Women’s Health Benefits Overview for integrative Hormones
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Abstract
As a clinician working at the intersection of chiropractic care, advanced practice nursing, and functional medicine, I have witnessed how the mouth mirrors systemic health across a woman’s lifespan. In this educational post, I explore the intricate, evidence-based links between oral health and chronic disease, focusing on the oral microbiome, hormonal fluctuations, and the oral-gut axis. I explain how conditions such as gingivitis, periodontitis, xerostomia, and burning mouth syndrome arise from shifting endocrine and immune landscapes, and why these oral phenomena often reflect underlying systemic issues, including diabetes, cardiovascular disease, pulmonary disease, and even neurodegenerative conditions. I also detail our integrative model at Injury Medical Clinic PA in El Paso, Texas, where I collaborate with Dr. Maria Guadalupe Cardenas, MD, a board-certified internist and our Medical Director and Collaborative Physician, to blend chiropractic care, internal medicine oversight, functional medicine, rehabilitation, and personal injury care into precise, research-informed treatment plans. Throughout, I present insights from leading researchers, using modern, evidence-based methods, and share clinical observations from my practice and research, documented on WellnessDoctorRx.com and LinkedIn.
Our Integrative Team: Medical Oversight and Chiropractic Care Working As One
I am Dr. Alexander Jimenez, DC, APRN, FNP-BC, CFMP, IFMCP, ATN, CCST. At Injury Medical Clinic PA (also known as Mission Plaza Injury Medical Clinic) in El Paso, Texas, our patients receive care within a multidisciplinary setup common in integrative and injury care clinics: an MD provides medical direction alongside a chiropractor.
Chiropractic and Functional Medicine Integration: I provide chiropractic care, advanced practice nursing, and functional medicine protocols, bridging musculoskeletal alignment with metabolic, endocrine, and microbiome optimization.
Comprehensive Services:
Chiropractic care and spinal manipulation
Internal medicine consultation and oversight
Functional medicine testing and protocols
Personal injury care and trauma rehabilitation
Nutritional counseling with microbiome-focused strategies
Rehabilitation and movement therapy
Care coordination with dentistry for oral-systemic issues
This model enables us to address root causes across systems, recognizing the mouth as a gateway—and a barometer—of overall health.
Unifying the Mouth and Body: Why Oral Health Is Systemic Health
For years, my clinical lens centered on the musculoskeletal and nervous systems. Working with patients managing diabetes and cardiometabolic conditions profoundly expanded that lens: I saw the indisputable link between oral inflammation and systemic disease. You cannot disconnect the mouth from the rest of the body.
Key insight:Oral dysbiosis—an imbalance in the mouth’s microbial ecology—doesn’t remain local. It drives systemic inflammation, modulates immune responses, and interacts with hormonal rhythms, often accelerating the progression of chronic disease (Hujoel et al., 2018).
Clinical impact: We consider oral status a vital sign and screen for gingival inflammation, biofilm accumulation, xerostomia, and enamel erosion during wellness evaluations. This approach is particularly crucial in women’s health, where hormonal changes dramatically shape the oral environment.
The Oral Microbiome: Dynamic Communities, Host Immunity, and Disease Risk
The oral microbiome harbors over 700 identifiable species and functions as a dynamic community that orchestrates local defense and systemic signaling (Lamont et al., 2018). In balance, gram-positive flora help stabilize pH and deter pathogens; in dysbiosis, organisms such as Streptococcus mutans and S. sobrinus acidify the environment, demineralize enamel, and inflame gingival tissue.
Cariogenic bacteria:
Streptococcus mutans thrives in plaque biofilm, metabolizing sugars into acids that demineralize enamel.
Streptococcus sobrinus often predominates under high-glucose conditions, increasing the risk of decay in poorly controlled diabetes.
Clinical physiology: The mouth’s mucosal immunity (secretory IgA, antimicrobial peptides), salivary buffering, and biofilm dynamics interact continuously. When saliva is reduced or plaque persists, defensive thresholds drop, allowing gingivitis to progress to periodontitis, with bone resorption and pocket formation (Scannapieco & Cantos, 2016).
Why this matters: Periodontal inflammation sends cytokines (e.g., IL-6) into circulation, elevating CRP, impairing insulin signaling, and promulgating endothelial dysfunction—a molecular bridge to cardiovascular disease and metabolic deterioration (Tonetti et al., 2013; Winning & Linden, 2017).
