Maria Diaz-Meco Archives - Sanford Burnham Prebys

Tag: Maria Diaz-Meco

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Cancer’s final frontier: the tumor microenvironment

AuthorMonica May
Date

September 3, 2019

tumor microenvironment

Cancer researchers are setting their sights on a new kind of cancer treatment that targets the tumor’s surrounding environment, called the tumor microenvironment, in contrast to targeting the tumor directly. 

To learn more about this approach, we spoke with cancer experts Jorge Moscat, PhD, director and professor in the Cancer Metabolism and Signaling Networks Program at Sanford Burnham Prebys; and Maria Diaz-Meco, PhD, professor in the Cancer Metabolism and Signaling Networks Program at Sanford Burnham Prebys. Both scientists recently authored a review article centered on a family of cancer-linked proteins that regulate the tumor’s microenvironment. The paper was published in Cancer Cell

What is the tumor microenvironment exactly? 
Moscat: Just like every person is surrounded by a supportive community—their friends, family or teachers—every tumor is surrounded by a microenvironment. This ecosystem includes blood vessels that supply the tumor with nutrients; immune cells that the tumor has inactivated to evade detection; and stroma, glue-like connective tissue that holds the cells together and provides the tumor with nutrients.

Diaz-Meco: These elements are similar to the three legs of a stool. If we remove all three legs, we can deliver a deadly blow to the tumor. FDA-approved drugs exist that target blood vessel growth and reactivate the immune system to destroy the tumor. The final frontier is targeting the stroma.

When did scientists realize it’s important to focus on the tumor’s surroundings—not the tumor itself? 
Diaz-Meco: Scientists have known for more than a century that the tumor’s surroundings are different from normal cells. The tissue surrounding a tumor is inflamed—tumors are often called “wounds that never heal”—and their metabolism is radically different from healthy cells. 

Moscat: The discovery of oncogenes—genes that can lead to cancer—in the 1970s shifted the field’s focus to treatments that target the tumor directly. These targeted treatments work incredibly well, but only for a short time. Cancer researchers are realizing that tumors quickly adapt to this roadblock and become treatment resistant. In addition, many oncogenes are difficult to target, earning the title “undruggable.” As a result, cancer researchers are returning their focus to the tumor microenvironment—especially the stroma. Only a handful of stroma-targeting drugs are in development. None are FDA approved.

Which cancers could benefit most from a stroma-targeting drug? 
Moscat: Pancreatic, colorectal and liver cancers stand to benefit most from a stroma-targeting drug. For example, 90% of a pancreatic tumor consists of stroma—not cancer cells. Combined, these cancers are responsible for more than 20% of all cancer deaths in the U.S. each year. 

What is the focus of your lab’s research? 
Diaz-Meco: Our lab studies the cross talk between tumors and their environment. This conversation is very complex. In addition to “talking” with the tumor, the stroma also “speaks” with the immune system. We are working to map these interactions so we can create drugs that silence this conversation—or change it. For example, we recently showed—in a mouse model that faithfully recapitulates the most aggressive form of human colorectal cancer—that by altering the stroma’s interactions with the immune system, we might make tumors vulnerable to immunotherapy. 

What do new insights into the tumor microenvironment mean for cancer drug development? 
Moscat: It’s likely that the ultimate cancer “cure” won’t be just one drug that kills the tumor cells, but a combination of therapies. I expect this will be a three-part combination treatment that stops blood vessel growth, activates the immune system to attack the tumor and targets the stroma. 

Additionally, this research shows that experimental models of cancer drug development need to take the tumor microenvironment into account. Many current models use mice that lack an immune system—in order to get the tumor to grow—or focus on the tumor in isolation. Based on our knowledge of the tumor microenvironment, this isn’t an accurate representation of human disease. 

Diaz-Meco: In our lab, we have created several animal models of cancers that preserve the immune system and mirror tumor progression. In addition to better modeling human disease, this also allows us to study cancer from its earliest beginnings. This work could lead to early interventions—before the cancer has become large and hard to treat.

Anything else you’d like to add? 
Moscat: We are truly in the golden age of cancer biology. We understand more than we ever have before. New technologies are allowing us to obtain an unprecedented amount of information—we can even map every gene that is “turned on” in a single cancer cell. I am incredibly hopeful for the future. 

Learn more about the future of cancer treatment by attending our next “Conquering Cancer” event at the Fleet Science Center. Details

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How tumors shape their environment for their benefit

AuthorSusan Gammon
Date

June 21, 2017

Tumor Cells

In a new review article published in Current Opinions in Cell Biology, Professors Jorge Moscat, Maria Diaz-Meco and their graduate student Miguel Reina-Campos summarize evidence from their labs and others of how tumor cells play a large part in converting their surroundings to promote cancer progression. The research is important for developing therapies aimed at the area surrounding a tumor—the stroma—to reduce the likelihood of drug resistance, which is the main problem that today’s cancer therapies face.

“Although tumor cells carry mutations that are responsible for their altered behavior, the ability of tumors to grow and metastasize is controlled to a surprising extent by contributions from elements supplied by normal host (patient) cells,” says Diaz-Meco. “Blood vessels that provide nutrients to tumors are a good example of host elements that are critical for tumor growth and metastasis, but other host components such as fat cells, fibroblasts, and immune cells also contribute in important ways to tumor progression. These host components are known collectively as the tumor stroma or tumor microenvironment (TME).”

