The molecules of feeling

In the 1990s, neuroscientist Jaak Panksepp did something extraordinary: he demonstrated that emotions are grounded in ancient, biological systems that all mammals share. Through decades of work examining hormones, neurotransmitters, peptides and steroids, he identified seven fundamental emotional experiences–CARE, SEEKING, FEAR, RAGE, LUST, GRIEF and PLAY–each guided by its own dedicated circuit.

This page lets you explore Panksepp’s ideas at a molecular level. Each emotion system has signature neurochemicals – tiny messengers with shapes, charges and folds that let them slip into just the right receptors and evoke the feelings we know so well. Here, you can rotate them, highlight their functional features and see how their structure helps give rise to the feelings you already feel every day.

Take your time. Play with the models and let yourself be a little bit amazed that those instincts that make you human all have shapes you can hold in the palm of your hand!

Oxytocin · 3D Molecular View

Rotate, zoom and highlight parts of this real oxytocin molecule to see how its shape, receptors and brain circuits support the CARE system.

Real oxytocin structure (PDB: 7OFG)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

S · sulfur

H · hydrogen

Oxytocin · CARE / PANIC–GRIEF

1. Structural role

2. Binding & circuits

3. Felt experience

Residues in focus

Oxytocin’s life cycle at the receptor

1. Oxytocin briefly docks on the oxytocin receptor, like a key touching a lock.
2. The receptor passes the message inward, nudging brain circuits toward safety, warmth and social connection.
3. Oxytocin lets go and is broken down. The receptor resets, ready for the next pulse — so the feeling comes from many tiny “you’re okay here” messages over time, not one long blast.

This widget shows an experimentally determined 3D structure of oxytocin (PDB: 7OFG) in ball-and-stick form. Most hydrogens are omitted for clarity. Oxytocin works in short pulses: it binds briefly, sends its signal, is cleared away, and the receptor is ready again — so the chemistry and the felt experience are both dynamic, not fixed.

Dopamine · 3D Molecular View

Rotate, zoom and highlight features of this real dopamine molecule to see how its shape supports the SEEKING system: curiosity, pursuit and energized engagement.

Dopamine structure (PubChem CID 681)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

H · hydrogen

Dopamine · SEEKING

1. Structural role

2. Binding & circuits

3. Felt experience

Features in focus

Dopamine’s life cycle in SEEKING

1. Dopamine is packed into tiny vesicles in dopamine neurons, waiting for something promising, surprising or important.
2. When the moment hits, dopamine is released into the synapse. It briefly touches its receptors, nudging circuits toward curiosity, effort and “go check this out”.
3. Transporters pull dopamine back in and enzymes break it down. The system resets, so SEEKING comes in short pulses instead of one long buzz.

This widget uses a real small-molecule structure for dopamine (PubChem CID 681), shown in ball-and-stick form. The highlighted regions pick out the aromatic ring, the catechol head and the amine tail — three features that help determine how dopamine fits into its receptors and supports brief, energized SEEKING bursts.

Norepinephrine · 3D Molecular View

Rotate, zoom and highlight features of this norepinephrine molecule to see how its shape supports the FEAR system: vigilance, alarm and rapid response.

Norepinephrine structure (PubChem CID 439260)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

H · hydrogen

Norepinephrine · FEAR

1. Structural role

2. Binding & circuits

3. Felt experience

Features in focus

Norepinephrine’s life cycle in FEAR

1. Norepinephrine is made from dopamine and stored in vesicles in locus coeruleus neurons and sympathetic nerves, ready for moments of possible danger.
2. When something feels threatening, norepinephrine is released into the synapse. It briefly touches adrenergic receptors, pushing circuits toward alertness, faster heart rate and “pay attention right now”.
3. Transporters pull norepinephrine back in and enzymes break it down. The system resets, so FEAR comes in short spikes of vigilance rather than a never-ending alarm.

This widget uses a real small-molecule structure for norepinephrine (PubChem CID 439260), shown in ball-and-stick form. The highlighted regions pick out the aromatic ring, the catechol head and the beta–hydroxyl/amine tail — features that help determine how norepinephrine engages its adrenergic receptors and supports fast, focused alarm responses.

Met-Enkephalin · 3D Molecular View

Rotate, zoom and highlight parts of this opioid peptide to see how it helps soften PANIC–GRIEF distress and support feelings of relief and comfort. In the brain, Met-enkephalin is part of a wider opioid family — endorphins, enkephalins, dynorphins and related peptides — which all work in slightly different ways but share the job of softening pain and distress. This little molecule is one clear example.

Met-Enkephalin peptide (PDB: 2LWC)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

S · sulfur

H · hydrogen

Met-Enkephalin · PANIC–GRIEF soothing

1. Structural role

2. Binding & circuits

3. Felt experience

Residues in focus

Met-Enkephalin’s life cycle at the receptor

1. The peptide is released from neurons during distress, pain or emotional overwhelm.
2. It briefly docks onto µ- and δ-opioid receptors, sending a “you’re safe for a moment” signal that dampens panic and eases emotional hurt.
3. Enkephalin is quickly broken down so the receptor can reset. Comfort washes in with gentle pulses, not one long numbing wave.

