Welcome to the next episode of the WOrM Podcast 🪱

Today we’re looking at something deceptively simple: a turn.

But not just that a worm turns —

how the brain decides to do it.

⸻

🧬 The central idea

Turning in C. elegans is not a reflex.

It’s a sequence.

A structured, repeatable pattern of neural activity that links:

• sensation

• decision

• and movement

into a single behavioural output.

⸻

🔬 What’s really happening?

Using whole-brain calcium imaging, this study captures activity across the nervous system during olfactory navigation.

What emerges is clear:

• turns act as error-correction events

• they occur when the worm deviates from its path

• and they are executed through ordered neural sequences

Each turn is not random.

It is built.

⸻

⚡ A sequence, not a signal

During a turn:

• specific neurons activate

• in a stereotyped order

• across time

Some neurons respond to sensory cues.

Others anticipate the direction of the upcoming turn.

This is not reaction.

It is prediction unfolding in time.

⸻

🧠 The role of modulation

A key player here is tyramine.

It helps coordinate these neural sequences —

linking circuit structure to dynamic control of behaviour.

So the system is not just wired.

It is tuned.

⸻

🧠 The take-home message

Behaviour is not the output of single neurons.

It is the product of time-ordered neural activity.

In this case:

sensory input → neural sequence → predicted action

And the shift is important:

To understand behaviour, we need to think in time, not just space.

⸻

📄 Paper discussed

Kramer, T. S.; Wan, F. K.; Pugliese, S. M.; Atanas, A. A.; Pradhan, S.; Hiser, A. W.; Godinez, L. M.; Luo, J.; Bueno, E.; Felt, T.; Flavell, S. W. (2026)

Neural sequences underlying directed turning in Caenorhabditis elegans

Nature

https://doi.org/10.1038/s41593-026-02257-5

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

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🔗 www.veerenchauhan.com

📧 veeren.chauhan@nottingham.ac.uk

Welcome to the next episode of the WOrM Podcast 🪱

Today we flip the usual perspective.

We often think about how the environment shapes the worm.

But what if the worm is shaping the environment?

⸻

🧬 The central idea

C. elegans doesn’t just respond to microbes — it actively reshapes microbial communities.

Across a naturalistic “boom-to-bust” lifecycle, worm populations:

• expand rapidly

• consume and interact with bacteria

• then collapse into dauer

And through that process, they leave a lasting imprint on their surroundings.

⸻

🌱 What happens to the environment?

Even without worms, microbial communities change over time.

But with worms present, something different happens:

• microbial communities follow distinct trajectories

• initially different environments begin to converge

• specific bacterial families are consistently depleted or enriched

In other words, worms don’t just graze — they engineer microbial ecosystems.

⸻

🦠 The microbiome connection

The key link is the worm’s own gut microbiome.

Bacterial families that:

• thrive inside the worm

• are selected during feeding

are the same ones that become enriched in the environment.

While others — like Pseudomonadaceae — are depleted over time.

So the worm is not just consuming bacteria.

It is:

• selecting

• amplifying

• and redistributing microbial populations

⸻

⚡ A bidirectional system

This is the important shift.

We move from:

environment → worm

to:

environment ↔ worm

A feedback loop where:

• microbes shape the worm

• worms reshape microbes

• and the ecosystem evolves as a result

⸻

🧠 The take-home message

C. elegans is not just a model organism.

It’s an ecosystem engineer.

And this matters, because nematodes are one of the most abundant life forms on Earth.

So small-scale interactions — feeding, microbiome assembly, population cycles — may scale up to influence:

• nutrient cycling

• microbial diversity

• and ecosystem function

⸻

📄 Paper discussed

Bodkhe, R.; Sankaran, K.; Shapira, M. (2026)

Caenorhabditis elegans populations shape their microbial environment

npj Biofilms and Microbiomes

DOI: 10.1038/s41522-026-00975-z

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication or product featured on the show, please get in touch.

