Integrative Hormone Health: A Clinical Journey Explained
Table of Contents
This educational post guides you through a comprehensive, first-person exploration of hormone therapy decisions, iron metabolism and ferritin interpretations, intrauterine device (IUD) pharmacology and thrombosis risk, thyroid optimization strategies, cortisol testing, fertility considerations in male patients on testosterone therapy, endometriosis management in menopause, and navigating hormone therapy after transient ischemic attack (TIA) or breast pathology. I share the latest findings from top researchers using up-to-date, evidence-based approaches and include chiropractic care by focusing on how the body systems work together—highlighting the balance of the nervous system, connections between hormones and the immune Drawing on my clinical observations and experience, I clarify misconceptions, explain physiological underpinnings, and offer pragmatic protocols, including nutrition, lifestyle, and carefully titrated pharmacology. You will find narrative explanations, step-by-step reasoning, and references to support clinical decision-making.
In practice, I frequently see confusion about iron status. Patients present with fatigue, hair shedding, decreased exercise tolerance, and cognitive fog. Many have normal hemoglobin yet low iron stores. When I evaluate iron, I do not rely on a single marker. I interpret serum ferritin, transferrin saturation, serum iron, total iron-binding capacity (TIBC), reticulocyte indices, and inflammatory markers.
Physiologically, iron fuels mitochondrial oxidative phosphorylation, supports thyroid peroxidase activity, and enables dopamine and norepinephrine synthesis. Low iron levels depress ATP production and thyroid signaling, which explains fatigue, cold intolerance, and impaired cognition. In athletes or menstruating individuals, I often find hidden contributors:
When ferritin is less than about 30 ng/mL, evidence suggests this is consistent with iron deficiency—even if hemoglobin is normal—and symptoms respond to replenishment. I tailor iron repletion:
I always ask why iron is low. For example, in postpartum patients and neonates, there are predictable periods of increased turnover and heightened risk of latent anemia. My approach includes nutritional counseling, GI evaluation, and precise dosing that avoids overshooting and oxidative stress.
citation: Iron deficiency without anemia: a clinical review (Camaschella, 2019).
Patients often ask me about hormonal IUDs and clot risk. It is essential to differentiate progestin families:
Mechanistically, estrogen in systemic combined contraceptives increases hepatic synthesis of clotting factors (II, VII, IX, X) and decreases antithrombin III levels, thereby elevating the risk of venous thromboembolism. A levonorgestrel IUD largely avoids this hepatic first-pass effect, providing local endometrial suppression without meaningfully increasing systemic thrombosis risk in most patients.
I emphasize individualized assessment:
citation: Levonorgestrel intrauterine system and risk of venous thromboembolism (ACOG, 2017).
As a chiropractor and nurse practitioner with functional medicine training, I integrate biomechanics, autonomic nervous system (ANS) regulation, and neuroendocrine-immune crosstalk into hormone care. Chronic pain and postural dysfunction elevate sympathetic tone, thereby increasing cortisol and catecholamine levels, which can blunt gonadotropin-releasing hormone (GnRH) pulsatility and reduce luteinizing hormone (LH)/follicle-stimulating hormone (FSH) output. This stress axis suppresses sex steroid production and impairs thyroid hormone conversion (T4 to T3) via modulation of deiodinases.
What I see clinically:
Chiropractic care fits into the broader plan by addressing the musculoskeletal drivers of neuroendocrine dysregulation, facilitating better responses to nutrition and pharmacotherapy. My clinical observations on these systems approaches are available across my educational media and case narratives:
citation: Autonomic nervous system and endocrine interactions (Tsigos & Chrousos, 2002).
Patients with progesterone sensitivity often report mood shifts, sleep disturbance, or irritability. I first clarify whether the compound is micronized progesterone (bioidentical) or a synthetic progestin; the former metabolizes to allopregnanolone, a neurosteroid that modulates GABA-A receptors, typically enhancing sleep and anxiolysis. Synthetic progestins may not share this profile and can provoke adverse mood effects.
Dosing rationale:
In patients with PCOS or androgen excess, I consider androgen balance, insulin resistance, and inflammatory signaling. Introducing progesterone must be matched with dietary anti-inflammatory strategies, insulin sensitizers (e.g., lifestyle, inositol), and attention to mood. When tolerance is poor, sublingual troches divided into quarters can fine-tune dosing to avoid peaks.
Physiologically, progesterone stabilizes endometrial tissue during estrogen exposure and may modulate mast cells and immune tone, which is relevant to cyclic mood/sleep syndromes. Patients commonly tolerate 100 mg nightly oral micronized progesterone; when not, I step down or use sublingual titration.
citation: Micronized progesterone: clinical pharmacology (Prior, 2018).