The Oral-Gut Axis: A Two-Way Street of Microbial and Immune Signaling
We swallow more than a liter of saliva a day, continuously transferring oral microbes to the gut. The oral-gut axis is bidirectional: oral dysbiosis can colonize the gut, and gut dysbiosis can heighten oral inflammation (Olsen & Yamazaki, 2019; Jia et al., 2021).
From mouth to gut:
Bacterial translocation: Pathogens such as Porphyromonas gingivalis have been identified in gut samples of patients with IBD and colorectal cancer, linking oral pathogens to intestinal inflammation and barrier breakdown (Olsen & Yamazaki, 2019).
Immune modulation: A dysbiotic gut impairs regulatory T cell balance, amplifying gingival reactivity to plaque.
Nutrient malabsorption: Deficits in vitamins A, C, D, and K, and minerals like calcium and magnesium weaken enamel, bone, and mucosa.
Clinical reasoning: Stabilizing the gut barrier and microbiome reduces systemic inflammatory tone, lowering gingival hyperresponsiveness and improving oral outcomes.
Hormones Across the Lifespan: Puberty, Pregnancy, Reproductive Years, and Menopause
Women’s oral health mirrors endocrine changes, with estrogen, progesterone, and testosterone reshaping mucosa, saliva, immune tone, and microbiota (Aparna & Gupta, 2014; Kumar, 2017; Levin & Ashkenazi, 2019).
Puberty: Estrogen/Progesterone and Gingival Sensitivity
Puberty gingivitis: Elevated estrogen and progesterone increase gingival vascularity and edema. Even with plaque levels similar to those of boys, girls exhibit more pronounced gingival inflammation, reflecting hormone-sensitized immune reactivity.
Microbial shifts: Adolescence alters oral microbiota composition; certain taxa can modulate endocrine signaling (e.g., leptin pathways), highlighting microbiome-hormone feedback loops.
Clinical approach: Early education on biofilm disruption (brushing technique, flossing, professional cleanings) reduces hormone-amplified gingival responses.
Pregnancy: Gingivitis, Periodontitis Risk, and Systemic Outcomes
Pregnancy gingivitis:Estrogen elevations heighten gingival sensitivity and bleeding.
Relaxin and tooth mobility:Relaxin can transiently loosen periodontal ligaments, producing a sensation of tooth mobility.
Adverse outcomes: Untreated periodontitis correlates with preterm delivery, low birth weight, and preeclampsia, likely via systemic inflammatory pathways (Boggess, 2008; Wu et al., 2015).
Clinical reasoning: Reducing oral inflammation may lower maternal systemic cytokine levels, thereby mitigating pregnancy risks. Coordinated obstetric-dental care is essential.
Reproductive Years: Oral Contraceptives and Stress
Hormonal formulations: Some oral contraceptives mimic high-estrogen states, increasing gingival vascularity and susceptibility to gingivitis.
Stress physiology: Chronic cortisol elevation temporarily dampens immunity while fostering long-term microbial shifts that favor periodontal pathogens.
Clinical approach: Combine periodontal maintenance with stress modulation strategies—sleep hygiene, mindfulness, targeted exercise—and monitor for hormone-related gingival changes.
Menopause: Xerostomia, Bone Loss, and Burning Mouth Syndrome
Dry mouth (xerostomia): One in three postmenopausal women reports xerostomia; reduced saliva undermines acid buffering, antimicrobial defense, and biofilm clearance, thereby increasing the risk of caries and candidiasis.
Bone loss: Estrogen decline accelerates alveolar bone resorption; women not on HRT often exhibit increased periodontitis compared with those on therapy, suggesting a protective effect that warrants individualized discussion (Levin & Ashkenazi, 2019).
Burning mouth syndrome: Disproportionately affects women (≈7:1), linked to small fiber neuropathy, altered taste, and possible vitamin B12/vitamin D deficiencies (Le & El-Khashab, 2020).
Clinical reasoning: Proactive saliva support, periodontal surveillance, bone health optimization, and nutritional assessment are central to mitigating menopausal oral sequelae.
Prenatal and Early-Life Foundations: Microbiome Transfer and Epigenetic Context
Maternal oral health shapes fetal development through microbiome transfer and epigenetic signaling, affecting immune programming and enamel formation (Boggess, 2008).
