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    Cannabis Terpenes: What Science Shows About the Compounds Behind the Aroma

    Six cannabis terpenes represented as translucent colored droplets — limonene (yellow), linalool (purple), pinene (green), β-caryophyllene (amber), myrcene (teal), and humulene (sage) — each with distinct pharmacological properties

    Cannabis Terpenes: The Science Behind Aroma and Function

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    Six cannabis terpenes represented as translucent colored droplets — limonene (yellow), linalool (purple), pinene (green), β-caryophyllene (amber), myrcene (teal), and humulene (sage) — each with distinct pharmacological properties

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Cannabis Terpenes: What Science Shows About the Compounds Behind the Aroma

Christian Pronk by Christian Pronk
03/30/2026
in Terpenes
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Table of Contents

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  • Cannabis Terpenes: What Science Shows About the Compounds Behind the Aroma
    • What Are Terpenes — and Why Does Cannabis Produce So Many?
    • Do Terpenes Actually Have Therapeutic Effects?
    • The Key Cannabis Terpenes: Individual Profiles
      • β-Caryophyllene — the dietary cannabinoid
      • Limonene — the anxiety modulator
      • Linalool — the sedative analgesic
      • α-Pinene — the memory protector
      • Myrcene — the sedative
      • α-Humulene — the anti-inflammatory
      • Geraniol — the emerging neuroprotectant
      • Nerolidol — the skin penetration enhancer
    • How Terpenes Are Lost — and Preserved — in CBD Products
    • What This Means for Choosing CBD Products in Europe
    • Frequently Asked Questions
          • Do cannabis terpenes have real health benefits?
          • Which cannabis terpene is best for anxiety?
          • Are terpenes in CBD oil the same as in the cannabis plant?
          • Do terpenes get you high?
          • What happens to terpenes when cannabis is processed?
    • Sources and Further Reading

Cannabis Terpenes: What Science Shows About the Compounds Behind the Aroma

CBD.Help Editorial Team
CBD.Help Editorial Team
Science & Research · Published March 2026

In a 2024 study published in the journal PAIN, researchers at the University of Arizona tested five cannabis terpenes against chronic neuropathic pain in animal models. Each terpene reduced pain at levels comparable to or exceeding the peak effect of morphine. When combined with morphine, the analgesic effects increased further — without triggering the reward behaviour associated with opioid addiction (Streicher et al., 2024). The compounds responsible are the same ones you smell when you open a jar of cannabis flower.

Cannabis terpenes have moved well beyond their original designation as aromatic curiosities. Over the past five years, a series of preclinical and receptor-level studies has revealed that these compounds interact directly with the endocannabinoid system, modulate pain pathways, and may complement the effects of cannabinoids like CBD and THC in ways that are only now being measured. This article reflects research and regulations available as of February 2026.

In brief: Cannabis terpenes are aromatic compounds produced in the plant’s trichomes alongside cannabinoids. Over 150 have been identified. Recent research shows they are far more than flavour molecules: a 2023 in vitro study found all sixteen terpenes tested activated CB1 cannabinoid receptors independently (Raz et al., 2023), while a 2024 preclinical study found five terpenes matched morphine for neuropathic pain relief without addiction potential (Streicher et al., 2024). Their individual profiles — and how they are preserved in products — determine much of what makes one CBD formulation different from another.

What this article covers:

  • Five cannabis terpenes matched morphine for chronic pain relief in a 2024 preclinical study — and showed no signs of addiction potential (Streicher et al., 2024).
  • All sixteen cannabis terpenes tested in a 2023 study activated CB1 cannabinoid receptors on their own, at 10–50% of THC’s potency (Raz et al., 2023).
  • Individual profiles of the eight most researched cannabis terpenes — what each one does, what receptor it targets, and how strong the evidence is.
  • The finding that terpenes given by injection produced strong effects while oral and inhaled routes showed significantly weaker results — a nuance with major implications for product claims that most guides ignore.
  • What terpene profiles actually tell you when choosing between CBD products in Europe.

What Are Terpenes — and Why Does Cannabis Produce So Many?

Before examining the pharmacological evidence, it helps to understand what terpenes actually are — and why cannabis is unusually rich in them.

