Management of rare types Mycosis fungoides and Sézary syndrome

Management of rare types of Mycosis fungoides and Sézary syndrome

Mycosis Fungoides and Sézary Syndrome

Mycosis fungoides and Sézary syndrome are rare types of CTCL. Sézary syndrome is more aggressive, with widespread skin redness (erythroderma), blood, and lymph nodes, whereas mycosis fungoides develops gradually with patchy rashes. There is no cure, but therapies can help manage symptoms and delay progression.

Mycosis Fungoides

Type: Non-Hodgkin lymphoma affecting cutaneous T cells.
It has a slow onset and is commonly misinterpreted as eczema or psoriasis.

Symptoms:

Early symptoms include scaly patches and itchy rash on sun-protected areas (buttocks, thighs, and breasts).
Later, plaques, tumours, hair loss, and swollen lymph nodes may develop.
Progression: Skin-confined for years; may spread to lymph nodes, blood, or organs.

Treatment:

Steroid creams, topical chemotherapy with mechlorethamine, and phototherapy (PUVA, UVB) are all options for skin treatment.
Interferon, HDAC inhibitors, monoclonal antibodies, and retinoids (bexarotene) are systemic.
Localised or complete skin radiation.
Advanced bone marrow transplant.
Prognosis: Early stages have a 95% 10-year survival probability, while advanced disease reduces life expectancy to 3-5 years.

Sézary Syndrome

Leukemic CTCL affects skin, blood, and lymph nodes.
Rapid, systemic engagement.

Symptoms:

Rash with severe itching, burning, and discomfort.
Swollen lymph nodes, hair loss, nail changes, and ectropion.
Fever, fatigue, and weight loss.

Diagnosis:

Blood smear displaying Sézary cells (malignant T cells with folded “brain-like” nuclei).
CT/PET imaging, skin and lymph node biopsy, and flow cytometry were performed.

Treatment:

The video is about the Treatment of the early stages of disease

Skin-directed treatments include topical steroids, retinoids, phototherapy, and whole skin electron beam therapy.
Systemic: ECP, targeted therapy, immunotherapy, HDAC inhibitors, and chemotherapy.
Allogeneic bone marrow transplant in advanced instances.
Prognosis: Chronic, incurable; ~24% 5-year survival rate.

Mycosis fungoides causes and Sézary syndrome

Causes of Mycosis Fungoides include DNA abnormalities in T-cells, which impede normal cell death and cause uncontrolled proliferation.
Despite its name, it is not fungal.

Risk factors:

More common in 50+ adults
Men are more likely
Blacks are at higher risk, typically younger.

Possible causes:

Environmental toxins (e.g., industrial chemicals, fire retardants)
Long-term immune stimulation (autoimmune illness)
Studying viral illnesses, no definitive link yet
Genetics: Mutations are normally acquired, not inherited.

Sézary Syndrome Causes

T-cell genetic mutations: Similar to MF, but cancerous cells called “Sézary cells” circulate in blood.
Leukemic variant: Systemic CTCL affecting skin, blood, and lymph nodes.

Risk factors:

Elderly (usually diagnosed in 60s–70s)
Mycosis fungoides history (MF can become SS)
HTLV‑1/II virus infection may be linked in certain places (Japan, the Caribbean, and the Middle East).

Pathophysiology:

Malignant CD4+ T-cells have aberrant markers (CD7, CD26 deletion).
Cytokines from these cells weaken immunity, increasing infection risk.

Who's vulnerable?

Though the cause is unknown, mycosis fungoides and Sézary syndrome patients share demographic and clinical traits. Risk patterns have been found for some uncommon malignancies.

General CTCL Risks

Cases mostly affect adults over 50.
Men are impacted twice as often as women.
Ethnicity: Blacks are more likely to be diagnosed early and with advanced disease.
Immunological system dysfunction: Autoimmune or chronic immunological activation may raise risk.
Exposure to industrial chemicals, insecticides, or fire retardants may be a factor (under study).
Some cases have been connected to HTLV-1/II infection, particularly in endemic countries like Japan, the Caribbean, and the Middle East.

Specific Mycosis Fungoides Risks

Slow onset: Misdiagnosed as eczema or psoriasis early on.
Risk: Older men, especially darker-skinned ones, are more likely to develop MF.
A small percentage of MF patients develop progressive disease or Sézary syndrome.

