Formation of an invasion-permissive matrix requires TGFβ/SNAIL1-regulated alternative splicing of fibronectin

Formation of an invasion-permissive matrix requires TGFβ/SNAIL1-regulated alternative splicing of fibronectin

As in most solid cancers, the emergence of cells with oncogenic mutations in the mammary epithelium alters the tissue homeostasis. Some soluble factors, such as TGFβ, potently modify the behavior of healthy stromal cells. A subpopulation of cancer-associated fibroblasts expressing a TGFβ target, the...

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Bibliographic Details
Published in:Breast cancer research : BCR Vol. 25; no. 1; p. 143
Main Authors: Franco-Valls, Héctor, Tusquets-Uxó, Elsa, Sala, Laura, Val, Maria, Peña, Raúl, Iaconcig, Alessandra, Villarino, Álvaro, Jiménez-Arriola, Martín, Massó, Pere, Trincado, Juan L, Eyras, Eduardo, Muro, Andrés F, Otero, Jorge, García de Herreros, Antonio, Baulida, Josep
Format: Journal Article
Language:English
Published: England BioMed Central 14-11-2023
BMC
Subjects:
Alternative Splicing
Animals
Antibodies
Breast cancer
Breast Neoplasms - genetics
Cell activation
EDA+ Fibronectin
Epithelium
Extracellular matrix
Female
Fibroblasts
Fibronectin
Fibronectins - genetics
Fibronectins - metabolism
Homeostasis
Humans
Isoforms
Lung cancer
Lung Neoplasms
Matrix architecture
Mechanical properties
Medical prognosis
Metastases
Metastasis
Mice
Protein Isoforms - genetics
Protein Isoforms - metabolism
Proteins
Serine-Arginine Splicing Factors - genetics
Serine-Arginine Splicing Factors - metabolism
Skin cancer
Snail protein
SNAIL1
Splicing factors
Stromal cells
TGFβ
Transforming Growth Factor beta - metabolism
Tumors
SNAIL1
Matrix architecture
EDA+ Fibronectin
TGFβ
Extracellular matrix
Breast cancer
Matrix rigidity
Metastasis
Myofibroblasts
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Summary:As in most solid cancers, the emergence of cells with oncogenic mutations in the mammary epithelium alters the tissue homeostasis. Some soluble factors, such as TGFβ, potently modify the behavior of healthy stromal cells. A subpopulation of cancer-associated fibroblasts expressing a TGFβ target, the SNAIL1 transcription factor, display myofibroblastic abilities that rearrange the stromal architecture. Breast tumors with the presence of SNAIL1 in the stromal compartment, and with aligned extracellular fiber, are associated with poor survival prognoses. We used deep RNA sequencing and biochemical techniques to study alternative splicing and human tumor databases to test for associations (correlation t-test) between SNAIL1 and fibronectin isoforms. Three-dimensional extracellular matrices generated from fibroblasts were used to study the mechanical properties and actions of the extracellular matrices on tumor cell and fibroblast behaviors. A metastatic mouse model of breast cancer was used to test the action of fibronectin isoforms on lung metastasis. In silico studies showed that SNAIL1 correlates with the expression of the extra domain A (EDA)-containing (EDA+) fibronectin in advanced human breast cancer and other types of epithelial cancers. In TGFβ-activated fibroblasts, alternative splicing of fibronectin as well as of 500 other genes was modified by eliminating SNAIL1. Biochemical analyses demonstrated that SNAIL1 favors the inclusion of the EDA exon by modulating the activity of the SRSF1 splicing factor. Similar to Snai1 knockout fibroblasts, EDA- fibronectin fibroblasts produce an extracellular matrix  that does not sustain TGFβ-induced fiber organization, rigidity, fibroblast activation, or tumor cell invasion. The presence of EDA+ fibronectin changes the action of metalloproteinases on fibronectin fibers. Critically, in an mouse orthotopic breast cancer model, the absence of the fibronectin EDA domain completely prevents lung metastasis. Our results support the requirement of EDA+ fibronectin in the generation of a metastasis permissive stromal architecture in breast cancers and its molecular control by SNAIL1. From a pharmacological point of view, specifically blocking EDA+ fibronectin deposition could be included in studies to reduce the formation of a pro-metastatic environment.
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ISSN:1465-542X
1465-5411
1465-542X
DOI:10.1186/s13058-023-01736-y