Terpenes are organic compounds produced by nearly all plants. They are the primary components of essential oils — the reason lavender smells like lavender, lemons smell like lemons, and black pepper smells like black pepper. Over 20,000 terpenes have been characterised across the plant kingdom. They serve ecological functions: repelling insects, attracting pollinators, protecting against UV radiation, and defending against fungal and bacterial pathogens.

Cannabis is exceptional in its terpene diversity. Over 150 distinct terpenes have been identified in the plant, with multiple terpenes often co-dominant in a single variety — a feature that is unusual in the botanical world. These compounds are synthesised in the same glandular trichomes that produce cannabinoids like THC and CBD, and they share a common biochemical precursor: geranyl pyrophosphate. This shared biosynthetic origin is not a coincidence — it is the foundation of the entourage effect hypothesis, which proposes that cannabinoids and terpenes evolved together and function together.

Structurally, cannabis terpenes fall into two main categories. Monoterpenes — including limonene, myrcene, α-pinene, and linalool — are built from ten carbon atoms. They are small, light, and highly volatile, which is why they dominate the initial aroma of fresh cannabis flower but diminish rapidly with drying and storage. Sesquiterpenes — including β-caryophyllene, α-humulene, and nerolidol — have fifteen carbon atoms. They are heavier, less volatile, and persist more reliably through processing and extraction. This structural difference has direct consequences for what ends up in a finished CBD product.

[SVG-PLACEHOLDER: Cannabis terpene biosynthesis pathway — simplified diagram showing geranyl pyrophosphate as precursor branching into monoterpenoid and sesquiterpenoid pathways, with key terpenes placed at their branch endpoints]

Key takeaway: Cannabis produces an unusually large number of terpenes in the same structures that produce cannabinoids, from the same biochemical precursor — a co-production that positions terpenes not as incidental aroma molecules, but as potential functional partners in the plant’s pharmacology.

Do Terpenes Actually Have Therapeutic Effects?

For decades, the therapeutic properties of terpenes were studied primarily in the context of essential oils and aromatherapy — fields that, fairly or not, carried less scientific credibility than mainstream pharmacology. That perception has shifted substantially since 2021, driven by a series of rigorous preclinical studies that subjected cannabis terpenes to the same experimental standards applied to conventional analgesics.

The turning point came from the Comprehensive Pain and Addiction Center at the University of Arizona. In 2021, a study published in Scientific Reports tested four cannabis terpenes — α-humulene, geraniol, linalool, and β-pinene — individually and in combination with a synthetic cannabinoid agonist. Each terpene, administered alone, reduced pain sensitivity in mouse models. When combined with the cannabinoid, pain reduction was greater than either compound achieved independently — without an increase in negative side effects (LaVigne et al., 2021). The authors described the terpenes as “cannabimimetic”: they mimicked the behavioural effects of cannabinoids, including analgesia.

The same laboratory then raised the stakes considerably.

In a 2024 follow-up published in the journal PAIN, Streicher and colleagues tested five cannabis terpenes against chronic neuropathic pain — the type of nerve pain that is notoriously difficult to treat and frequently drives long-term opioid use. Morphine served as the comparator. Each terpene reduced pain at levels near to or exceeding morphine’s peak effect. When the terpenes were combined with morphine, the analgesic effects of all five combinations were significantly enhanced. And critically, the terpenes showed no signs of producing reward — the mice did not “like” the terpenes the way they respond to opioids — suggesting that these compounds may lack addiction potential (Streicher et al., 2024).

As with any wellness decision, consulting a healthcare provider is recommended — particularly for those on existing medication.

Conventional treatments for chronic neuropathic pain — including opioids, gabapentinoids, and tricyclic antidepressants — carry well-documented side-effect profiles including sedation, dependence, cognitive impairment, and, in the case of opioids, respiratory depression and addiction. In this context, the identification of compounds that match opioid-level analgesia without reward behaviour represents a genuinely significant preclinical finding.

