Breaking Update: Here’s a clear explanation of the latest developments related to Breaking News:In axolotls and flatworms, regeneration is a body-wide choreograph– What Just Happened and why it matters right now.
Planarian flatworms are small, unassuming creatures with an astonishing talent. Cut one into pieces, and each fragment can regrow a complete animal. This seemingly magical ability comes from their prolific stem cells, known as neoblasts, which can produce every tissue in the body.
In most animals, such regenerative stem cells grow under the care of nearby niche cells, small micro-environments that signal when to divide. But planarians, despite their extraordinary powers of renewal, appear to lack any such neighbourhoods, leaving biologists puzzled about where their stem cells get their cues.
In a new study in Cell Reports, researchers at the Stowers Institute for Medical Research in Missouri, USA, found that the missing niche might not be local at all, but comes from the gut. They combined a powerful gene-mapping tool called Slide-seqV2 with electron microscopy to chart where thousands of stem cells sit and which genes they switch on. The maps revealed that neoblasts rarely stay in contact with nearby tissues, yet their activity depends on chemical messages sent from the intestine. When key intestinal genes were turned off, the usual post-injury burst of cell division disappeared and regeneration faltered; even day-to-day cell replacement changed.
“The planarian gut functions as a central regulator for whole-body regeneration,” the study’s corresponding author Alejandro Sánchez Alvarado, a molecular biologist at the Stowers Institute, said. He added that the same gut signals may also help guide routine tissue renewal across the body.
The findings don’t put the intestine in charge. Instead, they point to a cooperative system in which many tissues, including the gut, help steer stem cells through shared chemical cues. Because stem and intestinal cells sit only a few micrometres apart (roughly a single cell’s width), their conversations are likely carried by molecules such as small proteins, fats or other metabolic signals rather than direct contact.
That is to say, in planarians, regeneration seems to depend on a diffuse web of nearby chemical signals rather than a single, fixed neighborhood.
A composite image of a planarian flatworm regrowing itself from a truncated form.
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Special arrangement
Poised to heal
In another species, that same kind of long-range communication runs through the nervous system rather than the gut.
When an axolotl (Ambystoma mexicanum) loses a limb, the cells at the stump gather and multiply into a mound of tissue called the blastema, which becomes an engine of new growth. For decades, scientists believed this small structure contained a major part of the regenerative programme. But a new study in Cell by a group at the Harvard Stem Cell Institute in Massachusetts, USA, has reported that the body itself joins the act.
After amputation, a burst of activity in the animal’s stress response nerves briefly drives cells throughout the body to reenter the cycle of division. This organism-wide systemic activation seems to prime the animal for repair. When a previously uninjured limb is later amputated, its blastema is noticeably larger by two weeks.
The response was found to be carried by special proteins on cells that sensed stress signals. In distant tissues, one group of these proteins switched on a growth control system called mTOR, putting the body into a temporary state of readiness. At the injury site, another group kept the new limb growing. In both places, the same stress hormone, norepinephrine, a close chemical cousin of adrenaline, acted as the messenger.
When the researchers blocked the animal’s stress nerves, regeneration slowed down. But when they used common blood pressure drugs to mimic or block those stress signals, they could dial the response up or down, showing that the body’s repair mode could be switched on and off chemically. The primed state itself faded after about four weeks, suggesting that regeneration is not a permanent condition but a short-lived ‘repair mode’ under the nervous system’s control.
The group also expressed suspicion that the system actively shut down this state rather than letting it fade, perhaps through a surveillance mechanism that reined in cell growth once the injury response had served its purpose.
Rethinking regeneration
The same signalling machinery exists in mammals, so scientists are now wondering if mammals could have such abilities, too. However, regenerative biologist and associate professor Jessica Whited, who led the Harvard group, strongly emphasised that any parallels to humans remain speculative.
“It could be possible that humans have latent regenerative abilities that need to be coaxed out with the proper molecular instructions, in a specific sequence,” she said, stressing that such hypotheses still require direct testing.
Her team is considering whether mammals could even trigger a similar adrenergic response after severe injury but become “stuck” before the process can proceed, a failure that could reflect molecular brakes blocking the later steps of regeneration.
Even in axolotls, she noted, regeneration is tightly confined to the wound.
“Systemically activated cells don’t grow new limbs all over the body,” she said. “They appear to be held in check by brakes that limit where and how regeneration proceeds.”
Some of these cells near the stump may themselves become blastema precursors while others might act indirectly, signalling to their neighbors to initiate growth. In both cases, she said, the process depends on communication across tissues rather than within a single compartment.
Even so, the way this global coordination works is not the same in every animal. Ken Poss, a biologist at Duke University in North Carolina in the USA, said evolution seems to have invented several ways to achieve that coordination.
“Innate regeneration as a whole certainly uses different architectures,” Dr. Poss said. “Nerves and their signals can have major, minor or no role in regeneration, depending on the species and tissue. Finding commonalities and differences helps us piece the puzzle together.”
However, those differences don’t contradict the idea of body-wide coordination; they refine it.
These studies address an outstanding question: how local is the regenerative response to injury?” Nadia Rosenthal, a researcher at Imperial College of London, said. “They reveal a more complex, coordinated response where the entire organism is involved in the regenerative process.”
Salamanders may rely on neural signals and flatworms on metabolic cues, but both, she added, expose “a dynamic balance between local responses and whole-body governance of tissue repair.”
Together, the two studies recast regeneration as a team effort, not a solo act. Whether driven by gut signals or nerve impulses, the process depends on a dialogue between the wound and the rest of the body. The next challenge is to learn how those conversations start, and how the body knows when to stop them.
Anirban Mukhopadhyay is a geneticist by training and science communicator from New Delhi.