Cariogenic flora transfer: A mother’s high burden of cavity-causing bacteria predisposes infants to early caries.
Placental health: Oral bacteria can enter maternal circulation, influencing placental inflammation.
Enamel development: Maternal vitamin D supports enamel mineralization; deficiencies increase hypomineralization risk in molars and incisors.
Clinical reasoning: Preconception and prenatal periodontal screening, along with vitamin D optimization, are practical, high-yield preventive steps.
Gingival Enlargement vs. Gingivitis: Differentiating Physiology, Pathology, and Medications
Gingival enlargement may arise from physiological states (puberty, pregnancy), hereditary conditions (gingival fibromatosis), systemic disease (e.g., leukemia, sarcoidosis), or medications—notably calcium channel blockers, phenytoin, and cyclosporine.
Drug-induced gingival overgrowth (DGO): Overgrown gingiva creates pseudopockets, harbors pathogens, complicates hygiene, and affects self-esteem; in our clinic, we have seen significant enlargement associated with metoprolol.
Gingivitis: A reversible inflammatory response to plaque toxins, presenting with redness, swelling, tenderness, bleeding, and halitosis.
Clinical reasoning: Differentiation guides management. With DGO, we coordinate with internal medicine and pharmacy to review alternatives, step down risks, and intensify periodontal maintenance.
Aligned & Empowered: Chiropractic Conversations on Women’s Health- Video
Oral Health and Chronic Disease: Cardiovascular, Diabetes, Pulmonary, Cancer, and Neurodegeneration
The oral-systemic link is robust and clinically actionable.
Cardiovascular disease:Periodontal disease elevates IL-6, CRP, and leukocyte counts, fueling atherogenesis, arterial stiffness, and possibly atrial remodeling, which increases AFib susceptibility (Desvarieux et al., 2013; Tonetti et al., 2013).
Endocarditis: Oral bacteremia, especially Streptococcus viridans, can seed damaged valves; vigilance and dental coordination are paramount.
Diabetes: Bidirectional relationship—periodontitis worsens glycemic control via systemic inflammation; hyperglycemia impairs neutrophil function and wound healing. Periodontal care improves HbA1c (Chapple & Genco, 2013).
Pulmonary disease: Oral pathogens are aspirated, contributing to pneumonia and worsening COPD/asthma, especially in the elderly and immunocompromised.
Cancer risk: Chronic oral inflammation is associated with increased risk across multiple cancers, potentially through immune dysregulation and microbial translocation (Michaud et al., 2007).
Alzheimer’s disease:Porphyromonas gingivalis and its gingipains are found in Alzheimer’s brains; mechanisms include blood-brain barrier penetration, neuroinflammation, and amyloid acceleration (Dominy et al., 2019).
Clinical reasoning: Treating periodontal disease is not merely a dental task—it is a systemic prevention strategy that may lower cardiometabolic risk, pulmonary complications, and neuroinflammatory burden.
Endothelial Dysfunction and Biological Aging: Oral Inflammation as a Vascular Accelerator
Young adults with periodontal disease show endothelial dysfunction similar to much older counterparts, indicating that oral inflammation accelerates biological aging at the vascular level. We incorporate vascular age markers and inflammatory panels into functional assessments, aiming to reverse periodontal drivers to slow vascular aging trajectories.
Evidence-Based Oral Hygiene: Techniques Patients Rarely Get Taught
Most adults brush incorrectly. Correct technique matters because biofilm removal determines gingival and enamel outcomes.
Brush twice daily for two minutes with a 45-degree angle to the gumline
Small circular strokes, not horizontal scrubbing, to avoid enamel abrasion
Cover front, back, and occlusal surfaces
Brush the tongue to reduce biofilm and volatile sulfur compounds
Use a pea-sized fluoride toothpaste; larger amounts add no benefit
Do not rinse for 15–20 minutes post-brushing to allow fluoride remineralization
Floss daily to disrupt interproximal biofilm
Clinical reasoning: These steps align with ADA guidance and improve biofilm disruption, pH buffering, and enamel remineralization, reducing the inflammatory substrate for systemic disease.
Functional Medicine Strategies: Nutrition, Microbiome, and Stress Modulation
We employ advanced testing and integrative protocols to restore systemic balance:
Dietary strategies:Anti-inflammatory, whole-food nutrition; lower sugar and refined carbohydrates to reduce cariogenic fuel; targeted prebiotics/probiotics to support Lactobacilli and re-establish oral and gut microbial symmetry.
