"Scientists have created a new cowpox-style virus in a bid to cure cancer.

The treatment, called CF33, can kill every type of cancer in a petrie dish and has shrunk tumours in mice, The Daily Telegraph reported.

US cancer expert Professor Yuman Fong is engineering the treatment, which is being developed by Australia biotech company Imugene.

They are hoping the treatment will be tested on breast cancer patients, among other cancer sufferers, next year."

https://www.msn.com/en-nz/news/techandscience/breakthrough-as-scientists-create-a-new-cowpox-style-virus-that-can-kill-every-type-of-cancer/ar-BBWwhcp

'Smart needle' could speed up cancer detection 'with a less intrusive process'

Cancer detection could become much quicker and easier in the future after scientists developed a new "smart needle" that uses a mini laser to identify diseased tissue within seconds.

Researchers have demonstrated the technique works in the lab and have just begun a major three-year clinical trial to test it in living people.

They have focused on lymphoma so far but are hopeful the technique could also be used to diagnose other forms of the disease, such as breast and prostate cancer, further down the line.

https://inews.co.uk/news/science/smart-needle-cancer-detection-breast-cancer-prostate-cancer-process-explained-921561

No info in the article re. what chemicals exactly. --Rude! Well always good to use vinegar for cleaning! Cheap and pretty effective. Seems like if that is the case-- household detergents- chemicals that they would see a higher incidence of BC in people who clean for a living.

Researchers Halt Spread of Breast Cancer by Blocking Metastasis-Promoting Enzyme

In a breakthrough with important implications for the future of immunotherapy for breast cancer, UC San Francisco scientists have found that blocking the activity of a single enzyme can prevent a common type [luminol B] of breast cancer from spreading to distant organs.

The new study, published Nov. 14 in the journal Life Science Alliance, shows that these metastases can be stopped before they are able to lay the foundations for tumor growth. By administering an antibody that specifically targets and disrupts MMP9 activity, the scientists were able to prevent cancer from colonizing the lungs of mice. But interestingly, interfering with MMP9 had no effect on the primary tumor, which suggests that the enzyme's primary role in this scenario is helping existing malignancies metastasize and colonize other organs rather than promoting the growth of established primary tumors...

The researchers also discovered that interfering with MMP9 activity helped recruit and activate cancer-fighting immune cells to metastatic sites, a result with important implications for treating certain types of metastatic breast cancer with immunotherapy...

"These findings come at an exciting time in cancer immunology, with antibodies targeting MMP9 being actively explored for clinical use within the biotech industry," Plaks said. "There's been great interest in trying to use immunotherapy to treat metastatic breast cancers of the luminal B type, but so far, success has been limited. Our work indicates that a combination approach of immunotherapy with antibodies targeting MMP9 activity might actually succeed."

https://www.ucsf.edu/news/2019/11/415941/researchers-halt-spread-breast-cancer-blocking-metastasis-promoting-enzyme

Profound.

Environmental toxins. Reading "Anti Cancer Living " Cohen and Jeffries. In their chapter on "The Environment and Quest for Health" and "Appendix C, Environmental Toxin Hit List", the list is extensive and includes far more than just pesticides/herbicides. The book has an extensive bibliography. I used to read labels for added sugar, artificial ingredients. I need to become much more informed. Need to watch the soaps/shampoos, and other cleaners, toothpaste, Not ready to throw out all the yogurt containers I use for left overs and invest in glass containers.

For anyone who is interested in finding out about clinical trials in immunotherapy, go to the Cancer Research Institute -- website is https://www.cancerresearch.org

I went to one of their patient summits today up at Johns Hopkins, and it was a fabulous program. Lots of opportunities for information sharing, both with patients and practitioners. Very worthwhile program (they already have 2 set up for 2020 -- see their website).

Pivotal Data in HER2+ Breast Cancer Transform Paradigm

Erika P. Hamilton, MD, discusses several studies in the HER2-positive breast cancer space and sequencing challenges that have emerged.

Research Efforts in HER2+ Breast Cancer Focused on Optimizing Novel Agents

Gregory Vidal, MD, PhD, highights ways in which available and investigational agents are being evaluated across HER2-positive breast cancer settings.

Adjuvant T-DM1 Approaches EU Approval for HER2+ Early Breast Cancer

Will the phase III KATHERINE data lead to a European approval in the adjuvant setting?

Exciting Advances Continue in HER2+ Breast Cancer and Other Subtypes

Kurt W. Tauer, MD, FACP, discusses encouraging updates across the spectrum of breast cancer subtypes.

mysticalcity - thank you for the post to clinical trials. BC for the third time!!! When I contacted one research facility, they said they had no trials, did not know of any for my situatain, and would be prescribing the same treatment as my DR. They sounded bored with my history and treatment of BC. This site will help me do a little of my own "research" and maybe ask questions that I had not thought about.