There is, however, an important caveat that most terpene guides do not mention. The Streicher 2024 study found that when terpenes were administered orally or inhaled as vapour rather than injected, the analgesic effects were significantly reduced or absent. This is a critical nuance. It means that the pain-relief potential demonstrated in these studies may not translate directly to consumer products that deliver terpenes through ingestion or inhalation — the two routes most relevant to CBD oil and cannabis flower users. The researchers attributed part of this gap to the rapid metabolism and redistribution of volatile terpenes, and noted that the difficulty of masking terpene aromas made placebo-controlled inhalation studies challenging.

Running in parallel, the Raz et al. 2023 study published in Biochemical Pharmacology provided the receptor-level explanation for how these effects might occur. All sixteen cannabis terpenes tested activated CB1 cannabinoid receptors independently, at 10–50% of THC’s potency. Several synergised with THC at plant-natural ratios. A 2025 follow-up extended these findings to CB2 receptors. Together, these studies establish that cannabis terpenes are not merely aromatic passengers — they are pharmacologically active compounds that engage the same receptor systems as cannabinoids.

The bottom line: Cannabis terpenes have moved from hypothetical contributors to experimentally demonstrated pharmacological agents — with analgesic effects comparable to morphine in preclinical models and confirmed activity at both CB1 and CB2 cannabinoid receptors. The route-of-administration question remains the critical gap between laboratory findings and consumer product claims.

The Key Cannabis Terpenes: Individual Profiles

With the broader evidence established, the next question is practical: which terpenes carry the most research support, and what does each one do? The following profiles cover the eight most studied cannabis terpenes, drawing on the foundational pharmacology catalogued by Russo in his 2011 British Journal of Pharmacology review and substantially updated with research published through 2025.

β-Caryophyllene — the dietary cannabinoid

β-Caryophyllene is the most pharmacologically distinctive terpene in cannabis. In 2008, a study published in the Proceedings of the National Academy of Sciences demonstrated that this sesquiterpene — also abundant in black pepper, cloves, and cinnamon — is a selective full agonist at the CB2 cannabinoid receptor (Gertsch et al., 2008). It was the first compound from outside the cannabis genus proven to function as a cannabinoid. Because CB2 is not associated with psychoactivity, β-caryophyllene offers anti-inflammatory and neuroprotective potential without intoxication.

The evidence has deepened substantially since that initial discovery. A 2024 review in the International Journal of Molecular Sciences documented β-caryophyllene’s activity across CB2 and PPAR receptor pathways, highlighting its therapeutic potential for depression, anxiety, neuroinflammation, and metabolic disorders (Ricardi et al., 2024). Preclinical studies have also demonstrated effects on food addiction behaviour and liver disease. As the most heat-stable terpene in cannabis — frequently the dominant terpenoid in decarboxylated extracts — β-caryophyllene is the terpene most likely to survive processing and appear in finished CBD products. For a detailed examination, see our complete guide to β-caryophyllene.

Limonene — the anxiety modulator

Limonene, the second most widely distributed terpene in nature, gives citrus fruits their characteristic scent. In cannabis, it contributes a bright, uplifting aromatic note. Its pharmacological profile has been studied extensively — and now includes the first human data linking a cannabis terpene to modulation of cannabinoid effects.

A 2024 double-blind, placebo-controlled crossover study published in Drug and Alcohol Dependence found that when human participants inhaled vaporised limonene alongside THC, they reported significantly reduced anxiety, nervousness, and paranoia compared to THC alone (Spindle et al., 2024). This is — to date — the strongest human evidence for a specific terpene-cannabinoid interaction. Earlier research documented limonene’s anxiolytic effects in animal models and a remarkable clinical study in which hospitalised depressed patients exposed to citrus fragrance showed normalised depression scores and successful antidepressant discontinuation in nine of twelve participants (Komori et al., 1995). Limonene is highly bioavailable through pulmonary absorption, with human uptake estimated at 70%.

Linalool — the sedative analgesic

Linalool is the primary terpenoid in lavender and the compound most responsible for lavender’s documented calming effects. Its pharmacological profile is broad: sedative, anticonvulsant, anti-glutamatergic, and locally anaesthetic — with potency comparable to procaine in some experimental models. In the Streicher 2024 pain study, linalool was among the five terpenes that matched morphine’s analgesic effect in neuropathic pain models.

