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Can Nerves Stop Skin Cancer? New Study Says Yes


Melanoma growth may be slowed by harnessing involuntary nerve signals instead of sensory nerves.

The divergent roles of sensory versus sympathetic nerves unmask the dual effects of the peripheral nervous system on skin cancer (melanoma).(1 Trusted Source
A local sympathetic-immune axis inhibits melanoma growth in mice by dictating adrenergic control

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While sensory nerves, which handle sensations like pain and itch, were found to promote tumor growth, the ‘fight-or-flight’ (sympathetic) nerves surprisingly inhibited melanoma progression. This contradicts the general view that the nervous system fuels cancer.

The study, led by researchers at Weill Cornell Medicine and published in the journal Neuron, shows that sympathetic nerves act as a natural brake against skin cancer.

By releasing specific signals, these nerves reprogram macrophages (immune cells) that often support tumors to stop fueling the disease. The discovery marks a shift in melanoma research, suggesting that targeting the nervous system could lead to new immunotherapy strategies.

The nervous system typically has been considered as a driver of cancer growth, but here we’ve found that it can be a brake on cancer growth in some contexts,” said study senior author Dr. David J. Simon, an assistant professor of biochemistry and biophysics at Weill Cornell Medicine. “Now the key will be to see how broadly relevant this is for human cancers, and how we can best step on that brake to help cancer patients.”

Nerve Signals Act as a Critical Regulator of Skin Cancer Outcomes

The peripheral nervous system is the tree-like system of nerves that extends outside the brain and spinal cord. It includes the sensory nerves that underlie feelings such as heat and cold, pain and itch. Further, it includes the nerves of the sympathetic nervous system, which transmit signals from the brain to influence the functions of various organs.

In the skin, most sympathetic nerve fibers can release the stress hormone norepinephrine, affecting immune cells, sweat glands and other targets as part of the “fight-or-flight” response.

Peripheral nerves are commonly found in tumors, but it is only in recent years that researchers have begun examining the roles of these nerves in cancer outcomes. Most of these investigations have found that sensory and sympathetic nerves can enhance tumor growth, for example by releasing molecules that suppress antitumor immunity.

In just the last few years, however, there have been hints that peripheral nerves in some cases may be able to slow tumor growth instead.

Turning Tissue Samples Transparent to Trace Nerve Paths in Tumors

Dr. Simon and his team have expertise in studying the growth and survival of peripheral nerve fibers, especially those that grow into the skin. “We knew that these nerves entered melanoma, but studying their role in cancer growth was not our main goal,” said Dr. Simon.

“But we were fortunate to receive generous early-stage support from the Pershing Square Sohn Cancer Research Alliance that allowed us to take a risk and explore these nerve-tumor interactions in detail.”

“We used a technique called whole mount immuno-labeling, in which an entire tissue sample is made optically transparent, to count, identify and trace the paths of the nerves in the tumors,” said study first author Dr. Tingting Liu, a postdoctoral research associate in the Simon Lab.

These initial investigations revealed that pain-sensitive nerves and sympathetic nerves were prevalent in the melanomas, increasing in number as the tumors grew, particularly in slower-growing tumors. The pain-sensitive nerves, consistent with prior studies, appeared to have a pro-tumor effect—depleting them inhibited tumor growth—but the sympathetic nerves surprisingly exerted an anti-tumor effect.

Nerve Signaling Reprograms Macrophages to Halt Tumor Growth

The sympathetic nerves identified in the study release norepinephrine, which can activate receptors called adrenergic receptors on other cells in the vicinity. The researchers traced the anti-tumor effect in their models to a subset of adrenergic receptors called alpha adrenergic receptors.

They identified immune cells called macrophages as the key cellular targets of this alpha adrenergic signaling. Tumors often turn macrophages into allies, for example by switching them into an immunosuppressive mode, but the alpha adrenergic signaling reduced the numbers of such pro-tumor macrophages, thereby slowing tumor growth.

The findings open up the prospect of future anti-cancer therapies that target sympathetic nerves within tumors, or even the alpha adrenergic receptors on tumor-associated macrophages. Drugs targeting these receptors are already in use as common blood pressure medicines.

For now, Dr. Simon plans to continue with more fundamental research, for example to tease apart how these adrenergic receptors are activated and signal in actual cancers in humans. “There’s a lot still to do in terms of the basic biology here,” he said.

Reference:

  1. A local sympathetic-immune axis inhibits melanoma growth in mice by dictating adrenergic control – (https://www.cell.com/neuron/abstract/S0896-6273(26)00285-0)

Source-Eurekalert

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