Breast cancer may affect as many as 1 in 8 women. It’s important for patients and providers to understand the role that estrogen detoxification plays in breast cancer so that they can make more informed mitigation and treatment decisions.
WHAT IS BREAST CANCER?
Cancer occurs when cells begin to grow uncontrollably. Cells normally follow a controlled process by which they are created and destroyed. The immune system manages this process and helps identify any abnormal changes that may occur within the cell. Breast cancer appears when the immune system is not able to regulate abnormalities in the breast cells.
TYPES OF BREAST CANCER
There are many different types of breast cancers. A breast cancer’s type is based on which cells in the breast excessively proliferate and become cancerous. Some breast cancers have hormone receptors, such as estrogen receptor positive (ER+) and progesterone receptor positive (PR+) breast cancers, and some express a protein called HER2 (i.e., HER2+ cancers). There are also breast cancers that do not have hormone receptors or HER2 proteins (e.g., triple negative breast cancers). Some factors that increase risk for breast cancer include family history, older age, and environmental factors.
CAN ESTROGEN DETOXIFICATION INFLUENCE BREAST CANCER RISK?
The way the body detoxifies estrogens may play a role in breast cancer. After the body manufactures estrogens, such as estrone (E1), estradiol (E2), and estriol (E3), they must be processed and metabolized through the liver.
PHASE I ESTROGEN METABOLISM
Phase I estrogen metabolites (including 2-OH-E1, 2-OH-E2, 4-OH-E1, 4-OH-E2, and 16-OH-E1) have oxidative potential; however, some are more damaging than others. It is preferred that most estrogen is metabolized into the 2-OH metabolites, as these are the most stable estrogen metabolites in Phase I that cause the least amount of harm to the body. For example, the 2-OH metabolites cause less DNA damage than the 4-OH metabolites, and their bond with the estrogen receptor is the weakest so they are removed from estrogen receptors most efficiently.
The 16-OH metabolite may have an increased capacity for proliferation as it is a more potent estrogenic metabolite. It binds more tightly to estrogen receptors than the 2-OH metabolites and can cause tissue proliferation in breast tissue (e.g., fibrocystic breasts), endometrial tissue (e.g., heavy bleeding), or ovarian tissue (e.g., ovarian cysts). Conversely, it can have benefits in bone tissue leading to improved bone mineral density.
The most concerning estrogen metabolite is the 4-OH-E1 metabolite. The body must make some of these metabolites, so it is expected that at least some 4-OH metabolites will be present in the body. Some research suggests that the 4-OH-E2 metabolite may not have the same carcinogenic effects of 4-OH-E1. However, it’s currently recommended that the number of 4-OH metabolites should be minimized.
We also see that the enzyme that drives the 4-OH pathway, when upregulated, creates an increased production of this 4-OH metabolite. The enzyme responsible for this conversion is the CYP1B1 enzyme. The CYP enyzmes are found in Phase I of liver metabolism. CYP1B1 can be upregulated with inflammation, smoking, and exposure to PAH (polyaromatic hydrocarbons). Our main exposure to PAHs is in cosmetics including shampoos, conditioners, lotions, make-up, and ingredients that are tar or oil-based. We can also be exposed to PAHs through smoked and charbroiled foods depending on the fuel used for cooking/prep. PAHs may also be in the air/environment depending on your location.
The 4-OH metabolites have the strongest bond to the estrogen receptor; therefore, the body must work extremely hard to break this bond. It takes a lot more energy to break off the 4-OH metabolites for detoxification than the other metabolites. The 4-OH-E1 metabolite also has the potential to become a reactive quinone that causes DNA damage. Research has evidenced that quinone production from the 4-OH metabolite may create damaging quinones or DNA adducts. These adducts are found in the breast tissue of women that have breast cancer. Thus, if the body is not able to neutralize the 4-OH metabolites well or efficiently, they can wreak havoc on DNA, further contributing to adduct formation in breast cells.
When DNA is damaged, it disrupts cellular signaling and the body’s ability to repair itself and stop abnormal cell growth. There is a correlation between increased 4-OH-E1 metabolites and breast cancer risk. Miao, et al state: “Among many alterations of sex hormone metabolisms, 4-hydroxy estrogen (4-OH-E) metabolite was found to be significantly increased in the urine samples of patients with breast cancer compared with the normal healthy controls. This was the most important risk factor for breast cancer”.
