Scientists map how cinnamon’s bioactives interact with cancer signaling

By Priyanjana Pramanik, MSc.Reviewed by Susha Cheriyedath, M.Sc.Dec 15 2025

Laboratory studies suggest cinnamon’s bioactive compounds can alter key cancer-related signaling pathways, but researchers caution that human trials are essential before any preventive or therapeutic claims can be made.

Study: Potential effects of cinnamon on cancer prevention and progression. Image Credit: Birol Dincer 

In a recent review published in the journal Frontiers in Nutrition, researchers examined the compounds found in cinnamon and summarized evidence on how these components influence cancer-related pathways.

Based on in vitro and animal studies, cinnamon may have cancer-preventive and anti-cancer potential. However, rigorous animal and human clinical studies are needed to establish its safety, efficacy, appropriate dosing, and whether biologically active concentrations can be achieved in human tissues.

Traditional Medicine and Modern Research Interest

Cinnamon is a traditional medicinal spice used for metabolic disorders and gastrointestinal complaints. In recent decades, scientific interest has expanded beyond its debated antidiabetic effects to include potential roles in cancer prevention and treatment.

This growing interest reflects both rising healthcare costs and increased public demand for complementary and alternative therapies. Given that many modern drugs are derived from plant compounds, understanding whether cinnamon can meaningfully influence cancer biology is important, while avoiding overinterpretation of early-stage mechanistic findings and acknowledging translational limitations.

Bioactive Compounds in Cinnamon

The most extensively studied compound in cinnamon is cinnamaldehyde, but other notable constituents include cinnamyl acetate, cinnamic acid, caffeic acid, coumarin, and eugenol. Cinnamon is also rich in polyphenols, which are widely investigated for their antioxidant and anti-cancer properties.

Several in vitro studies suggest that cinnamaldehyde and related compounds can induce cancer cell death. Screening studies using drug-likeness and bioavailability criteria have identified cinnamaldehyde as a key candidate affecting receptors linked to metabolism, inflammation, and tumor progression, although these findings remain predictive rather than confirmatory and do not guarantee in vivo activity at dietary intake levels.

Procyanidin-B2, another cinnamon-derived compound, has been shown to inhibit proteasome activity, thereby reducing cancer cell proliferation and promoting programmed cell death. In addition, derivatives of chemically modified cinnamic acid have demonstrated anti-metastatic and cytotoxic effects across multiple cancer cell lines, highlighting the importance of molecular structure in biological activity.

Transcription Factor Modulation Mechanisms

Nuclear factor kappa-light-chain-enhancer of activated B cells (NFκB) is a stress-responsive transcription factor that regulates genes involved in inflammation, cell survival, angiogenesis, and metastasis. It is frequently overactivated in cancer and contributes to tumor progression and treatment resistance.

Cinnamon polyphenols have been shown to inhibit NFκB activation, primarily by interfering with the IKK–IκB signaling axis that regulates NFκB nuclear translocation. By suppressing NFκB signaling, cinnamon components may reduce inflammation, angiogenesis, and anti-apoptotic gene expression. Experimental studies, including mouse tumor models, have demonstrated reduced tumor growth and decreased NFκB activity following cinnamon treatment under controlled dosing conditions.

Activator protein 1 (AP-1) is another transcription factor implicated in cancer cell proliferation, survival, inflammation, and metastasis. Like NFκB, it is activated by inflammatory stimuli and oncogenic signaling.

Phytochemicals, including cinnamon extracts, have been shown to reduce AP-1 activity by inhibiting upstream signaling pathways such as mitogen-activated protein kinase (MAPK). In mouse tumor models, cinnamon administration led to smaller tumors and reduced expression of AP-1 target genes associated with cell survival, suggesting that AP-1 inhibition contributes to cinnamon’s pro-apoptotic effects.

Nuclear factor erythroid 2–related factor 2 (Nrf2) regulates antioxidant and detoxification genes and plays a complex role in cancer. While its activation may prevent cancer initiation, persistent Nrf2 activation in established tumors can support cancer cell survival, metabolic adaptation, and resistance to therapy.

Cinnamon-derived compounds, particularly cinnamaldehyde, are potent activators of Nrf2. While this may be beneficial for cancer prevention, the review cautions that activating Nrf2 in existing tumors could potentially worsen outcomes, including effects on the tumor immune microenvironment, highlighting the need for context-specific evaluation.

Angiogenesis and Kinase Pathway Effects

Tumor growth depends on angiogenesis, often driven by hypoxia-inducible factor 1 (HIF-1) and vascular endothelial growth factor (VEGF). Cinnamon extracts and cinnamaldehyde can suppress HIF-1α expression and VEGF signaling, thereby reducing tumor growth and angiogenesis in experimental models. These effects may involve inhibition of HIF-1α protein synthesis via PI3K/Akt/mTOR-related pathways, with most evidence derived from preclinical systems.

Cinnamon components also interact with serine/threonine kinases, which regulate proliferation and survival. Certain cinnamaldehyde derivatives directly inhibit these kinases, promoting apoptosis in cancer cells. Other studies report reduced MAPK phosphorylation, contributing to anti-angiogenic and anti-proliferative effects.

Microbiome, Inflammation, and Safety Considerations

Beyond direct anti-cancer effects, cinnamon may contribute to cancer prevention by improving gut microbiome health and reducing chronic inflammation.

Cinnamon polyphenols can be metabolized by gut bacteria and, in animal models, have been shown to restore microbial balance, strengthen intestinal barriers, and reduce pro-inflammatory cytokine levels. Small clinical trials in non-cancer populations suggest cinnamon may modestly lower inflammatory markers such as NFκB, tumor necrosis factor alpha (TNFα), and C-reactive protein (CRP), although findings are variable and based on surrogate endpoints.

A key limitation is the poor oral bioavailability of cinnamaldehyde, linked to limited solubility and rapid metabolism, which may restrict systemic exposure following dietary consumption. Novel delivery systems, including nanoparticle-based approaches, are being explored to enhance targeting and reduce side effects.

Safety considerations are critical, as cinnamon contains coumarin, which at high doses may cause liver toxicity and has shown carcinogenic effects in animal studies. At lower doses, coumarin has also demonstrated anti-cancer activity in experimental settings, underscoring the importance of controlled dosing, compound standardization, and long-term safety assessment.

Evidence Gaps and Clinical Implications

Cinnamon has credible potential to influence multiple cancer-related pathways, particularly inflammation, apoptosis, and angiogenesis. However, most evidence comes from in vitro and animal studies, and many proposed mechanisms should not be overinterpreted without pharmacokinetic and tissue-distribution data.

Carefully designed clinical trials and safety assessments are essential before cinnamon, or its components, can be recommended as effective adjuncts or preventive strategies in cancer care.