📩 More info:

🔗 www.veerenchauhan.com

📧 veeren.chauhan@nottingham.ac.uk

Welcome to the next episode of the WOrM Podcast 🪱

Today we’re talking about something fundamental — feeding behaviour — but through a lens you might not expect.

Not calories.

Not food availability.

But fat composition.

⸻

🧬 The central idea

In C. elegans, feeding isn’t just about energy — it’s about lipid balance.

Specifically, the ratio of:

• saturated fatty acids (SFAs)

• and monounsaturated fatty acids (MUFAs)

And this balance determines whether worms:

• stay on food

• leave food

• or actively ignore it

⸻

🔬 What’s really being sensed?

This isn’t happening at the surface.

It’s happening at the endoplasmic reticulum (ER) — where lipid composition alters membrane properties and activates the stress sensor IRE-1.

That signal is then translated into behaviour through:

• neuronal serotonin

• AMPK signalling

• and a neuropeptide system

⸻

⚡ A new behavioural state: “food apathy”

One of the most interesting outcomes in this study is a state the authors call food apathy.

Worms:

• leave concentrated food

• roam even when food is present

• and reduce overall intake

This is not starvation.

It’s not avoidance of toxins.

It’s a metabolically driven behavioural shift.

⸻

🧠 The big connection: GLP-1-like signalling

Here’s where it gets very interesting.

The pathway that drives this behaviour — PDF-1 / PDFR-1 — shows structural and functional similarity to:

• GLP-1

• GIP

• glucagon-related signalling

In other words, the same systems now targeted by weight-loss drugs may have deep evolutionary roots in simple organisms like worms.

Even more striking — a peptide derived from this worm pathway shows:

• reduced food intake

• improved insulin sensitivity

in mice.

⸻

🧠 The take-home message

Feeding behaviour is not just about hunger.

It’s about how metabolism is sensed and interpreted.

In this case:

lipids → ER stress → neuronal signalling → behaviour

And the implication is big:

Some of the most important metabolic signalling systems in humans may have started as basic lipid-sensing circuits in simple organisms.

⸻

📄 Paper discussed

Zhu, F.; Castillo-Quan, J. I.; Ogawa, T.; Wu, Z.; Ding, L.; Sura, M.; Watanabe, Y.; Lentsch, H.; Fernández-Cárdenas, L. P.; Dag, U.; Beck-Sickinger, A.; Wang, M. C.; Kahn, C. R.; Blackwell, T. K. (2026)

Fatty acid regulation of feeding in Caenorhabditis elegans reveals the potential ancestral origin of a GLP-1-like multiagonist signaling system

Proceedings of the National Academy of Sciences (PNAS)

DOI: 10.1073/pnas.2530979123

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

📩 More info:

🔗 www.veerenchauhan.com

📧 veeren.chauhan@nottingham.ac.uk

Welcome to the next episode of the WOrM Podcast 🪱

Today we’re looking at something surprisingly familiar in worm biology: alcohol.

But not just exposure — we’re talking about behaviour, tolerance, withdrawal, and how core neurotransmitter systems shape all of it.

⸻

🧬 The central question

What actually happens when a worm is exposed to ethanol?

Not just in terms of movement — but across:

• behaviour

• lifespan

• neuronal signalling

• and gene expression

This study takes a multi-layered approach to understand how alcohol reshapes the worm.

⸻

🔬 What they did

Worms were exposed to ethanol for 24 hours, followed by a withdrawal phase, and then tested in a behavioural assay — the classic diacetyl race.

This creates a simple but powerful 3-step model:

1. exposure

2. withdrawal

3. re-exposure

A framework that starts to look a lot like tolerance biology.

⸻

🧠 What they found

The response to ethanol isn’t uniform — it depends on the nervous system.

• Wild-type worms show reduced lifespan at higher ethanol doses

• Dopamine (dop-3) and serotonin (tph-1) mutants respond differently

• Behaviour during chemotaxis is altered — not just slower, but less coordinated

• Re-exposure can rescue or worsen behaviour, depending on genotype

This is not just toxicity.

It’s state-dependent behaviour.

