Showing papers by "Yibin Kang published in 2018"
TL;DR: It is reported that a glutaminolytic enzyme, glutamate dehydrogenase 1 (GDH1), upregulated upon detachment via pleomorphic adenoma gene 1 (PLAG1), provides anti-anoikis and pro-metastatic signals in LKB1-deficient lung cancer.
159 citations
TL;DR: In this article, a non-linear hysteretic response of E-cadherin repression was found to be tightly controlled by the strength of the miR-200s/ZEBs negative feedback loop.
Abstract: Epithelial-mesenchymal transition (EMT) have been extensively characterized in development and cancer, and its dynamics have been modeled as a non-linear process. However, less is known about how such dynamics may affect its biological impact. Here, we use mathematical modeling and experimental analysis of the TGF-β-induced EMT to reveal a non-linear hysteretic response of E-cadherin repression tightly controlled by the strength of the miR-200s/ZEBs negative feedback loop. Hysteretic EMT conveys memory state, ensures rapid and robust cellular response and enables EMT to persist long after withdrawal of stimuli. Importantly, while both hysteretic and non-hysteretic EMT confer similar morphological changes and invasive potential of cancer cells, only hysteretic EMT enhances lung metastatic colonization efficiency. Cells that undergo hysteretic EMT differentially express subsets of stem cell and extracellular matrix related genes with significant clinical prognosis value. These findings illustrate distinct biological impact of EMT depending on the dynamics of the transition.
153 citations
TL;DR: Dll1cKO mice have a reduced number of MaSCs at different stages of mammary gland development in virgin and pregnant animals, and it is demonstrated that Dll1+ Ma SCs can both basal and luminal cells generate the important cellular components of the Mammary gland stem cell niche through inter-turning.
Abstract: The stem cell niche is a specialized environment that dictates stem cell function during development and homeostasis. We show that Dll1, a Notch pathway ligand, is enriched in mammary gland stem cells (MaSCs) and mediates critical interactions with stromal macrophages in the surrounding niche in mouse models. Conditional deletion of Dll1 reduced the number of MaSCs and impaired ductal morphogenesis in the mammary gland. Moreover, MaSC-expressed Dll1 activates Notch signaling in stromal macrophages, increasing their expression of Wnt family ligands such as Wnt3, Wnt10A, and Wnt16, thereby initiating a feedback loop that promotes the function of Dll1-expressing MaSCs. Together, these findings reveal functionally important cross-talk between MaSCs and their macrophageal niche through Dll1-mediated Notch signaling.
138 citations
TL;DR: This work identifies the common functions of different metastatic niches: anchorage, survival support, protection from external insults, licensing proliferation and outgrowth, and highlights the emerging role of the metastatic niche in maintaining cancer stemness and promoting immune evasion.
Abstract: Metastasis is an inefficient process, especially during colonization at a distant organ. This bottleneck underlies the importance of the metastatic niche for seeding and outgrowth of metastases. Here, we classify the common functions of different metastatic niches: anchorage, survival support, protection from external insults, licensing proliferation and outgrowth. We highlight the emerging role of the metastatic niche in maintaining cancer stemness and promoting immune evasion, and discuss therapeutic opportunities against the metastatic niche.
123 citations
TL;DR: Targeting the processes of dormancy and initial outgrowth offers the most therapeutic promise in the bone metastasis niche, from controlling tumor-cell survival to growth into clinically detectable disease.
Abstract: Bone metastasis, or the development of secondary tumors within the bone of cancer patients, is a debilitating and incurable disease. Despite its morbidity, the biology of bone metastasis represents one of the most complex and intriguing of all oncogenic processes. This complexity derives from the intricately organized bone microenvironment in which the various stages of hematopoiesis, osteogenesis, and osteolysis are jointly regulated but spatially restricted. Disseminated tumor cells (DTCs) from various common malignancies such as breast, prostate, lung, and kidney cancers or myeloma are uniquely primed to subvert these endogenous bone stromal elements to grow into pathological osteolytic or osteoblastic lesions. This colonization process can be separated into three key steps: seeding, dormancy, and outgrowth. Targeting the processes of dormancy and initial outgrowth offers the most therapeutic promise. Here, we discuss the concepts of the bone metastasis niche, from controlling tumor-cell survival to growth into clinically detectable disease.
114 citations
TL;DR: An overview of the essential components in TME and the remodeling of TME in response to anti-cancer treatments is provided and the strategies that aim to enhance therapeutic efficacy by modulating TME are summarized.
Abstract: Tumor microenvironment (TME) is comprised of cellular and non-cellular components that exist within and around the tumor mass. The TME is highly dynamic and its importance in different stages of cancer progression has been well recognized. A growing body of evidence suggests that TME also plays pivotal roles in cancer treatment responses. TME is significantly remodeled upon cancer therapies, and such change either enhances the responses or induces drug resistance. Given the importance of TME in tumor progression and therapy resistance, strategies that remodel TME to improve therapeutic responses are under developing. In this review, we provide an overview of the essential components in TME and the remodeling of TME in response to anti-cancer treatments. We also summarize the strategies that aim to enhance therapeutic efficacy by modulating TME.
28 citations
TL;DR: The tumor microenvironment contains heterogeneous populations of stromal cells with important roles in cancer progression and metastasis, and pSTAT3+ reactive astrocytes represent a promising target for the treatment of brain metastasis.
2 citations
Patent•
11 Oct 2018TL;DR: In this paper, a method of combination therapy for prevention or treatment of cancer bone metastasis comprising administering to a patient in need thereof a therapeutically effective amount of an anti-Jagged1 antibody or an antigen-binding fragment thereof and a chemotherapeutic agent is presented.
Abstract: Provided is a method of combination therapy for prevention or treatment of cancer bone metastasis comprising administering to a patient in need thereof a therapeutically effective amount of an anti-Jagged1 antibody or an antigen-binding fragment thereof and a chemotherapeutic agent The combination therapy achieves an excellent synergistic effect In preferred embodiments, the patient is a human female and the cancer is breast cancer