Hygiene adjuncts:Frequent toothbrush replacement, tongue brushing, and pillowcase hygiene to minimize nightly re-inoculation.
Clinical reasoning: By lowering systemic inflammatory tone, normalizing the gut barrier, and reducing oral acid load, we create conditions in which gingival tissues heal and microbiota re-stabilize.
Integrative Chiropractic Care: Nervous System Regulation and Inflammation Control
From a chiropractic perspective, spinal alignment and autonomic balance influence salivary function, immune regulation, and stress physiology, which are central to oral outcomes.
Autonomic modulation: Cervical and thoracic spinal segments influence parasympathetic output to salivary glands; adjustments may optimize salivary flow and mucosal defense.
Inflammation reduction: Adjustments may be associated with lower IL-6 and CRP levels, aligning with periodontal and cardiometabolic goals.
Vagus nerve and gut-brain axis: By improving vagal tone, we support gut motility, immune regulation, and microbiome stability, indirectly benefiting oral health (Bowen et al., 2018).
Clinical reasoning: Chiropractic care complements medical and functional protocols by addressing neurophysiological drivers of inflammation and salivary function, reducing the systemic substrate for oral disease.
Medication-Induced Oral Changes: Anticipation, Alternatives, and Coordination
Medications commonly alter oral physiology:
Xerostomia:Antidepressants, diuretics, antihistamines, and decongestants reduce saliva.
Clinical reasoning: Proactive management prevents downstream periodontal complications and improves patient quality of life.
Closing Gaps in Women’s Oral Health: Access, Policy, and Practical Care
Oral health is often excluded from adult insurance coverage, creating disparities—especially for women in caregiving roles and non-traditional employment. Despite women often visiting dentists more frequently, coverage gaps persist.
In-clinic interventions: Include toothbrushes in wellness kits, ask about brushing habits and dental frequency, and connect patients with community dental resources.
Care integration: Build referral partnerships with dentists to enable bidirectional management of periodontitis, medication-induced changes, and pregnancy-related oral care.
Clinical reasoning: Small, consistent steps yield large preventive dividends, reducing chronic disease burden and improving systemic outcomes.
Clinical Observations and Patient Education
From our ongoing clinical work and research documented at WellnessDoctorRx.com and my LinkedIn profile, I consistently observe:
Patients with well-coordinated dental-medical-chiropractic care exhibit lower inflammatory markers and improved glycemic control.
Teaching brushing technique and non-rinsing fluoride retention significantly reduces gingival bleeding within weeks.
Addressing stress physiology and sleep quality enhances resilience of the oral and gut microbiomes, with improvements in halitosis, plaque scores, and periodontal pocket depths.
We educate patients on the “why” behind every recommendation to bolster adherence and outcomes.
Practical Takeaways: What You Can Do Today
Emphasize daily biofilm disruption: correct brushing, flossing, and tongue cleaning.
Reduce sugar and refined carbohydrates to lower acid load
Support saliva: hydrate, xylitol gum, saliva substitutes if needed
Coordinate medical-dental care, especially for medications impacting oral health
Address gut health: anti-inflammatory diet, targeted probiotics
Schedule periodontal maintenance more frequently if you have chronic inflammatory conditions
Conclusion: One Body, One System
The mouth is not an isolated organ; it is a living interface with the body’s endocrine, immune, and neurological networks. Periodontal disease, oral dysbiosis, and medication-induced changes are systemic risk modifiers that influence heart disease, diabetes, lung health, cancer risk, and neurodegeneration. At our clinic in El Paso, under the collaborative guidance of Dr. Maria Guadalupe Cardenas, MD, and me, we deliver integrative, evidence-based care centered on the whole person. The future of health lies in collaboration, prevention, and whole-system thinking—and oral health is a vital chapter in every patient’s wellness story.
The information on this blog site is not intended to replace a one-on-one relationship with a qualified healthcare 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.
Welcome to El Paso's Premier Wellness and Injury Care Clinic & Wellness Blog, where Dr. Alex Jimenez, DC, FNP-C, a board-certified Family Practice Nurse Practitioner (FNP-BC) and Chiropractor (DC), presents insights on how our 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.comsite, focusing on restoring health naturally for patients of all ages.
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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.
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
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