Breaking through to the Other Side: Microenvironment Contributions to DCIS Initiation and Progression

Nelson, Andrew C.; Machado, Heather L.; Schwertfeger, Kathryn L.

doi:10.1007/s10911-018-9409-z

Cited by 41 publications

(38 citation statements)

References 97 publications

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“…There are currently no known functional determinants of DCIS progression to an invasive lesion; in fact, DCIS and IDC lesions are very similar transcriptionally and epigenetically . This study profiles global lncRNA expression in a unique patient‐based model of breast cancer progression wherein early DCIS lesions are directly contiguous with an IDC lesion.…”

Section: Discussionmentioning

confidence: 99%

Long noncoding RNA BHLHE40‐AS1 promotes early breast cancer progression through modulating IL‐6/STAT3 signaling

DeVaux

Ropri

Grimm

et al. 2020

J of Cellular Biochemistry

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Ductal carcinoma in situ (DCIS) is a nonobligate precursor to invasive breast cancer. Only a small percentage of DCIS cases are predicted to progress; however, there is no method to determine which DCIS lesions will remain innocuous from those that will become invasive disease. Therefore, DCIS is treated aggressively creating a current state of overdiagnosis and overtreatment. There is a critical need to identify functional determinants of progression of DCIS to invasive ductal carcinoma (IDC). Interrogating biopsies from five patients with contiguous DCIS and IDC lesions, we have shown that expression of the long noncoding RNA BHLHE40-AS1 increases with disease progression.BHLHE40-AS1 expression supports DCIS cell proliferation, motility, and invasive potential. Mechanistically, BHLHE40-AS1 modulates interleukin (IL)-6/signal transducer and activator of transcription 3 (STAT3) activity and a proinflammatory cytokine signature, in part through interaction with interleukin enhancer-binding factor 3. These data suggest that BHLHE40-AS1 supports early breast cancer progression by engaging STAT3 signaling, creating an immune-permissive microenvironment.

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Section: Discussionmentioning

confidence: 99%

Long noncoding RNA BHLHE40‐AS1 promotes early breast cancer progression through modulating IL‐6/STAT3 signaling

DeVaux

Ropri

Grimm

et al. 2020

J of Cellular Biochemistry

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“…In light of the SMT's failure to explain carcinogenesis and deliver promised therapeutic successes, a third group of cancer theories has been introduced that combines a cell-based theory with elements of the tissue-based theory to explain the initial steps of carcinogenesis [36,37]. In essence, this latter group of theories retain the core of the SMT while adding the microenvironment in the form of the multiple cell types that surround the single initiating "cancer cell" [64][65][66][67][68]. They claim that either the cancer cell and its descendants "recruit" the cells in their microenvironment to "prosper" or that perturbations in the stroma induce DNA mutations and translocations in the parenchymal cells [69][70][71].…”

Section: Evaluating Theories Of Carcinogenesismentioning

confidence: 99%

Over a century of cancer research: Inconvenient truths and promising leads

Sonnenschein

Soto

2020

PLoS Biol

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Despite over a century of intensive efforts, the great gains promised by the War on Cancer nearly 50 years ago have not materialized. Since 1999, we have analyzed the lack of progress in explaining and "curing" cancer by examining the merits of the premises that determine how cancer is understood and treated. Our ongoing critical analyses have aimed at clarifying the sources of misunderstandings at the root of the cancer puzzle while providing a plausible and comprehensive biomedical perspective as well as a new theory of carcinogenesis that is compatible with evolutionary theory. In this essay, we explain how this new theory, the tissue organization field theory (TOFT), can help chart a path to progress for cancer researchers by explaining features of cancer that remain unexplainable from the perspective of the still hegemonic somatic mutation theory (SMT) and its variants. Of equal significance, the premises underlying the TOFT offer new perspectives on basic biological phenomena.

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“…The MIND model is based on the injection of human breast DCIS cells such as the MCF10DCIS.com cell line into the mouse mammary duct (Figure 4A) [35–37]. Compared to the other breast cancer xenograft models such as mammary fat pad injection, the MIND model has been shown to better recapitulate the mammary gland microenvironment [36], a key regulator of breast cancer progression [31, 38], and is therefore a more clinically relevant model for this disease. In our experiments, MCF10DCIS.com-Luc cells were injected intraductally into the mammary glands of mice where they form tumours that faithfully model the process of DCIS progression over the course of 10 weeks (Figure 4B-D) [35].…”

Section: Resultsmentioning

confidence: 99%

A mouse SWATH-MS reference spectral library enables deconvolution of species-specific proteomic alterations in human tumour xenografts

Krásný

Bland

Burns

et al. 2020

Preprint

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2 SWATH-mass spectrometry (MS) enables accurate and reproducible proteomic profiling in 3 multiple model organisms including the mouse. Here we present a comprehensive mouse 4 reference spectral library (MouseRefSWATH) that permits quantification of up to 10,597 5 proteins (62.2% of the mouse proteome) by SWATH-MS. We exploit MouseRefSWATH to 6 develop an analytical pipeline for species-specific deconvolution of proteomic alterations in 7 human tumour xenografts (XenoSWATH). This method overcomes the challenge of high 8 sequence similarity between mouse and human proteins, facilitating the study of host 9 microenvironment-tumour interactions from 'bulk tumour' measurements. We apply the 10 XenoSWATH pipeline to characterise an intraductal xenograft model of breast ductal 11 carcinoma in-situ and uncover complex regulation of cell migration pathways that are not 12 restricted to tumour cells but also operate in the mouse stroma upon progression to invasive 13 disease. MouseRefSWATH and XenoSWATH opens new opportunities for in-depth and 14 reproducible proteomic assessment to address wide-ranging biological questions involving 15 this important model organism. 16 17 18 19Key to the success of SWATH-MS is the use of retention-time calibrated spectral libraries to 20 identify and quantify peptides from the complex fragment ion mass spectra encoded within 21 digital proteome maps [13]. While most published SWATH-MS studies have utilised study-22

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Breaking through to the Other Side: Microenvironment Contributions to DCIS Initiation and Progression

Cited by 41 publications

References 97 publications

Long noncoding RNA BHLHE40‐AS1 promotes early breast cancer progression through modulating IL‐6/STAT3 signaling

Long noncoding RNA BHLHE40‐AS1 promotes early breast cancer progression through modulating IL‐6/STAT3 signaling

Over a century of cancer research: Inconvenient truths and promising leads

A mouse SWATH-MS reference spectral library enables deconvolution of species-specific proteomic alterations in human tumour xenografts

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