Specific Sézary Syndrome Risks

Age: Usually diagnosed in the 60s–70s.
Patients with long-term MF may acquire SS as a leukemic change.
Systemic involvement: Immune suppression makes SS more aggressive and infectious.

Comparative Table Feature: Mycosis Fungoides Sézary Syndrome

Slow, skin-specific onset. Systemic, fast
Pimples, plaques, tumours. Scaling, diffuse erythroderma
In late-stage disease, blood involvement occurs, and early Sézary cells appear.
Prognosis: Early good, poor, aggressive
Treatment focus: Skin-directed and systemic. Systemic + skin-directed

Key Risks

Both disorders weaken the immune system, increasing infection risk.
Sézary syndrome can become aggressive lymphoma.
Emotional and quality-of-life impacts from continuous itching, noticeable skin changes, and long-term treatment.

Recent cutaneous T cell lymphoma therapy

New CTCL treatments for mycosis fungoides and Sézary syndrome include mogamulizumab, lacutamab, CAR-T therapies, and new skin-directed techniques including HyBryte photodynamic therapy. These breakthroughs improve response rates and quality of life, especially for relapsed or refractory individuals.

Important New Therapies

Anti-CCR4 monoclonal antibody Mogamulizumab plays a significant role in inflammation and autoimmune diseases and is often overexpressed in specific T-cells.
Improves symptoms and survival in patients with relapsed/refractory mycosis fungoides and Sézary syndrome.
Data from the 2026 World Congress of Cutaneous Lymphomas demonstrate real-world efficacy and patient-reported results.

Lacutamab is an anti-KIR3DL2 antibody.

The FDA granted breakthrough treatment status for Sézary syndrome in 2025.
Results: ~43% response rate, median length of 25.6 months.

CAR-T Therapy

CTX130, a CD70-directed allogeneic CAR-T, resolved T-cell fratricide concerns.
It met a response rate of ~46% in strongly pretreated individuals.
Combine HDAC and PI3K inhibitors
Combine tenalisib, duvelisib, and linperlisib with HDAC inhibitors.
Refractory CTCL response rates 50–60%.

HYBRYTE Photodynamic Therapy

Light-activated synthetic hypericin.
The Phase 3 FLASH trial helped with early-stage disease.

Risks and Factors

Possible side effects include skin irritation (phototherapy), immunological suppression (CAR-T, antibodies), and GI toxicity (HDAC/PI3K combinations).
Access: Many medicines are in clinical trials; availability varies by region.
Quality of life: Toxicology might reduce survival benefits, therefore patient-reported outcomes are increasingly included in approvals.

CTCL diagnostics

The diagnosis of cutaneous T-cell lymphoma (CTCL) involves skin samples, blood testing, and sophisticated imaging techniques. CTCL commonly mimics eczema or psoriasis, requiring numerous biopsies and specialist molecular tests to diagnose.

Essential Diagnostics

Physical checkup
A dermatologist checks for scaly patches, plaques, and malignancies.
Assesses lymph node swelling and systemic involvement.

Biopsy of skin

Circular punch or scalpel biopsy.
A pathologist checks tissue for cancerous T-cells.
Since early lesions resemble benign rashes, many biopsies may be needed.

Tests of blood

All-blood CBC with differential.
Buffy coat smear for Sézary cells (malignant T-cells with folded nucleus).
Assess disease aggressiveness with LDH and uric acid.

Cytometry flow

Identifies aberrant T-cells (e.g., CD4/CD8 ratio >10).
Detects T-cell antigen loss (CD2, CD3, CD4, CD5).
Verifies pathogenic clones.

Molecular tests

Use PCR or Southern blot to identify a dominant T-cell clone.
Differentiates CTCL from inflammatory dermatoses.

Genetic testing

Identifies DNA alterations causing T-cell proliferation issues.

Imaging tests

CT or PET scans for lymph node or organ spread.
X-ray of the chest for lung involvement.

Diagnostic Criteria for Sézary Syndrome

≥1000/µL absolute Sézary cell count.
The immune system is abnormal, with an increased CD4+ population and a changed CD4/CD8 ratio.
There is evidence of a cancerous T-cell clone in the peripheral blood.

Risks and Challenges

Possible misdiagnosis: Early CTCL lesions resemble eczema/psoriasis.
Need for repeat biopsies: Initial samples may not include cancer cells.
Systemic involvement: Needs imaging and blood tests to prevent understaging.

