Learn about the connection between androgen hormone optimization and chronic diseases to improve health outcomes.
Table of Contents
Welcome to our educational series on achieving optimal health. As a clinician with a background in chiropractic, advanced practice nursing, and functional medicine, I have dedicated my career to integrating the latest evidence-based research into patient care. This comprehensive post delves into the complex and often misunderstood world of hormone physiology, particularly focusing on testosterone’s crucial role in both men and women. We will synthesize findings from leading experts like Dr. Abraham Morgentaler and Dr. Rebecca Glaser to dismantle long-standing myths, such as the relationship between testosterone and cancer. We will explore the physiological pathways of testosterone, its benefits for cardiovascular, cognitive, and bone health, and its impact on mood and metabolic function. Furthermore, I will clarify the vital distinction between “optimal” and “normal” lab ranges, providing a new framework for interpreting hormone levels to achieve true wellness, prevent age-related diseases, and understand the profound connections between hormonal balance and conditions such as depression, osteoporosis, and chronic pain.
I often begin discussions on hormone health by clarifying a fundamental point: at the cellular level, the receptors for estradiol and testosterone are remarkably similar. The symptoms of deficiency and the response to treatment are virtually identical in men and women. Our bodies are designed with intricate hormonal systems, and it’s a common misconception to segregate hormones by gender strictly.
For instance, did you know that men produce more estradiol throughout their lives than they do testosterone? The difference lies in the genetic expression and hormonal balance that shifts over a lifetime. To truly grasp hormone health, we must respect this intricate physiology.
Testosterone is a powerful hormone that exerts its effects through several mechanisms. Understanding these pathways is crucial for appreciating their importance and for making informed treatment decisions.
It’s important to highlight the role of DHT. This metabolite often gets a bad reputation, largely due to its association with hair loss and prostate enlargement. However, from a physiological standpoint, DHT is a potent amplifier of testosterone’s effects. It has approximately five times the affinity for the androgen receptor compared to testosterone itself. Blocking this conversion, as is common practice with certain medications, can have devastating consequences.
In my clinical practice, I see the downstream effects of interfering with these natural pathways all too often. I’ve had 35-year-old men come into my office in tears. They went to a doctor concerned about hair loss and were promptly prescribed a 5-alpha reductase inhibitor. Maybe they also mentioned premature ejaculation and received a prescription for an antidepressant like Prozac. Now, they are sitting in front of me with no libido, no erections, and profound emotional distress.
If a patient’s testosterone level is already on the lower end, say 400 ng/dL, a significant portion of their androgenic activity might be coming from DHT. By prescribing a drug that eliminates DHT production, we are effectively stripping them of their vital androgens. We must respect the physiology. Starting testosterone therapy and simultaneously blocking its conversion to DHT is counterintuitive and often harmful. Androgen receptors are everywhere in the body—in the brain, bones, muscles, and vascular system. They are meant to be stimulated.
Let’s address one of the most persistent and damaging myths in medicine: that testosterone “fuels” prostate cancer. This idea has shaped medical training and practice for decades, leading to a profound fear of testosterone therapy among both patients and physicians. The credit for dismantling this myth largely goes to Dr. Abraham Morgentaler, the former chairman of urology at Harvard. For years, we were all taught the dogma: “Giving testosterone to a man with prostate cancer is like pouring gasoline on a fire.”
As part of his Ph.D. thesis, Dr. Morgentaler traced the origin of this quote. He found it in a research paper from the 1940s. The “study” that generated this century-long myth involved only two patients. That was the entire basis for this pervasive medical belief. Dr. Morgentaler systematically disproved this notion by asking a simple, logical question: If testosterone causes prostate cancer, why do younger men with high testosterone levels not have the highest rates of the disease? And why do older men with low testosterone have the highest incidence?
His research demonstrated the exact opposite of the old myth:
Another common concern I hear in my clinic is from men with benign prostatic hyperplasia (BPH) or elevated prostate-specific antigen (PSA) levels who believe they cannot take testosterone. This is where Dr. Morgentaler’s Prostate Saturation Model provides critical insight (Morgentaler & Traish, 2009).
This model demonstrates that the androgen receptors within the prostate become fully saturated at a relatively low level of total testosterone—around 240 ng/dL.
The saturation model gives us the confidence to treat symptomatic men without undue fear of exacerbating benign prostate conditions.
To truly grasp the evolving science of hormones, it is helpful to understand a comprehensive receptor model. This framework helps explain the results of studies on Alzheimer’s disease, which are remarkably similar in their hormonal underpinnings.
At the heart of this model is a protein called BCL-2. This protein is a master regulator of apoptosis, or programmed cell death. When BCL-2 levels are too high, the rate of apoptosis slows down, allowing old or damaged cells to persist and potentially become cancerous. Different hormones influence BCL-2 levels:
The idea of using testosterone to address chronic diseases may sound radical, but the historical and clinical evidence is compelling. One of the leading voices in this area is Dr. Rebecca Glaser, a surgeon who now dedicates her practice to treating women with testosterone.