A notable clinical finding: in a study of morbidly obese patients undergoing gastric banding surgery, inhalation of lavender essential oil — whose primary active component is linalool — reduced post-operative morphine consumption compared to placebo (Kim et al., 2007). In the Raz et al. 2023/2025 receptor studies, linalool activated both CB1 and CB2, with selectivity toward CB2. This dual receptor engagement, combined with its modulation of glutamate and GABA neurotransmitter systems, gives linalool one of the broadest mechanistic profiles of any cannabis terpene.

α-Pinene — the memory protector

α-Pinene is the most widely encountered terpene in nature — the molecule that gives pine forests their characteristic scent. In cannabis, it contributes a sharp, resinous note. Its most intriguing property is its activity as an acetylcholinesterase inhibitor: it helps preserve acetylcholine, the neurotransmitter most directly associated with memory formation and cognitive function.

This property has led to the hypothesis — proposed by Russo in 2011 and supported by historical cannabis “antidotes” dating back to ancient Persia and Rome — that pinene may counteract the short-term memory impairment caused by THC. A 2024 study by Laws and Smid found that α-pinene and β-pinene demonstrated neuroprotective and anti-aggregatory effects against β-amyloid-mediated toxicity, suggesting potential relevance to neurodegenerative conditions. α-Pinene is also a bronchodilator in humans at low exposure levels and a broad-spectrum antimicrobial.

Myrcene — the sedative

Myrcene is frequently the most abundant monoterpene in cannabis flower. It is also a recognised sedative component of hops — the plant most closely related to cannabis — where it has been used in German herbal medicine to aid sleep. Preclinical studies have demonstrated muscle relaxant and analgesic properties, with the analgesic effect blocked by naloxone, suggesting involvement of opioid receptor pathways.

In a 2023 observational study using real-time patient-reported outcomes, cannabis flowers with elevated myrcene levels were associated with the greatest perceived symptom relief among 633 products assessed (Vigil et al., 2023). As a highly volatile monoterpene, myrcene is one of the first compounds lost during drying and storage — which means that the myrcene content on a laboratory certificate of analysis may not reflect what remains in the product by the time a consumer uses it.

α-Humulene — the anti-inflammatory

α-Humulene, a sesquiterpene also found in hops and sage, has demonstrated anti-inflammatory effects in multiple experimental models. A 2024 scoping review documented its anti-proliferative, analgesic, and appetite-suppressing properties. In the Streicher 2024 pain study, α-humulene was among the five terpenes that matched morphine-level analgesia in neuropathic pain models. Its anti-inflammatory activity has been attributed to inhibition of key pro-inflammatory cytokines, including TNF-α and IL-1β.

Geraniol — the emerging neuroprotectant

Geraniol, a monoterpenoid with a sweet, floral rose scent, has received increasing attention since 2021. It was one of the four terpenes in the original LaVigne et al. cannabimimetic study, where it demonstrated pain-relieving effects comparable to the other terpenes tested. A 2024 study found that geraniol may enhance cognitive function and protect brain cells, with antioxidant properties that reduce oxidative stress. Its presence in cannabis is typically modest, but its inclusion in the Streicher group’s morphine-comparison studies positions it as a terpene of growing research interest.

Nerolidol — the skin penetration enhancer

Nerolidol is a sesquiterpene alcohol present at low levels in cannabis and in citrus peels. Its most distinctive property is its ability to enhance skin penetration of other compounds — a characteristic that has been leveraged in topical drug delivery research, including studies with the chemotherapy agent 5-fluorouracil. Nerolidol has also demonstrated sedative, antifungal, antimalarial, and anti-leishmanial activity. For topical CBD products, its presence could theoretically enhance transcutaneous absorption of cannabinoids, though this specific application has not been tested in controlled human studies.