Conclusion

Cutaneous T-cell lymphomas (CTCL), also known as mycosis fungoides and Sézary syndrome, are rare but serious blood cancers that affect the skin.

Early skin-directed therapy helps manage slow-growing mycosis fungoides, which can remain on the skin for years.

Sézary syndrome is an aggressive leukemia that affects the blood and lymph nodes early and has inferior survival.

CTCL is a difficult disease that requires multidisciplinary diagnosis and tailored treatment. Research is improving patient survival and quality of life.

Incontinence associated dermatitis management

Incontinence-associated dermatitis management

Incontinence-Related Dermatitis

Incontinence-associated dermatitis (IAD) is a common skin disorder caused by prolonged exposure to urine or faeces, resulting in irritation, pain, and infection. IAD can affect people of all ages, but it is most common in the elderly and those with limited mobility. Avoiding dampness, utilizing absorbent items, and using skin barriers are prevention methods.

Incontinence-associated dermatitis

What is IAD?

Repeated urine and stool exposure causes irritating contact dermatitis.

Itching, burning, erythema, maceration, erosion, scaling, and secondary infections (mostly Candida albicans) may occur. Skin folds in the buttocks, perineal, and perianal areas. The incidence is 3–30% among elderly individuals, especially those in long-term care.

Possible Risks

Infants (diaper dermatitis) and elderly adults (skin thinning, poorer recovery).
Mobility Issues: Sitting or lying increases danger.
Health issues: Diabetes, obesity, chronic diarrhea.
Incontinence can worsen with diuretics, laxatives, antibiotics, and sedatives.
Weak Skin Barrier: Frequent harsh soap washing or absorbent product occlusion.

Diagnosis

Clinical Examination: Clear inflammation in exposed regions.
Severity Scales: GLOBIAD classifies moderate (erythema without erosion) and severe (erosions).
Differentiation: From allergic contact dermatitis, pressure injuries, and intertrigo.

Prevention/Management

Zinc oxide and dimethicone barrier creams and gentle cleansers protect skin.
Briefs/diapers with high absorbency, changed often.
Moisture control: External urine/stool collectors or catheters in extreme situations.

The 4 types of incontinence?

Stress, urge, overflow, and functional incontinence are the main categories. Treatment depends on the aetiology and symptoms of each type.

Incontinence under stress

Physical exercise, coughing, sneezing, and laughing cause leakage.
This condition is due to pelvic floor weakness or urethral sphincter injury.
This condition is common among postpartum women and men who have had prostate surgery.

Overactive bladder (urge)

Involuntary urination after a strong need.
This condition is related to hyperactive bladder muscles, nerve injury, diabetes, Parkinson's, or stroke.
More common among seniors.

Overflowing urine

Dribbling or leaks result from incomplete bladder emptying.
This is usually caused by weak bladder muscles, nerve injury, or obstruction, such as an enlarged prostate or tumours.

Commoner among guys.

Functional incontinence
Leakage happens when physical or cognitive problems delay restroom use.
Arthritis (loss of mobility) and dementia.

Risks and Factors

Skin irritation (IAD), UTIs, and social isolation.
Hot, humid weather accelerates skin deterioration from leaks. Protection, such as barrier creams and frequent changes, is crucial.
Depending on the type, treatment may include pelvic floor exercises, bladder training, medications, absorbents, or surgery.

IAD risk factors

Major IAD Risk Factors

Extended dampness
Urine and faeces overhydrate the skin, break down the stratum corneum, and irritate it.
Frequent diarrhoea, stools
Loose stools (particularly Bristol Stool Chart type 7) raise the risk 51-fold over formed stools.

Limited mobility

Bedridden and wheelchair-bound patients have extended skin occlusion and friction, increasing risk.

Occlusion, friction

Multiple linen layers, diapers, and briefs trap moisture and create shear pressures, damaging skin.

Age-related skin changes

The thinner epidermis, slower healing, and decreased barrier integrity make older adults more susceptible to complications.

Comorbidities

Diabetes, obesity, and vascular disease weaken skin.

Medications

Incontinence and skin barrier weakness can result from diuretics, laxatives, antibiotics, sedatives, and corticosteroids.

Sex and critical disease

Female sex, vasopressor use, and ICU stays increase IAD risk.

