The breast cancer microenvironment and cancer cell secretion - specific effects on cancer progression and subtypes of cancer cells
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Date
2021-01-22
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Abstract
Breast cancer is the cancer form responsible for the most cancer-related deaths
among women worldwide, and novel targeted therapies are highly needed. The
tumor microenvironment consists of several components, including different
cell types, extracellular matrix, oxygen and nutrient gradients and soluble
factors that plays a key role in cancer progression. Cancer cell secretion affects
tumor characteristics, such as proliferation, migration, invasion and priming of
the pre-metastatic niche. In this thesis, we have investigated the effect of tumor
microenvironmental-induced secretion by studying hypoxia and the
extracellular matrix and the induction of secretion in relation to cancer
progression and subpopulations of breast cancer cells. We demonstrated that
hypoxia-induced secretion affects the cancer stem cell subpopulation, but in
opposing directions depending on estrogen receptor status. Moreover, by
developing a novel in vivo-like model based on decellularized breast cancer
tissue we could show induced changes in reintroduced cell lines in gene
expression and cell secretion, both towards a more dedifferentiated cell state
compared to monolayer cells. In addition, we demonstrated that one subgroup
of decellularized breast cancers induced secretion of proteins such as
interlukin-6, chemokine (C-C motif) ligand 2 and plasminogen activator
inhibitor 1, all associated with cancer stem cell characteristics and priming of
the pre-metastatic niche. This subgroup also included tumors of higher grade
and with shorter patient relapse-free survival, further displaying the
aggressiveness of these microenvironments. Further, we revealed that the wellknown cancer stem cell inducing cytokine interlukin-6 increased after
treatment with the hypoxia-induced growth factor progranulin and that
interlukin-6 increased the cancer stem cell propagation in a sortilin dependent
way. In conclusion, in this thesis we explored the importance of the tumor
microenvironment and continued to unravel the complex network of tumor
microenvironmental-induced secretion and the significance for breast cancer
progression and patient outcome.
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Keywords
Breast cancer, cancer microenvironment, secretion, hypoxia