Cannabis Terpene Master Reference
Terpene Class Aroma Also Found In Key Research Finding Receptor Activity
β-Caryophyllene Sesquiterpene Spicy, peppery, woody Black pepper, cloves, cinnamon Selective full CB2 agonist — first dietary cannabinoid (Gertsch et al., 2008) CB2 full agonist; PPAR-α/γ activator
Limonene Monoterpene Citrus, lemon, orange Citrus peel, juniper Reduced THC-induced anxiety in humans (Spindle et al., 2024) CB1 agonist (10–50% of THC); CB2 selective in Raz 2025
Linalool Monoterpene alcohol Floral, lavender Lavender, basil, coriander Matched morphine analgesia in neuropathic pain (Streicher et al., 2024) CB1 + CB2 agonist; modulates glutamate/GABA
α-Pinene Monoterpene Pine, resinous, sharp Pine, rosemary, eucalyptus Acetylcholinesterase inhibitor; neuroprotective against β-amyloid (Laws & Smid, 2024) CB1 agonist; bronchodilator; AChE inhibitor
Myrcene Monoterpene Earthy, musky, herbal Hops, lemongrass, mango Associated with greatest symptom relief in chemovar study (Vigil et al., 2023) CB1 agonist; analgesic via opioid pathway
α-Humulene Sesquiterpene Woody, hoppy, earthy Hops, sage, ginseng Matched morphine analgesia; anti-inflammatory via TNF-α/IL-1β inhibition Cannabimimetic (LaVigne et al., 2021)
Geraniol Monoterpenoid Sweet, floral, rose Geraniums, roses, citrus Cannabimimetic analgesic; neuroprotective and antioxidant (2024) Cannabimimetic (LaVigne et al., 2021)
Nerolidol Sesquiterpene alcohol Woody, floral, citrus Citrus peel, jasmine, tea tree Enhances skin penetration of other compounds; antifungal, antimalarial Sedative; skin permeation enhancer

Why it matters: Each terpene has a distinct pharmacological fingerprint — different receptor targets, different evidence levels, different survival rates through processing. Understanding these individual profiles is the prerequisite for evaluating any product claim that invokes terpene content as a quality marker.

How Terpenes Are Lost — and Preserved — in CBD Products

Understanding which terpenes do what is only useful if you also understand which ones actually survive the journey from plant to product. This is the practical dimension that separates a lab-tested terpene profile from what a consumer ultimately encounters — and it is where the difference between monoterpenes and sesquiterpenes becomes directly relevant.

Monoterpenes — limonene, myrcene, α-pinene, linalool — are the most pharmacologically diverse group, but also the most fragile. They are small, volatile molecules with relatively low boiling points. They begin evaporating from the moment cannabis flower is harvested. Drying reduces their concentration. Storage continues the loss. Heat-based extraction or decarboxylation (the process that converts inactive cannabinoid acids into active forms like CBD and THC) accelerates it further. A laboratory certificate of analysis performed on freshly harvested flower may show a rich monoterpene profile that no longer exists by the time the product reaches a shelf.

Sesquiterpenes — β-caryophyllene, α-humulene, nerolidol — are heavier, less volatile, and considerably more heat-stable. β-Caryophyllene in particular is frequently the dominant terpenoid in decarboxylated cannabis extracts and finished CBD oils, precisely because it survives the conditions that strip away monoterpenes. This means that the terpene profile of a processed product is not a miniature version of the plant’s original profile — it is a fundamentally different composition, enriched in sesquiterpenes and depleted in monoterpenes.

Terpene Volatility and Product Implications
Terpene Class Examples Vulnerability Product Implication
Monoterpenes (C₁₀) Limonene, myrcene, α-pinene, linalool High — lost through drying, storage, heat, extraction Depleted in most finished CBD oils; presence indicates gentle processing and/or re-addition
Sesquiterpenes (C₁₅) β-Caryophyllene, α-humulene, nerolidol Low — survives drying, heat, most extraction methods Dominant in decarboxylated extracts; β-caryophyllene often the primary terpenoid in CBD oils
Diterpenes (C₂₀) Phytol Very low — stable breakdown product of chlorophyll Present in extracts as a processing artefact; modest GABA-related activity

This has direct implications for how to read a product label. A CBD oil that lists β-caryophyllene as its dominant terpene is reflecting normal extraction chemistry — this is expected. A CBD oil that also retains meaningful levels of limonene, linalool, or myrcene is telling you something about how the product was processed: either the extraction was unusually gentle, the terpenes were captured separately and reintroduced, or the product is closer to the plant’s original profile than most. Third-party certificates of analysis that include a detailed terpene panel — not just total terpene percentage — are the only reliable way to evaluate these claims.

