News Release

Nutrients and organelle signaling shape tissue immunity

Scientists at St. Jude Children’s Research Hospital have shown that nutrient availability and organelle biology affect the development of tissue-resident memory T cells.

Peer-Reviewed Publication

St. Jude Children's Research Hospital

Researchers at St. Jude Children’s Research Hospital discovered that nutrient availability and organelle signaling influence tissue-resident memory T cells (TRM) development, highlighting a critical link between metabolism and immunity.

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(L to R) Corresponding author Hongbo Chi, PhD, and first author Jana Raynor, PhD, St. Jude Department of Immunology.

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Credit: Courtesy of St. Jude Children's Research Hospital

(MEMPHIS, Tenn. – October 14, 2024) – The ability to therapeutically manipulate the immune system presents a multitude of potential opportunities for treating infectious diseases, cancer and other diseases, but first, researchers must fully understand the processes that shape immunity. Scientists at St. Jude Children’s Research Hospital have added another piece to the puzzle, showing how metabolic factors influence tissue immunity in an intricate interplay between nutrient availability, organelle biology and tissue-resident memory T (TRM) cell development. The team found that TRM cells rely on mitochondrial activity for development and are inhibited by nutrient-sensing pathways in lysosomes. The findings were published today in Immunity.

 

“We are excited to introduce a new layer of regulation in tissue immunity, which we believe will significantly enhance our understanding of this field. Our findings have the potential to inform new strategies for modulating tissue immunity, particularly for improving anti-infection responses,” said corresponding author Hongbo Chi, PhD, St. Jude Department of Immunology.

 

The crucial role of memory T cells

 

CD8+ T cells are vital in defending against infections and cancer while promoting tissue health. During primary infections, they differentiate into effector cells, which provide immediate responses, and memory cells, which persist long-term for quicker responses upon re-exposure. TRM cells are a specialized subset of memory cells that remain in tissues, offering rapid, localized responses by monitoring for signs of infection. Their ability to act as first responders enhances tissue-specific immunity, making them crucial for effective adaptive or long-term immunity.

 

“Our study focuses on tissue immunity, specifically examining TRM cell formation,” said first author Jana Raynor, PhD, St. Jude Department of Immunology. “These cells migrate to specific tissues — such as the lungs, intestines or skin — and establish long-term residency. They help provide the first line of defense against infections, and TRM-like cells are increasingly recognized for their role in responding to tumors.”

 

TRM and TRM-like cells are of great interest due to their potential use in immunotherapy since they provide rapid, localized immune responses at the site of infection or tumor growth. Their long-term presence in tissues ensures lasting immunity and strong immune memory, allowing rapid reactions to previously encountered pathogens or cancer cells.

 

Organelle signaling and immune cell development

 

The researchers used CRISPR-Cas9 genetic screens to uncover critical signaling pathways influencing TRM cell development and differentiation. They found that TRM cell formation depends on processes in cellular organelles called mitochondria. Additionally, signaling nodes at the lysosome (another organelle), such as Folliculin (Flcn), Ragulator and Rag GTPases, restrict TRM formation and development.

 

“What we found particularly intriguing was that Flcn-mediated regulation is specific to the intestine, making this the first identified negative regulator of TRM cells at a localized site,” said Raynor. “We’re excited about targeting this pathway to enhance long-term TRM cells in the gut, as our study shows that increased Flcn-deficient TRM cell levels provide better protection against infections.”

 

Apart from organelle signaling, the study also found that nutrient availability played a role in tissue immunity. Specifically, Flcn modulates the activity of transcription factor EB (Tfeb). Flcn–Tfeb signaling, induced by amino acid deprivation, contributes to TRM cell development. The relationship links nutrient stress to cell fate decisions. Therefore, the Flcn–Tfeb axis is a regulatory pathway that coordinates immune responses to nutrient availability and lysosomal function.

 

“T cells migrate to various tissues and must adapt to the local nutrient environment. Our research uncovers the mechanisms by which T cells adjust to extracellular nutrient conditions and connect them to a key intracellular organelle, lysosome,” said Chi. “This discovery further cements the emerging concept we helped champion that nutrients serve as a unique type of signal, known as ‘Signal 4,’ to license T-cell immunity”.

 

This work underscores metabolism-associated mechanisms that drive immune memory response to occur in a highly tissue-specific manner, showcasing promising future applications such as dietary interventions, vaccination strategies and personalized medicine approaches.

 

“We’re particularly excited about the potential of nutrient availability and diet, as it’s something individuals can actively manage and apply. Exploring how to modulate nutrition may significantly influence the establishment of stronger immune responses,” added Raynor.

 

Authors and funding

The study’s other authors are Hao Shi, Clifford Guy, Jordy Saravia, Nicole Chapman, Yan Wang, Yu Sun, Anil KC, Renqiang Sun, Jon Connelly and Shondra Pruett-Miller, all of St. Jude; Seon Ah Lim, Peipei Zhou, Isabel Risch, Haoran Hu, Sharad Shrestha and Hongling Huang, formerly of St. Jude; Nicholas Collins, formerly of the National Institutes of Health, now of Weill Cornell Medicine; Miguel Reina-Campos, formerly of the University of California San Diego, now of La Jolla Institute for Immunology; Ananda Goldrath, formerly of the University of California San Diego, now of Allen Institute for Immunology; Yasmine Belkaid, formerly of National Institutes of Health, now of Pasteur Institute.

 

The study was supported by grants from the National Institutes of Health (CA253188, AI131703, Al105887, Al140761, Al150241 and Al150514), the St. Jude Comprehensive Cancer Center Support Grant (P30 CA021765) and ALSAC, the fundraising and awareness organization of St. Jude.

 

St. Jude Media Relations Contacts

Michael Sheffield
Desk: (901) 595-0221
Cell: (901) 379-6072
michael.sheffield@stjude.org
media@stjude.org

 

Rae Lyn Hartley

Cell: (901) 686-2597

raelyn.hartley@stjude.org

media@stjude.org

 

St. Jude Children's Research Hospital

St. Jude Children's Research Hospital is leading the way the world understands, treats and cures childhood cancer, sickle cell disease and other life-threatening disorders. It is the only National Cancer Institute-designated Comprehensive Cancer Center devoted solely to children. Treatments developed at St. Jude have helped push the overall childhood cancer survival rate from 20% to 80% since the hospital opened more than 60 years ago. St. Jude shares the breakthroughs it makes to help doctors and researchers at local hospitals and cancer centers around the world improve the quality of treatment and care for even more children. To learn more, visit stjude.org, read St. Jude Progress, a digital magazine, and follow St. Jude on social media at @stjuderesearch

 


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