This widget displays Met-enkephalin using its NMR-based structure (PDB: 2LWC). Enkephalins, endorphins and dynorphins share similar receptor-binding motifs; this compact five-residue peptide illustrates the core “opioid hook → hinge → calming tail” organisation that helps soften PANIC–GRIEF responses.

Endocannabinoids · 3D Molecular View

Rotate, zoom and highlight features of this cannabinoid ligand to see how “endocannabinoid-style” molecules support the PLAY system: relaxed curiosity, social silliness and bodily ease. Your body makes endocannabinoids like anandamide and 2-AG, which share the same design idea even though they are longer, flexible fatty molecules.

Note: I had a bit of trouble with the anandamide and 2-arachidonoylgycerol renders so this is THC – similar function, different shape and, y’know, source.

Cannabinoid ligand (THC-style scaffold · PubChem CID 16078)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

H · hydrogen

Endocannabinoids · PLAY

1. Structural role

2. Binding & circuits

3. Felt experience

Features in focus

Endocannabinoid-style signalling in PLAY

1. Endocannabinoids are made “on demand” from membrane fats near active synapses.
2. They drift a short distance and bind to CB₁ receptors, softening over-eager circuits and supporting relaxed curiosity and social play.
3. Enzymes quickly break them down, creating brief pulses of “it’s okay to relax”.

This widget uses a cannabinoid ligand with a well-characterised 3D structure (a THC-style scaffold, PubChem CID 16078) as a visual stand-in. Natural endocannabinoids — anandamide and 2-AG — share the same broad design: a polar contact patch, a flexible mid-region and a long membrane-hugging tail.

Sex Steroids (Estradiol) · 3D Molecular View

Rotate, zoom and highlight features of this estradiol molecule to see how sex steroids support the LUST system: attraction, sexual motivation and bodily readiness for intimacy. Note that testosterone, the other major sex steroid, has a very similar structure and purpose. In the brain, testosterone frequently converts into estradiol, meaning both hormones act through closely overlapping molecular pathways.

Estradiol structure (PubChem CID 5757)

Element colours (CPK-style)

C · carbon

O · oxygen

H · hydrogen

Sex Steroids · LUST

1. Structural role

2. Binding & circuits

3. Felt experience

Features in focus

Estradiol’s life cycle in LUST

1. Sex steroids like estradiol and testosterone are built from cholesterol in the ovaries, testes and adrenal glands, then carried through blood on binding proteins.
2. When they reach target tissues, they slip through cell membranes and bind to steroid receptors, changing gene expression and gradually tuning brain and body toward sexual interest, sensitivity and arousal.
3. Enzymes convert and break down sex steroids over hours to days, so sexual arousal rises and falls more slowly than a quick pulse. Think of tides and seasons rather than a single spike.

This widget uses a small-molecule structure for estradiol (PubChem CID 5757), shown in ball-and-stick form. The highlighted regions pick out the rigid four-ring steroid core, the hydroxyl “hooks” and the overall scaffold that lets sex steroids slip through membranes and engage receptors that support sexual motivation and bodily readiness.

Substance P · 3D Molecular View

Rotate, zoom and highlight parts of this Substance P peptide to see how its shape, receptors and brain circuits support the RAGE / pain system.

Substance P peptide (PDB: 2KS9 · chain B)

Element colours (CPK-style)

C · carbon

O · oxygen

N · nitrogen

S · sulfur

H · hydrogen

Substance P · RAGE / pain

1. Structural role

2. Binding & circuits

3. Felt experience

Residues in focus

Substance P’s life cycle at the receptor

1. Pain-carrying nerve endings build Substance P and store it in tiny packets at their tips.
2. When tissue is damaged or boundaries are crossed, Substance P is released and binds to NK1 receptors, turning up pain, inflammation and “protect yourself now” signals.
3. Enzymes quickly chop up Substance P and the receptor is pulled inside the cell and reset — so you feel bursts of urgent alarm rather than one endless scream.

This widget uses an experimentally determined 3D structure that includes Substance P in a membrane environment (PDB: 2KS9). The view is restricted to the Substance P peptide chain (B) in ball-and-stick form. Residues 1–4, 5–6 and 7–11 are highlighted to show how the “alarm header”, “signal rail” and “attack tail” help the peptide latch onto NK1 receptors and drive strong pain and RAGE-related responses.

selected references

Important note: This article may include content generated with the assistance of AI. I have personally reviewed and approved all content to ensure its accuracy and alignment with my views.

Geoff Crane designs research-backed tools to make so-called “soft skills” concrete, measurable, and deeply human. After more than two decades in industry and another decade in personal intelligence research and program design, his work now supports coaches, educators, and organisations that want to understand people more clearly and help them grow with care.

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