Cortisol secretion follows a diurnal rhythm with a sharp awakening response, a midday decline, and a nocturnal nadir. To understand a patient’s stress physiology, I use:
The reason is clear: a single AM sample can miss post-awakening peaks or late-day flattening that correlates with fatigue, sleep issues, and metabolic dysfunction. Saliva reflects free cortisol, aligning better with tissue exposure. I also integrate heart rate variability and sleep data to contextualize endocrine output in relation to behavior and recovery.
citation: Diurnal cortisol analysis and clinical implications (Adam et al., 2017).
Young men in their 20s or 30s with low testosterone frequently present with hypogonadal symptoms yet desire fertility. Exogenous testosterone suppresses LH and FSH, decreasing intratesticular testosterone and impairing spermatogenesis. In these cases, I consider clomiphene citrate for a short course (e.g., 3–6 months) to increase endogenous LH/FSH and raise testosterone while supporting sperm counts.
Key points:
At the same time, I prioritize lifestyle interventions:
Many younger patients respond effectively to integrative protocols, achieving improvements in testosterone from ~300 ng/dL to >700 ng/dL over 6–9 months, provided adherence to movement, diet, sleep, and stress management.
citation: Clomiphene in male hypogonadism and fertility (Katz et al., 2012).
Navigating hormone therapy in patients with a history of breast pathology demands precision and individualized care. I clarify terminology with patients:
Clinical reasoning:
I use shared decision-making and, when appropriate, a risk acknowledgment waiver that documents understanding of uncertainties and alternatives. We weigh cognitive health, metabolic risks (type 2 diabetes, hypertension), and bone integrity against theoretical oncologic risks, prioritizing the patient’s informed values.
citations:
I often see patients told that all hormones must be stopped after a TIA or with migraines. Neurology training historically emphasized estrogen as the sole relevant hormone, but modern evidence paints a more nuanced picture:
In practice:
citations:
Thyroid replacement can be challenging. I see patients on levothyroxine (T4) with persistent fatigue, weight issues, and cold intolerance. Here is my framework:
Physiology and protocol:
I titrate gradually, aim for symptom relief and functional markers (a proxy for resting metabolic rate, warmth, energy, bowel regularity), and avoid overshooting, which risks palpitations and bone loss.
citations:
Even post-hysterectomy or in menopause, endometriosis can persist via ectopic endometrial-like implants on pelvic structures. Estrogen therapy without progesterone in a patient with a history of endometriosis can theoretically stimulate these residual implants. I follow guidance consistent with gynecologic recommendations:
I often increase progesterone slightly in postmenopausal patients with prior endometriosis, ensuring symptom control and pelvic comfort while balancing cognition, mood, and sleep.
citation: Endometriosis management in menopause and hormone therapy (Gemici et al., 2014).
Patients ask about estriol, particularly in topical creams for skin health. Estriol is a weaker estrogen that preferentially binds to ER-beta and is often discussed for its theoretical protective effects. In clinical reality:
When I aim for symptom control (hot flashes, sleep), I prefer transdermal estradiol, and if cosmetic skin goals are prominent, estriol can be layered topically. I monitor bleeding and adjust dosing to avoid endometrial stimulation without adequate progesterone.
citations:
Men on testosterone replacement therapy (TRT) can develop elevated hematocrit due to androgen-driven erythropoiesis. My protocol:
Chiropractic care supports thoracic mechanics and diaphragmatic function, which can improve sleep-disordered breathing, reduce nocturnal hypoxia, and help stabilize hematocrit.
citation: Testosterone therapy and erythrocytosis (Coviello et al., 2008).
When thyroid labs look “acceptable” yet patients still feel unwell, I investigate the gut-thyroid axis:
citation: Gut microbiota and thyroid axis (Fröhlich & Wahl, 2019).
Here is how I systematically approach common scenarios:
In my practice, I see consistent patterns:
General Disclaimer, Licenses and Board Certifications *
Professional Scope of Practice *
The information herein on "Integrative Hormone Health: A Clinical Journey Explained" 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 on this site and on our family practice-based chiromed.com site, focusing on naturally restoring health for patients of all ages.
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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
(Board Certified: Family Practice Nurse Practitioner—Multistate)*
(Licensed Nurse Practitioner & Chiropractor - Multistate)*
Clinical Director
Digital Business Card
Dr. Maria Cardenas, MD
(Board Certified: Internal Medicine)
(Licensed Medical Doctor)
Medical Director, Clinical Director & Collaborative Physician
NPI # 1164426749
MD License #: J2933
Licenses and Board Certifications:
MD: Medical Doctor
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
(Board Certified: Family Practice Nurse Practitioner—Multistate)*
(Licensed Nurse Practitioner & Chiropractor - Multistate)*
Clinical Director
Digital Business Card
Dr. Maria Cardenas, MD
(Board Certified: Internal Medicine)*
(Licensed Medical Doctor)*
Medical Director, Clinical Director & Collaborative Physician
NPI # 1164426749
MD License #: J2933
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