The 2023 chemovar indexing study by Vigil et al., published in the Journal of Cannabis Research, reinforced why this matters. Cannabis flowers with distinct terpene profiles — not just different THC or CBD levels — were associated with measurably different patient-reported outcomes. The terpene composition is not a secondary quality marker. It is a primary determinant of how a product behaves pharmacologically.

The essential point: The terpene profile on a product label is a snapshot of what survived processing — not a copy of what was in the plant. Monoterpenes are the first casualties. Sesquiterpenes, especially β-caryophyllene, are the survivors. Understanding this distinction is the difference between reading a terpene label and actually using one.

What This Means for Choosing CBD Products in Europe

The research covered in this guide transforms terpenes from marketing buzzwords into evaluable product characteristics. If you are considering CBD products in Europe, here is how to apply this knowledge practically.

First, look beyond CBD concentration. A product’s terpene profile — which compounds are present, at what levels, and in what ratios — shapes how it interacts with the endocannabinoid system. Full-spectrum CBD oils that retain natural terpene diversity preserve the broadest range of these compounds, though the volatile monoterpenes will inevitably be reduced relative to the plant’s fresh flower profile.

Second, ask for terpene-specific testing. A certificate of analysis that reports “total terpenes: 2%” is less informative than one that identifies which terpenes are present and at what individual concentrations. β-Caryophyllene dominance in a processed extract is normal. The presence of retained monoterpenes — limonene, linalool, myrcene — suggests more careful processing or deliberate reintroduction.

Third, maintain realistic expectations about delivery routes. The Streicher 2024 data showed that terpene analgesia was strongest via injection — a route that does not apply to consumer products. Oral and inhaled terpene delivery produced significantly weaker effects in the same study. This does not invalidate terpene relevance, but it does mean that the dramatic preclinical findings may not translate one-to-one to the experience of taking a CBD oil or inhaling cannabis flower. The science is real. The magnitude of effect through consumer routes remains to be established.

Individual responses to CBD and terpenes vary, as they do with most bioactive compounds. Consulting a healthcare professional is recommended before making decisions about supplementation, particularly for those taking other medications.

What this means in practice: Terpenes are not a marketing feature — they are pharmacologically active compounds with documented receptor activity and analgesic potential. The quality of a CBD product is partly determined by which terpenes it retains. But the research also demands honesty about what we don’t yet know: how much of the preclinical effect translates through oral and inhaled routes, and which terpene profiles are optimal for which conditions. Those are the questions the next generation of clinical trials will need to answer.

Regulatory note: Terpenes themselves are classified as Generally Recognized as Safe (GRAS) food additives and are widely used in food, cosmetics, and aromatherapy products across the EU. The regulatory complexity arises when terpenes are delivered as part of CBD products. Consumer CBD products for oral use remain classified as Novel Foods under EU Regulation 2015/2283, and no CBD food supplement has received EFSA authorisation regardless of its terpene content. For a complete overview of CBD’s legal and regulatory status across EU member states, see our dedicated guide: CBD Regulation in Europe: Current Status and What You Need to Know.

Frequently Asked Questions

Do cannabis terpenes have real health benefits?

Preclinical evidence is now substantial. A 2024 study published in the journal PAIN found five cannabis terpenes reduced chronic neuropathic pain at levels comparable to morphine in animal models — without addiction-related reward behaviour (Streicher et al., 2024). A 2023 in vitro study confirmed all sixteen cannabis terpenes tested activate CB1 cannabinoid receptors independently (Raz et al., 2023). Human clinical data remains limited, though a 2024 double-blind trial found that vaporised limonene reduced THC-induced anxiety in people (Spindle et al., 2024).

Which cannabis terpene is best for anxiety?