2009 ER+ left breast. 52 yrs. Lumpectomy, Sentinel node removal, negative. Radiation 6 weeks, tamoxifen 5 years. Dense lumpy left breast, normal right. Acupuncture offered at facility as part of integrative medicine. It really helped with anxiety/stress during radiation treatment.

2016 ER+ left breast. Probably a new cancer, but unknown. 4 rounds TC Aug-Oct 2016, Bi-lateral (my choice) Nov 2016, no reconstruction. 2 sentinel nodes remove, negative. Cold Capping using Chemo Cold Caps (DIGNICAP not available). Anastrozole 1 mg starting May 2017. Joint issues noticed immediately. Stopped Anastrozole after 3-4 months due to joint stiffness in. After several months of no AIs, fingers were feeling better. Started tamoxifen March 2018

7/19/2019 - swelling in R-arm, opposite side from where lymph nodes removed. Noticed 6/18/2019. Could have been swelling earlier but wearing long sleeves. Trip to urgent care. They did ultrasound, concerned that there might be a clot, there was not. Started seeing lymphatic therapist 7/2/2019.

8/2019 CT, Breast/chest , neck/thyroid ultra sound

9/2019 DR ordered biopsy, said it could be lymphoma, cancer, benign lymphatic. Biopsy R-axilla. Cancer. Genetic test showed no known markers (20+ looked for)

9/29/2019 PET scan, no indication of spread. Arimidex and Ibrance prescribed to shrink tumor prior to surgery.

10/2019 – Stopped Tamoxifen. Started Arimidex and Ibrance. Brand name Arimidex so far does not seem to have the SEs that generics did, but stiff/trigger finger on left middle finger returned.

Lumpie, please translate!

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Diet-related metabolomic signature of long-term breast cancer risk using penalized regression: an exploratory study in the SU.VI.MAX cohort

Lucie Lécuyer, Céline Dalle, Sophie Lefevre-Arbogast, Pierre Micheau, Bernard Lyan, Adrien Rossary, Aicha Demidem, Mélanie Petera, Marie Lagree, Delphine Centeno, Pilar Galan, Serge Hercberg, Cécilia Samieri, Nada Assi, Pietro Ferrari, Vivian Viallon, Mélanie Deschasaux, Valentin Partula, Bernard Srour, Paule Latino-Martel, Emmanuelle Kesse-Guyot, Nathalie Druesne-Pecollo, Marie-Paule Vasson, Stéphanie Durand, Estelle Pujos-Guillot, Claudine Manach and Mathilde Touvier

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DOI: 10.1158/1055-9965.EPI-19-0900

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Abstract

Background:Diet has been recognized as a modifiable risk factor for breast cancer. Highlighting predictive diet-related biomarkers would be of great public health relevance to identify at-risk subjects. The aim of this exploratory study was to select diet-related metabolites discriminating women at higher risk of breast cancer using untargeted metabolomics. Methods:Baseline plasma samples of 200 incident breast cancer cases and matched controls, from a nested case-control study within the SU.VI.MAX cohort, were analysed by untargeted LC-MS. Diet-related metabolites were identified by partial correlation with dietary exposures, and best predictors of breast cancer risk were then selected by Elastic Net penalized regression. The selection stability was assessed using bootstrap resampling. Results:595 ions were selected as candidate diet-related metabolites. 14 of them were selected by Elastic Net regression as breast cancer risk discriminant ions. A lower level of piperine (a compound from pepper) and higher levels of AcetylTributylCitrate (an alternative plasticizer to phthalates), pregnene-triol sulfate (a steroid sulfate) and 2-amino-4-cyano butanoic acid (a metabolite linked to microbiota metabolism) were observed in plasma from women who subsequently developed breast cancer. This metabolomic signature was related to several dietary exposures such as a "Western" dietary pattern and higher alcohol and coffee intakes. Conclusions:Our study suggested a diet-related plasma metabolic signature involving exogenous, steroid metabolites and microbiota-related compounds associated with long-term breast cancer risk that should be confirmed in large-scale independent studies. Impact:These results could help to identify healthy women at higher risk of breast cancer and improve the understanding of nutrition and health relationship.

• Received July 29, 2019.
• Revision received October 3, 2019.
• Accepted November 18, 2019.

• Copyright ©2019, American Association for Cancer Research.

ugh I don't like the vague *high amounts* on that. will look forward to more studies.