The conversation about hormone optimization must include the brain. Androgen receptors are abundant in neural tissues. Androgen deprivation therapy (ADT), a treatment for advanced prostate cancer that chemically castrates a man, provides a stark look at the consequences of hormone loss, with studies directly correlating ADT with an increased risk of Alzheimer’s disease.
Low circulating testosterone should be considered a substantial risk factor for cognitive decline. Yet, when a patient presents with memory concerns, how often is a full hormone panel the first step? It should be. A large-scale study involving over 160,000 men provided staggering evidence (Yeap et al., 2018):
This finding prompts a crucial discussion about how we interpret lab results.
Medical training conditions us to think in terms of a “normal range.” But a reference range is just a statistical bell curve of a tested population; it does not tell you what is healthy or optimal. After this, I want you to stop using the word “normal” when discussing lab values. There is only optimal, not non-optimal.
Let’s apply this to the dementia study. The lab range for testosterone might be 300 to 1,100 ng/dL. A man with a level of 350 is in the 10th percentile. The man with a level of 900 is in the 90th percentile. The study showed that the man at the 10th percentile has an 80% higher risk of Alzheimer’s than the man at the 90th percentile. Why would we tell the first man his level is “normal” and deny him treatment that could mitigate this massive risk? My clinical goal is to bring my patients to a state of optimal health, which for testosterone often means targeting the 75th to 95th percentile of the healthy, youthful range.
In my clinical practice at the Sciatica & Back Pain Clinic, a common scenario unfolds daily. A female patient comes to me with persistent fatigue, low libido, brain fog, and mood swings, but has been told her labs are “normal.” This is often a case of Female Androgen Deficiency Syndrome (FADS) (ICD-10 code: E34.8).
A classic triad of symptoms defines FADS:
The issue often lies with Sex Hormone-Binding Globulin (SHBG), a protein that binds testosterone, making it inactive. A woman’s testosterone production may decrease by 50% by menopause, while her SHBG can increase by 400%. Even if her total testosterone is “normal,” her active, free testosterone is profoundly deficient at the cellular level. Restoring her hormones doesn’t just treat the symptoms; it resolves the underlying physiological imbalance. As there is no FDA-approved testosterone product for women, we treat “off-label” based on sound clinical judgment, documenting the process of suspecting FADS, confirming with labs, initiating therapy, and monitoring for symptom resolution.
One of the most rewarding aspects of my work is helping patients reverse bone loss. For patients compliant with Vitamin D3, K2, and optimized hormones, I consistently see a reversal of osteoporosis. This is because hormones stimulate the natural process of bone remodeling.
A study showed that women using testosterone pellets achieved an 8.3% increase in bone density per year (Stone, 2013). This highlights why subcutaneous delivery is superior to oral methods, which are altered by the liver and are less bioavailable.
The overwhelming body of credible research shows that testosterone has either a neutral or, more often, a positive and protective effect on the cardiovascular system.
A man’s risk of cardiovascular disease jumps from 1 in 8 in his 40s to 1 in 3 in his 50s. What else plummets during that time? His testosterone levels. The correlation is clear.
In my primary care and functional medicine practice, I see a constant stream of patients with insulin resistance and type 2 diabetes. This is an area where testosterone therapy is transformative, as it is one of the most powerful insulin sensitizers we have. Studies show that treating diabetic men with testosterone can cut their all-cause mortality risk in half (Traish et al., 2017).
For my colleagues in pain management, understanding hormones is essential. The connection between hormone levels and pain is well-documented. A key concept is Opioid-Induced Androgen Deficiency (OPIAD).
Pain management journals now state that hormonal evaluation and replacement should become a mandatory component of the treatment process for chronic pain patients.
Dr. Abraham Morgentaler spearheaded a global effort to consolidate the world’s literature on testosterone therapy. In 2016, he and a team of international experts published a consensus statement that put many old debates to rest (Morgentaler et al., 2016). Its conclusions are clear and profound:
These resolutions provide the highest level of evidence to guide our clinical practice. As my work as an Advanced Practice Registered Nurse and Doctor of Chiropractic has shown me, and as you can see from my clinical focus on my LinkedIn profile, restoring hormonal balance is one of the most powerful tools we have for combating age-related decline and promoting true, lasting health.
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Professional Scope of Practice *
The information herein on "An Overview for Chronic Diseases Using Androgen Hormone Optimization" is not intended to replace a one-on-one relationship with a qualified health care professional or licensed physician and is not medical advice. We encourage you to make healthcare decisions based on your research and partnership with a qualified healthcare professional.