Different types of host stromal cells in the TME also contribute to a tumor’s ability to use different energy sources, and in turn are themselves influenced by the tumor’s metabolic activity. Reina-Campos points to cancer associated fibroblasts (CAFs) and pancreatic stellate cells (PSCs) as two cell types that interact with pancreatic cancer cells. He explains, “Under nutrient stress, PSCs can use a cell process called autophagy to produce the amino acid alanine, while CAFs produce the amino acid glutamine. Both of these amino acids serve as rich energy sources for the pancreatic tumor cells, which otherwise would have to rely on glucose—a less potent nutrient source.”

In addition to providing nutrients, CAFs and PSCs are also the source of fibrous material known as the extracellular matrix (ECM). The ECM is a potent stimulus for tumor progression and metastasis and is a particularly abundant component of pancreatic tumors. The authors stress that the properties of CAFs and PSCs in the TME are different from those of normal fibroblast and stellate cells, leading to the important concept that the stromal cells are strongly influenced by signals from the tumor cells, and reciprocally (once educated by the tumor cells) can sustain their growth to higher levels of malignancy.

Immune cells are another key TME component whose properties are profoundly influenced by tumor cells, and in turn have a significant ability to promote tumor growth. Moscat explains, “Given that the normal job of immune cells is to seek out and destroy abnormal invaders, the ability of tumors to convert immune cells into tumor promoting agents is really striking. Several different types of immune cells are re-programmed by tumors as a means of suppressing an anti-tumor immune response and generating a tumor promoting response”.

Overall, these studies reveal a number of ways by which tumor cells signal to stromal cells and, conversely, by which stromal cells signal back to tumors. Further defining these tumor-to-stroma and stroma-to-tumor signals can lead to deeper understanding of mechanisms of tumor-stroma crosstalk. Ideally, such mechanisms could then be inhibited by drugs as a means of improving tumor therapy, possibly in combination with other novel forms of cancer therapy that boost immune function.

Read the paper online here.

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High levels of protein p62 predict liver cancer recurrence

AuthorJessica Moore
Date

May 19, 2016

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CANCER METABOLISM AND SIGNALING NETWORKS PROGRAM

New research from SBP and UC San Diego shows that high levels of the protein p62 in human liver samples are strongly associated with cancer recurrence and reduced patient survival. p62 was also found to be required for liver cancer to form in mice. Continue reading “High levels of protein p62 predict liver cancer recurrence”

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Molecular “brake” prevents excessive inflammation

AuthorGuest Blogger
Date

February 25, 2016

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Inflammation is a catch-22: the body needs it to eliminate invasive organisms and foreign irritants, but excessive inflammation can harm healthy cells, contributing to aging and sometimes leading to organ failure and death. A study published in Cell, co-authored by Jorge Moscat, PhD, and Maria Diaz-Meco, PhD, professors in SBP’s NCI-designated Cancer Center, in collaboration with the laboratory of Michael Karin, PhD, at the University of California, San Diego School of Medicine, shows that a protein known as p62 acts as a molecular brake to keep inflammation in check and avoid collateral damage. Continue reading “Molecular “brake” prevents excessive inflammation”

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Pathway that controls cancer cell proliferation discovered

Authorsgammon
Date

August 13, 2015

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In a new study by SBP, researchers have identified a novel kinase cascade that regulates mTORC1, a protein complex implicated in the control of cancer cell growth in response to nutrients. The study, published in Cell Reports, provides further insight into the control of mTORC1 activation, and highlights several new potential drug targets to treat human pathologies linked to mTORC1 deregulation. Continue reading “Pathway that controls cancer cell proliferation discovered”

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New study sheds light on cancer stem cell regulation

Authorsgammon
Date

February 5, 2015

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Researchers at Sanford-Burnham have discovered a precise stem cell signaling process that can lead to intestinal tumors if disrupted. The findings add to our understanding of how stem cells give rise to tumors and identify specific stem cell molecules that may be targeted to prevent the onset, progression, and recurrence of intestinal cancers. The results of the study appear online in Cell Reports today. Continue reading “New study sheds light on cancer stem cell regulation”

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A new link between obesity, inflammation, and insulin resistance

Authorsgammon
Date

July 17, 2014

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A new study by researchers at Sanford-Burnham Medical Research Institute (Sanford-Burnham) has identified a new signal that triggers the events leading to insulin resistance in obesity. The signal causes inflammation in adipose tissue and leads to metabolic disease. The study, published July 17 in Cell Metabolism, suggests that blocking this signal may protect against the development of metabolic disease, type 2 diabetes, and other disorders caused by obesity-linked inflammation. Continue reading “A new link between obesity, inflammation, and insulin resistance”

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How tumors remodel their surroundings to grow

Authorsgammon
Date

July 7, 2014

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A team of scientists from Sanford Burnham Medical Research Institute (Sanford-Burnham) has found that the loss of a protein called p62 in the cells and tissue surrounding a tumor can enhance the growth and progression of tumors. The study suggests that therapies targeting the tumor microenvirnoment may be as important as targeting the tumor itself. Continue reading “How tumors remodel their surroundings to grow”