IAD-prevention methods

The best ways to prevent Incontinence-Associated Dermatitis (IAD) are to avoid urine and stool contact, cleanse gently, and use barrier products. To prevent moisture and fungal infections in Chennai's hot and humid atmosphere, permeable absorbent materials and frequent changes are essential.

Main Prevention Methods

Managing incontinence

Find and treat reversible causes (e.g., UTI, constipation, drug side effects).
Only use catheters or external urine/stool collection devices in extreme situations.

Products that absorb

Select pads/diapers with extremely absorbent polymers.
Change frequently to avoid skin overhydration.
Many layers of linen or pads trap heat and moisture.

Organised skincare

At least every day, gently cleanse skin after incontinence.
Avoid strong soaps and use pH-balanced cleaners.
Use zinc oxide or dimethicone barrier creams to avoid irritation.

Skin protection

Occlusion can be reduced with breathable garments and absorbent items.
Regularly check groin, buttocks, and abdominal apron skin folds.
Possible secondary Candida infection? Use antifungal creams.

IAD medication hazards

Certain drugs might aggravate incontinence or damage the skin's natural barrier, increasing the risk of IAD.

Medication Risks in IAD

Diuretics
Boost urine output to leak more.
Higher moisture exposure increases skin deterioration.
Laxatives
Diarrhoea is a prominent indicator of IAD.
Lipases and proteases in liquid poo irritate skin more than stool.

Antibiotics

Causes diarrhea by disrupting gut bacteria.
Affected skin is more susceptible to Candida albicans infections.
Hypnotics/sedatives
Lower bladder/bowel awareness.
Patients may delay their incontinence response, prolonging skin exposure.

Corticosteroids

This can lead to a weak skin barrier and slow wound healing.
Increase irritation and infection risk.

A Review of Medication Risk

Medication Impact on Clinical Issue
Increased urine leakage with diuretics. Frequent exposure, maceration
Laxatives: diarrhoea, loose stool. Strongest IAD predictor
Antibiotics alter gut flora. Fungus + diarrhea
Low awareness due to sedatives. Slow hygiene response
Corticosteroids: Weak skin barrier. Slower healing, infection risk

Also, https://www.droracle.ai/articles/1062687/what-is-the-recommended-management-for-skin-irritation-due

Treating incontinence-related dermatitis

Incontinence-Associated Dermatitis (IAD) treatment involves repairing the skin barrier, decreasing urine and stool exposure, and controlling subsequent infections. Barrier creams and gentle washing usually cure mild infections, while severe cases may require short-term corticosteroids or antifungal/antibiotic medication.

Key Treatment Principles

Reducing exposure
Treat UTIs and constipation to manage incontinence.
Change high-absorbency pads/diapers often.
Limited linen or garment layers limit heat and dampness.
Organised skincare
Avoid strong soaps and use pH-balanced cleansers.
After episodes, use zinc oxide or dimethicone barrier creams.
Perform daily skin inspections, focusing especially on creases and the perineum.

Topical remedies

Emollients and barrier creams for mild instances.
Add short-term topical corticosteroids for moderate instances.
Consider external urine/stool collecting devices and medicinal ointments for severe erosions.

Management of infections

Topical clotrimazole and nystatin for candida
Bacterial infections: Topical or systemic antibiotics for purulent exudate.

Treatment by Severity

The Severity Treatment Approach
Skin intact, erythema mild. Gentle cleaning, absorbing barrier creams
Moderate (pain, erosions) Barrier + short-term corticosteroids, regimented
Erosions + infection: severe Antifungal/antibiotic treatment, external collection
To treat chronic IAD, use long-term barrier care, avoid allergic items, and monitor for lichenification

Key Takeaway

IAD treatment must be holistic:
Avoid exposure.
Keep the skin barrier intact.
Treat infections quickly.
Adjust tactics for local climate.

Conclusion

Incontinence-Associated Dermatitis, caused by chronic urine and stool contact, is avoidable and prevalent. It causes discomfort, redness, erosion, and infection, lowering the quality of life.

Corticosteroids, antifungals, or antibiotics may be needed for severe instances, whereas barrier creams and cleansing work for minor cases.

Diuretics, laxatives, antibiotics, sedatives, and corticosteroids might increase incontinence and skin vulnerability.

How does one develop Hashimoto's thyroid disease?