Blog Information & Scope Discussions
Welcome to El Paso's Premier Wellness and Injury Care Clinic & Wellness Blog, where Dr. Alex Jimenez, DC, FNP-C, a Multi-State board-certified Family Practice Nurse Practitioner (FNP-BC) and Chiropractor (DC), presents insights on how our multidisciplinary team is dedicated to holistic healing and personalized care. Our practice aligns with evidence-based treatment protocols inspired by integrative medicine principles, similar to those found on this site and our family practice-based chiromed.com site, focusing on restoring health naturally for patients of all ages.
Our areas of multidisciplinary practice include Wellness & Nutrition, Chronic Pain, Personal Injury, Auto Accident Care, Work Injuries, Back Injury, Low Back Pain, Neck Pain, Migraine Headaches, Sports Injuries, Severe Sciatica, Scoliosis, Complex Herniated Discs, Fibromyalgia, Chronic Pain, Complex Injuries, Stress Management, Functional Medicine Treatments, and in-scope care protocols.
Our information scope is multidisciplinary, focusing on musculoskeletal and physical medicine, wellness, contributing etiological viscerosomatic disturbances within clinical presentations, associated somato-visceral reflex clinical dynamics, subluxation complexes, sensitive health issues, and functional medicine articles, topics, and discussions.
We provide and present clinical collaboration with specialists from various disciplines. Each specialist is governed by their professional scope of practice and their jurisdiction of licensure. We use functional health & wellness protocols to treat and support care for musculoskeletal injuries or disorders.
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We understand that we cover matters that require an additional explanation of how they may assist in a particular care plan or treatment protocol; therefore, to discuss the subject matter above further, please feel free to ask Dr. Alex Jimenez, DC, APRN, FNP-BC, or contact us at 915-850-0900.
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Dr. Alex Jimenez DC, MSACP, APRN, FNP-BC*, CCST, IFMCP, CFMP, ATN
email: coach@elpasofunctionalmedicine.com
Multidisciplinary Licensing & Board Certifications:
Licensed as a Doctor of Chiropractic (DC) in Texas & New Mexico*
Texas DC License #: TX5807, Verified: TX5807
New Mexico DC License #: NM-DC2182, Verified: NM-DC2182
Multi-State Advanced Practice Registered Nurse (APRN*) in Texas & Multi-States
Multi-state Compact APRN License by Endorsement (42 States)
Texas APRN License #: 1191402, Verified: 1191402 *
Florida APRN License #: 11043890, Verified: APRN11043890 *
Colorado License #: C-APN.0105610-C-NP, Verified: C-APN.0105610-C-NP
New York License #: N25929, Verified N25929
License Verification Link: Nursys License Verifier
* Prescriptive Authority Authorized
ANCC FNP-BC: Board Certified Nurse Practitioner*
Compact Status: Multi-State License: Authorized to Practice in 40 States*
Graduate with Honors: ICHS: MSN-FNP (Family Nurse Practitioner Program)
Degree Granted. Master's in Family Practice MSN Diploma (Cum Laude)
Dr. Alex Jimenez, DC, APRN, FNP-BC*, CFMP, IFMCP, ATN, CCST
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Licenses and Board Certifications:
DC: Doctor of Chiropractic
APRNP: Advanced Practice Registered Nurse
FNP-BC: Family Practice Specialization (Multi-State Board Certified)
RN: Registered Nurse (Multi-State Compact License)
CFMP: Certified Functional Medicine Provider
MSN-FNP: Master of Science in Family Practice Medicine
MSACP: Master of Science in Advanced Clinical Practice
IFMCP: Institute of Functional Medicine
CCST: Certified Chiropractic Spinal Trauma
ATN: Advanced Translational Neutrogenomics
Memberships & Associations:
TCA: Texas Chiropractic Association: Member ID: 104311
AANP: American Association of Nurse Practitioners: Member ID: 2198960
ANA: American Nurse Association: Member ID: 06458222 (District TX01)
TNA: Texas Nurse Association: Member ID: 06458222
NPI: 1205907805
| Primary Taxonomy | Selected Taxonomy | State | License Number |
|---|---|---|---|
| No | 111N00000X - Chiropractor | NM | DC2182 |
| Yes | 111N00000X - Chiropractor | TX | DC5807 |
| Yes | 363LF0000X - Nurse Practitioner - Family | TX | 1191402 |
| Yes | 363LF0000X - Nurse Practitioner - Family | FL | 11043890 |
| Yes | 363LF0000X - Nurse Practitioner - Family | CO | C-APN.0105610-C-NP |
| Yes | 363LF0000X - Nurse Practitioner - Family | NY | N25929 |
Dr. Alex Jimenez, DC, APRN, FNP-BC*, CFMP, IFMCP, ATN, CCST
My Digital Business Card
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