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    Lymphangioleiomyomatosis Medical Slides

    Generate publication-quality lymphangioleiomyomatosis lecture slides in 30 seconds. AI-powered content structured for clinical education.

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    Why teach Lymphangioleiomyomatosis?

    Lymphangioleiomyomatosis is a rare progressive cystic lung disease occurring almost exclusively in women of reproductive age, with a prevalence of 3-8 per million women. LAM can be sporadic or associated with tuberous sclerosis complex (TSC-LAM). The discovery of mTOR pathway activation led to the landmark MILES trial, establishing sirolimus as the first effective pharmacotherapy and transforming this disease from untreatable to manageable.

    Sample Lecture Slides

    What AI generates for Lymphangioleiomyomatosis

    Enter “Lymphangioleiomyomatosis” and SlideCraft generates a complete lecture deck with slides like these.

    01Pathogenesis: TSC1/TSC2 Mutations, mTOR Pathway Activation, and LAM Cell Biology
    02HRCT: Diffuse Thin-Walled Cysts, Uniform Size and Distribution
    03Clinical Presentation: Pneumothorax, Chylothorax, Renal Angiomyolipomas, and Dyspnea
    04Diagnosis: VEGF-D (≥800 pg/mL), HRCT Pattern, and When Biopsy Is Needed
    05Sirolimus Therapy: MILES Trial (FEV1 Stabilization) and Long-Term Management
    06Pregnancy and Hormonal Considerations: Estrogen Avoidance and Risk Counseling
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    Lymphangioleiomyomatosis Presentation FAQ

    How should the MILES trial be presented as the pivotal therapy evidence?

    Present the MILES trial (McCormack 2011, NEJM): double-blind RCT of sirolimus vs placebo in LAM patients with FEV1 <70%. Sirolimus stabilized FEV1 (mean change +1 mL/month vs -12 mL/month decline with placebo), improved quality of life, reduced serum VEGF-D levels, and stabilized gas trapping. However, FEV1 decline resumed after drug discontinuation. This established sirolimus as standard of care for progressive LAM, with indefinite treatment recommended.

    What diagnostic criteria should be included in LAM teaching slides?

    Present the ATS/JRS 2017 diagnostic criteria: Definite LAM requires characteristic cystic HRCT plus any one of: TSC diagnosis, renal angiomyolipoma, elevated VEGF-D ≥800 pg/mL, chylothorax/chylous ascites, LAM cells in biopsy. Probable LAM: characteristic HRCT plus compatible clinical history (pneumothorax in young woman). VEGF-D has 73% sensitivity and 100% specificity at ≥800 pg/mL threshold — often avoids need for surgical biopsy.

    How should the cystic lung disease differential be presented?

    Present the systematic HRCT-based differential: LAM (diffuse, round, thin-walled, uniform cysts in a woman of childbearing age), PLCH (irregular/bizarre-shaped cysts, upper-lobe predominant, smoker), Birt-Hogg-Dubé (lower-lobe/medial predominant cysts, skin fibrofolliculomas, renal tumors, FLCN gene mutation), lymphocytic interstitial pneumonia (lower-lobe ground-glass with cysts, associated with Sjögren syndrome), and cystic metastases (variable wall thickness, cancer history). VEGF-D helps distinguish LAM from mimics.

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