Hashimoto's Thyroid Info

Hashimoto's thyroiditis causes most hypothyroidism worldwide, especially in women aged 30–60. The immune system targets the thyroid gland, reducing hormone synthesis and causing fatigue, weight gain, cold sensitivity, and depression. Levothyroxine is frequently prescribed for life.

Hashimoto's Thyroid

Define Hashimoto's thyroiditis.

Autoimmune disorder: TPO and Tg antibodies assault thyroid cells. Inflammation, goitre, and hormone reduction affect the thyroid gland. This autoimmune disorder is the main cause of hypothyroidism in the U.S. and worldwide.

Symptoms

Early stage: Antibodies often cause no symptoms.

Stage progression:

Laziness, melancholy, fatigue
Weight gain, constipation, dry skin
Hair loss, brittle nails, bloated face
Thyroid enlargement causing neck discomfort or swallowing problems
Women's menstrual irregularities

Diagnosis

Blood tests: high TSH, low free T4, thyroid antibodies.
Ultrasound: May reveal thyroid inflammation or hypertrophy.
Autoimmune illnesses often run in families.

Risk Factor: Details

Females are 7-10 times more likely to develop Hashimoto's disease.
Typically, they are between 30 and 60 years old.
Family history of thyroid/autoimmune disease raises risk.
Lupus, rheumatoid arthritis, and Type 1 diabetes are autoimmune illnesses.
Hashimoto's can develop after pregnancy due to immune changes.
Consuming too much iodine may increase risk.
Radiation: Environmental radiation damages thyroids.

Possible complications if untreated

Thyroid enlargement affects swallowing/breathing.
High LDL, heart failure risk.
Depression and cognitive deterioration.
Infertility, irregular cycles, and poor pregnancy results.
Myxedema coma: Rare, life-threatening emergency requiring prompt treatment.

Why does Hashimoto's illness occur?

Unexpected immune system attacks on the thyroid gland produce chronic inflammation and gradual loss of thyroid hormone–producing cells in Hashimoto's disease. Genetic predisposition and environmental factors, including illnesses, stress, radiation exposure, and increased iodine intake, are likely causes.

Development of Hashimoto's

Autoimmune reaction: Anti-thyroid peroxidase and anti-thyroglobulin antibodies attack thyroid cells.
Cell damage: White blood cells inflame and scar the thyroid.
Decreased thyroid hormone production causes hypothyroidism.

The video explains what happens if Hashimoto's thyroiditis is not treated

What's the best Hashimoto's treatment?

Whether Hashimoto's illness has induced hypothyroidism determines its optimum treatment. As an autoimmune disease, Hashimoto's has no cure; thus, doctors manage thyroid hormone levels and symptoms.

Usual Treatment

Levothyroxine:

Synthetic thyroid hormone is similar to T4.
To normalize hormone levels, take them daily, generally forever.
Blood tests (TSH, free T₄) determine dose adjustments.

Monitoring:

Periodic thyroid tests (6–12 months).
Changes during pregnancy, illness, or weight.

Supportive Measures

Balanced diet: Selenium, zinc, and vitamin D may benefit thyroid function.

Keep iodine low to prevent autoimmune thyroid injury.
Manage stress: Stress might worsen autoimmune disease.
Treat comorbid autoimmune conditions: Many patients have type 1 diabetes, celiac disease, or rheumatoid arthritis.

In Need of Treatment

If thyroid hormones are normal: Monitor, no medication.
For hypothyroidism, lifelong levothyroxine is best.
If goitre impairs swallowing or breathing, surgery may be considered.

Details on levothyroxine therapy?

Lifelong replacement of thyroid hormone with synthetic levothyroxine is the best treatment for Hashimoto's illness. It fixes hormone levels, improves hypothyroidism symptoms, and is safe and effective when monitored.

Levothyroxine Treatment Details

Goal: Replaces T4 deficiency caused by Hashimoto's hypothyroidism.
One dose per day, usually in the morning on an empty stomach.
Take 30–60 minutes before eating for best absorption. Iron, calcium, soy, antacids, and cholesterol-lowering medications interact with absorption and should be taken 4 hours apart.

Dosing & Monitoring

Individualised dose: Age, weight, hypothyroidism severity, and other medical problems.
First monitoring: TSH levels 6–10 weeks following therapy.
After stabilization, thyroid function is evaluated annually or after dose adjustments.
New drugs, pregnancy, or considerable weight changes require adjustments.