PHASE II METABOLISM: ESTROGEN METHYLATION
After estrogens are processed through Phase I, some of them are methylated in Phase II. The process of methylation takes dangerous, oxidative Phase I metabolites and neutralizes them into stable, water-soluble metabolites that are ready for excretion.
Even if a person is metabolizing most of their estrogen into the preferred 2-OH metabolites, if these 2-OH metabolites are not adequately methylated, they can still be oxidizing. Oxidation can lead to cellular stress, poor cellular health, and an increased risk for abnormal cell function.
Methylation is dependent on catechol-o-methyltransferase (COMT) enzyme function. COMT relies on sufficient cofactors such as S-adenosyl-L-methionine (SAM), vitamin B6, and magnesium to function optimally. If COMT activity is slow, then the body may not be able to appropriately methylate estrogens through this final step of detoxification in the liver. With poor methylation we are unable to clear our estrogens through Phase II and the body will continue to recirculate these estrogens creating increased exposure and burden of estrogens in the body.
PHASE III METABOLISM: HEALTHY BOWEL CLEARANCE
Phase III of estrogen metabolism is required for the continued detoxification of estrogens. Phase II metabolites in the liver migrate to Phase III detoxification in the intestines. Phase III ends in the stool. Without productive stools and digestive regularity, estrogens can stay trapped in the body. These estrogens can be reabsorbed and recirculate, increasing the amount of estrogen to be detoxified.
When the body is overloaded with toxins, or unable to efficiently metabolize toxins, the burden of estrogen may start to create issues. Repeated exposure to the 4-OH metabolites (by poor Phase III clearance) increases the opportunity for DNA damage.
EVALUATING ESTROGEN DETOXIFICATION
Estrogen detoxification is an important component of metabolism. It is standard practice for the body to take compounds (hormones, foods, toxins), and process them—which usually means breaking them down into something “bad” in Phase I before turning them into something “good” or neutral in Phase II, and finally eliminating them in Phase III.
Additionally, supporting enzyme pathways for efficient detoxification can influence the success of estrogen metabolism. Lifestyle and supplements may strongly influence the different pathways for estrogen detoxification. We see cruciferous vegetables (broccoli, cauliflower, Brussel Sprouts) and vegetables from the apiaceae family (carrots, parsnips) support a preference for the 2-OH pathway in phase I. We also see that Rosemary, DIM, sulforophane, and isoflavones (like soy beans) also support an increased utilization of the 2-OH pathway (CYP1A1) over the 4-OH and 16-OH pathways.
It is noted that inflammation, obesity, high sugar diet, and oxidative exposure (smoking, variable consumption of alcohol) can push more activity down the 4-OH and 16-OH pathways, and reduce the activity down the 2-OH pathway.
These processes happen all the time, every day, in the body. It’s important to ensure the body has the capacity to clear toxins efficiently and without problems. Dried urine hormone testing can evaluate the different components in the process of estrogen detoxification and may be a helpful tool in understanding how these processes are working and guiding intervention choices.
Dr. Debbie Rice, ND, MPH
Director of Clinical Education
Precision Analytical Inc, creators of the DUTCH Test
Dr. Rice is the Director of Clinical Education for Precision Analytical and practices part-time as a naturopathic doctor where she focuses care on pediatric health, hormone health, thyroid health, and adrenal health. She has had experience working with communities in need, both in the United States and internationally. Her training has been primarily in women’s health, pediatric care, hormone therapy and hormone function, as well as complimentary adjunct care. Dr. Rice uses diet and lifestyle, botanical medicine, and conventional approaches to maximize care for her patients.
About Precision Analytical:
Precision Analytical created the DUTCH Test (dried urine test for comprehensive hormones) to help providers profoundly change their patients’ lives with insight into a patient’s sex and adrenal hormone health. The DUTCH Test uses convenient at-home collection to provide the most comprehensive report with accurate and research-validated results.
Where on the dutch test does it indicate if your metabolizing these hormones and on what pathways?
Hello Kesti, on this sample report it’s on pages 2 and 3 for the estrogen metabolism pathways. https://dutchtest.com/wp-content/uploads/2022/06/Sample-Report_DUTCH-Complete_Female_RevB1-062022.pdf
Excellent review!
Thank you Dr Rice