⸻

⚡ Neurons are doing the work

At the cellular level, ethanol increases vesicle exocytosis in both dopaminergic and serotonergic neurons.

So the system is not shutting down — it’s being actively rewired.

And importantly, intact dopamine and serotonin signalling are required for normal responses to ethanol.

⸻

🧪 The molecular layer

Ethanol exposure also shifts gene expression:

• Stress response genes like gst-4 and sod-3 are altered

• Metabolic genes like adh-1 are downregulated

• The response differs depending on dopamine and serotonin function

So behaviour, neurons, and metabolism are all coupled.

⸻

🧠 The take-home message

Ethanol in C. elegans is not just a stressor.

It’s a probe.

A way to reveal how:

• neurotransmitters

• behaviour

• and metabolism

interact at the whole-organism level.

And the key point?

You don’t get the phenotype without the network.

⸻

📄 Paper discussed

Rubio-Tomás, T.; Hunn, C. A.; Hajdú, G.; Sőti, C.; Tavernarakis, N.; Barta, C. (2026)

Specific genes of the dopaminergic (dop-3) and serotonergic (tph-1) pathways contribute to the effects of ethanol consumption in Caenorhabditis elegans

PLOS One, 21(3): e0344966

DOI: 10.1371/journal.pone.0344966

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

📩 More info:

🔗 www.veerenchauhan.com

📧 veeren.chauhan@nottingham.ac.uk

Welcome to the next episode of the WOrM Podcast 🪱🎬

Today we’re stepping slightly outside the lab… but not too far.

We’re asking a serious question with absolutely no serious consequences:

If there were an Oscar for Best Giant Movie Worm, who would win?

⸻

🪱 From soil to cinema

Worms in biology are elegant, transparent, genetically tractable.

Worms in film?

They’re enormous.
They’re apocalyptic.
They swallow cities.

From desert-dwelling leviathans to subterranean monsters shaking small towns apart, giant worms have carved out a strange and persistent niche in popular culture.

⸻

🎥 Why are we obsessed with giant worms?

There’s something primal about them.

No eyes.
No clear front or back.
Emerging from below.

They represent unpredictability — something ancient and unstoppable.

But what’s interesting is how different films use them.
Sometimes they’re villains.
Sometimes ecological forces.
Sometimes metaphors for nature pushing back.

⸻

🧠 The worm perspective

Here’s the twist.

Real worms are foundational to ecosystems. They aerate soil, regulate microbes, recycle nutrients.

They are engineers of the environment.

Cinema flips that script and scales them up into existential threats.

It’s fascinating how the same body plan — elongated, segmented, simple — can be interpreted as either ecological hero or planetary horror.

⸻

🏆 So who wins?

This episode walks through the contenders, looks at design, biological plausibility (yes, we go there), cultural impact, and sheer screen presence.

Because if we’re going to award an Oscar for Best Giant Movie Worm…

We need criteria.

⸻

🪱 The take-home message

Even in fiction, worms capture something fundamental.

They tap into scale, fear, ecology, and the unknown.

And maybe that’s why, whether under a microscope or under a desert planet, worms continue to fascinate us.

⸻

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

📩 More info:
🔗 www.veerenchauhan.com
📧 veeren.chauhan@nottingham.ac.uk

Welcome to the next episode of the WOrM Podcast 🪱

Today we return to a core question in worm biology: when stress extends lifespan, what is really doing the work?

Is it damage repair?
Is it signalling rewiring?
Or is it something more coordinated at the whole-organism level?

In this episode we explore new insights into how longevity pathways intersect with stress signalling in C. elegans, and what this means for how we interpret lifespan extension.

⸻

🧬 The central idea

Many longevity paradigms begin with a perturbation — mitochondrial disruption, metabolic alteration, environmental stress — and end with a longer-lived worm.

But the key question is not whether lifespan increases.

It’s why.

This paper dissects the signalling architecture behind stress-induced longevity and challenges overly simple models where one pathway equals one outcome.

⸻

🔬 What’s happening under the hood?

Rather than acting in isolation, canonical longevity regulators intersect with stress-activated signalling networks.