Limonene and linalool have the strongest anxiety-related evidence. Limonene is the only cannabis terpene with human data directly linking it to anxiety reduction: a 2024 double-blind crossover trial found it significantly reduced THC-induced anxiety when co-inhaled (Spindle et al., 2024). Linalool — the primary terpenoid in lavender — has decades of anxiolytic research from aromatherapy studies, and activates both CB1 and CB2 receptors with CB2 selectivity (Raz et al., 2025). β-Caryophyllene also shows anxiolytic potential via CB2 receptor activation.

Are terpenes in CBD oil the same as in the cannabis plant?

Not exactly. Volatile monoterpenes — limonene, myrcene, α-pinene — are significantly reduced or lost during drying, storage, and heat-based extraction. Sesquiterpenes like β-caryophyllene are more heat-stable and survive processing, often becoming the dominant terpenoid in finished CBD oils. A full-spectrum CBD product retains the broadest terpene diversity, but its profile will always differ from fresh flower. Some manufacturers capture terpenes separately and reintroduce them to preserve a more complete profile.

Do terpenes get you high?

No. While cannabis terpenes can activate CB1 and CB2 cannabinoid receptors, they do so at 10–50% of THC’s potency at CB1 — levels that produce pharmacological effects such as pain modulation but not the intoxication associated with THC (Raz et al., 2023). In preclinical studies, terpenes produced analgesic effects without reward behaviour or evidence of psychoactive response (Streicher et al., 2024). Terpenes may modulate how THC feels — limonene appears to reduce THC-induced anxiety — but they do not produce a “high” on their own.

What happens to terpenes when cannabis is processed?

Monoterpenes (limonene, myrcene, α-pinene, linalool) are the most volatile and are progressively lost through every processing step: harvesting, drying, storage, and heat-based extraction or decarboxylation. Sesquiterpenes (β-caryophyllene, α-humulene, nerolidol) are heavier and more heat-stable, surviving most processing methods. As a result, the terpene profile of a CBD oil is fundamentally different from fresh flower — typically dominated by sesquiterpenes. Certificates of analysis that report individual terpene concentrations, not just total percentages, are the most informative quality indicator.

Important: This article is for informational purposes only and does not constitute medical advice. CBD products are not medicines and are not intended to diagnose, treat, cure, or prevent any disease. Consult a healthcare professional before making decisions about your health. Regulations regarding CBD products vary across EU member states — read our complete guide to CBD regulation in Europe and verify the legal status in your country before purchasing.

Sources and Further Reading

  • Streicher et al., 2024 — Cannabis terpenes relieve chemotherapy-induced neuropathic pain (PAIN)
  • Raz et al., 2023 — Selected cannabis terpenes synergize with THC to produce increased CB1 receptor activation (Biochemical Pharmacology)
  • LaVigne et al., 2021 — Cannabis sativa terpenes are cannabimimetic and selectively enhance cannabinoid activity (Scientific Reports)
  • Gertsch et al., 2008 — Beta-caryophyllene is a dietary cannabinoid (PNAS)
  • Russo, 2011 — Taming THC: potential cannabis synergy and phytocannabinoid-terpenoid entourage effects (British Journal of Pharmacology)
  • Liktor-Busa et al., 2021 — Analgesic potential of terpenes derived from Cannabis sativa (Pharmacological Reviews)
  • Ricardi et al., 2024 — Beta-Caryophyllene, a CB2 selective agonist, in emotional and cognitive disorders (Int J Mol Sci)
  • Spindle et al., 2024 — Vaporized D-limonene selectively mitigates the acute anxiogenic effects of Δ9-tetrahydrocannabinol in healthy adults (Drug and Alcohol Dependence)
  • Vigil et al., 2023 — Systematic combinations of major cannabinoid and terpene contents in cannabis flower and patient outcomes (Journal of Cannabis Research)
  • Komori et al., 1995 — Effects of citrus fragrance on immune function and depressive states (Neuroimmunomodulation)
  • Kim et al., 2007 — Effects of aromatherapy on postoperative nausea and vomiting and analgesic requirement (Journal of Alternative and Complementary Medicine)
  • Laws & Smid, 2024 — Neuroprotective and anti-aggregatory effects of pinene terpenes against β-amyloid-mediated toxicity
  • EFSA NDA Panel, 2026 — Update of the statement on safety of cannabidiol as a novel food (EFSA Journal)

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