATV,    Crosstalk between Statins and Cancer Prevention and Therapy: An Update
Apoptosis↑, selectivity↑, eff↑, HMG-CoA↓, *cardioP↑, OS↑, IL1β↓, IL6↓, IL8↓, TNF-α↓, TumAuto↑, Histones↝, ac‑H3↑, ac‑H4↑, HDAC↓,

Showing Research Papers: 1 to 1 of 1

* indicates research on normal cells as opposed to diseased cells
Total Research Paper Matches: 1

Pathway results for Effect on Cancer / Diseased Cells:


Core Metabolism/Glycolysis

Histones↝, 1,   HMG-CoA↓, 1,  

Cell Death

Apoptosis↑, 1,  

Transcription & Epigenetics

ac‑H3↑, 1,   ac‑H4↑, 1,  

Autophagy & Lysosomes

TumAuto↑, 1,  

Proliferation, Differentiation & Cell State

HDAC↓, 1,  

Immune & Inflammatory Signaling

IL1β↓, 1,   IL6↓, 1,   IL8↓, 1,   TNF-α↓, 1,  

Drug Metabolism & Resistance

eff↑, 1,   selectivity↑, 1,  

Clinical Biomarkers

IL6↓, 1,  

Functional Outcomes

OS↑, 1,  
Total Targets: 15

Pathway results for Effect on Normal Cells:


Functional Outcomes

cardioP↑, 1,  
Total Targets: 1

Scientific Paper Hit Count for: Histones, Histones
Query results interpretion may depend on "conditions" listed in the research papers.
Such Conditions may include : 
  -low or high Dose
  -format for product, such as nano of lipid formations
  -different cell line effects
  -synergies with other products 
  -if effect was for normal or cancerous cells

Filter Conditions: Pro/AntiFlg:%  IllCat:%  CanType:%  Cells:%  prod#:2  Target#:1232  State#:%  Dir#:4
  wNotes=0  sortOrder:rid,rpid

 

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