We see coordination between:
• stress response transcription factors
• metabolic regulators
• immune signalling components
• and tissue-specific effects

The result is not just stress resistance — but systemic adaptation.

⸻

🧠 Why this matters

In worm biology, lifespan extension is often treated as the final readout.

But lifespan is an emergent property.

It reflects how well the organism integrates:
• damage sensing
• metabolic state
• immune tone
• and signalling fidelity

This episode steps back and asks whether we should think less about single “longevity genes” and more about network behaviour across the whole animal.

⸻

🪱 The worm lesson

C. elegans continues to show us that longevity is rarely about silencing stress.

It’s about interpreting it correctly.

Stress is not always damage.
Sometimes it’s information.

⸻

📄 Paper discussed

TJ O’Brien, EP Navarro, C Barroso, L Menzies, E Martinez-Perez, D Carling, AEX Brown
High-throughput behavioural phenotyping of 25 C. elegans disease models including patient-specific mutations
BMC Biology 23:281

⸻

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others in the community find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

📩 More info:
🔗 www.veerenchauhan.com
📧 veeren.chauhan@nottingham.ac.uk

Today we’re talking about a molecule that keeps popping up in “healthy ageing” conversations: cordycepin (3′-deoxyadenosine) 🍄

But instead of vague claims, we’re going to ground this in C. elegans data — lifespan, stress resistance, movement, oxidative stress markers, and what happens to lipids along the way.

⸻

🧬 What’s the question?

Cordycepin is linked to antioxidant, anti-inflammatory and neuroprotective effects, but its anti-ageing mechanism hasn’t been clear. This paper asks a simple question: does cordycepin extend worm lifespan, and if so — how?

⸻

⏱️ What they found in worms

Cordycepin extended lifespan under normal conditions and under heat stress. At the higher dose (2 mg/mL), mean lifespan increased by ~28.5% compared with controls.

It also improved healthspan-type measures: better locomotion (head swings), reduced age pigment lipofuscin, and lower oxidative stress.

Importantly, the authors report no obvious cost in body size or reproduction under their conditions.

⸻

🧪 The mechanism in plain terms

The story here has two big parts:

1) Antioxidant protection ✅

Cordycepin reduced ROS accumulation and increased antioxidant enzyme activities (CAT, SOD, GSH-PX).

2) Fatty acid metabolism gets rewired 🧈

Metabolomics showed cordycepin shifted multiple metabolites — notably decreasing linoleic acid and oleic acid, alongside changes in other metabolic intermediates.

Transcriptomics pointed to upregulation of fatty-acid and β-oxidation–linked genes, including acox-1.2/1.3/1.4, acs-1, acs-15, acdh-1, acdh-4, acdh-8, with pathway enrichment in fatty acid degradation/metabolism, peroxisome and related networks.

So the argument is: cordycepin extends lifespan by strengthening oxidative stress defences and shifting lipid handling in a pro-longevity direction.

⸻

🧠 The take-home message

Cordycepin isn’t framed here as a magic bullet — it’s framed as a compound that pushes two core ageing levers in worms: redox balance and fatty acid metabolism.

If you work on stress, metabolism, lipid biology, or whole-organism ageing, this one is worth a look.

⸻

📄 Paper discussed

Sun, Y.; Zhong, M.; Wang, J.; Feng, M.; Shen, C.; Han, Z.; Cao, X.; Zhang, Q. (2025). Cordycepin extends the longevity of Caenorhabditis elegans via antioxidation and regulation of fatty acid metabolism. European Journal of Pharmacology, 994, 177388. DOI: 10.1016/j.ejphar.2025.177388

⸻

If you enjoyed this episode, please like, follow, and subscribe wherever you listen to the WOrM Podcast ⭐🎧 It really helps others find the show.

This podcast is generated with artificial intelligence and curated by Veeren. If you’d like your publication featured on the show, please get in touch.

📩 More info:

🔗 www.veerenchauhan.com

📧 veeren.chauhan@nottingham.ac.uk