Warnings and Side Effects

Safe: Mimics natural hormones; therefore, adverse effects are rare with proper dosage.
Hormone overdose can cause tachycardia, anxiety, sleeplessness, and osteoporosis.
Supplements (iron, calcium), high-fibre diets, and medications can diminish efficacy.

Alternates and Additives

In cases of persistent symptoms despite normal TSH, liothyronine is added. Rapid heartbeat and anxiousness are side effects.
T4/T3 combination therapy: 3–6-month trial in selected patients.
Deriving from animal thyroid glands, hormone levels vary and are unpredictable. Many endocrinologists favour levothyroxine for consistency.

What is Hashimoto's initial stage?

Hashimoto's thyroiditis' early stage is often undetected. Anti-thyroid peroxidase and anti-thyroglobulin antibodies are produced by the immune system early on, while thyroid hormone levels remain normal.

Initial Features

Antibodies destroy thyroid tissue, but the gland adapts.
Euthyroid: T₄ and T₃ levels are normal.
A tiny goitre may develop in certain people.
Many people feel fine; fatigue or mood problems may occur.

Progression

Thyroid hormone production declines with time.
Normal T4 and slightly raised TSH cause subclinical hypothyroidism.
Progressive hypothyroidism causes weight gain, cold intolerance, and depression.

Hashimoto's stages

Description of Stage
Silent phase: Antibodies, normal thyroid function.
TSH rises, T₄ is normal, and there are minor symptoms from subclinical hypothyroidism.
Overt hypothyroidism: high TSH, low T4 levels, and distinct symptoms.
Advanced thyroid disease requires lifelong hormone supplementation due to shrinkage or fibrosis.

Hashimoto's: 10 foods to avoid?

10-Foods to Avoid with Hashimoto's

Grains with gluten. Molecular mimicry between gluten and thyroid tissue can aggravate autoimmune attack. Wheat, pasta, barley, rye, spelt, beer, soy sauce
Isoflavones in soy reduce the absorption of levothyroxine and the synthesis of thyroid hormones. Soy milk, tofu, edamame, protein powders
Too much iodine: Too much iodine stimulates thyroid autoimmunity. Spirulina, kelp, seaweed snacks, iodised salt mixes
Highly processed foods: Sugar, emulsifiers, and additives cause inflammation. Packaged snacks, quick food, candy, beverage
Cruciferous raw: Eaten in excess, goitrogens impede thyroid hormone synthesis. Kale, broccoli, cabbage, Brussels sprouts, raw
High omega-6 content in industrial seed oils causes inflammation. Soybean, corn, sunflower, and canola oils
If lactose-intolerant, dairy can decrease levothyroxine absorption and aggravate stomach discomfort. Milk, cheese, ice cream
Refined sugar can cause insulin resistance and inflammation. Desserts, cookies, and sweetened cereals
Alcohol: Impairs liver and thyroid hormone metabolism. Beer, wine, spirits
Preservatives and nitrates in processed meats can cause inflammation and intestinal permeability. Sausages, bacon, deli meats

Safer Options

Rice, quinoa, buckwheat, and certified GF oats.
Eggs, poultry, fish, and lentils are soy-free.
Use tiny amounts of plain iodised salt and avoid seaweed snacks.
Using steam to cook crucifers reduces goitrogen levels by ~60%.
Olive, avocado, and coconut oils are healthy.

Hashimoto's vs. hypothyroidism

Hashimoto’s disease

Definition: Thyroid-attacking autoimmune disease.
Mechanism: Antibodies (anti-TPO, anti-Tg) attack thyroid cells, causing inflammation and declining function.
Progression: Normal thyroid function → subclinical hypothyroidism → overt hypothyroidism.
Goiter, weariness, moderate mood changes, or no symptoms may start.
Early monitoring is followed by levothyroxine medication for hypothyroidism.

Hypothyroidism

Definition: An underactive thyroid gland that produces insufficient T4, T3.

Causes:
Hashimoto's thyroiditis dominates.
Iodine deficiency/excess, thyroid surgery, radiation therapy, and medicines are further reasons.
Fatigue, weight gain, cold intolerance, constipation, dry skin, depression, and menstrual abnormalities.
Treatment: Lifelong levothyroxine.