Which of the following is true regarding extended criteria donors for liver transplantation?

Donors aged >60 years with no significant comorbidities

Donors with well-controlled diabetes mellitus

Hepatitis C antibody positive donors

Donors with significant uncontrolled comorbidities

Which of the following is not true about lupus nephritis in pregnancy?

Ecosprin, methotrexate, cyclophosphamide, corticosteroids, azathioprine are safe in pregnancy

Pregnancy to be planned once the disease has been quiescent for at least 6 months and there is no evidence of renal dysfunction

High dose corticosteroids for lupus flare in pregnancy is safe

Immunosuppression can be continued during pregnancy

After the first postoperative year of cardiac transplantation, what is the most common cause of death?

Accelerated graft arteriosclerosis

Infection in a renal transplant patient is usually caused by which pathogen?

Human Immunodeficiency Virus (HIV)

Which of the following should be avoided in the long-term follow-up of a renal transplant recipient on ciclosporin?

Prescribe drugs that inhibit cytochrome P450 activity

Transplantation in Special Populations for FMGE: High-Yield Surgery Lessons

Transplantation in Special Populations - Tiny Titans, Big Hopes

Pediatric transplantation: unique challenges in growth, neurodevelopment, adherence, psychosocial aspects.
Anatomical: smaller vessels, organ size mismatch, technical modifications.
Immunosuppression: weight/BSA-based dosing; ↑risk PTLD (EBV-driven), infections. Monitor long-term effects.
Common indications:
- Liver: Biliary atresia (most common).
- Kidney: CAKUT (Congenital Anomalies of the Kidney and Urinary Tract).
- Heart: Congenital heart defects.
Growth & development: critical monitoring; nutritional support vital. Growth hormone considered.
Living donor kidney transplant often preferred for better outcomes.

⭐ PTLD (Post-Transplant Lymphoproliferative Disorder), often EBV-related, is a significant concern in pediatric solid organ transplant, with incidence varying by organ and immunosuppression intensity.

Transplantation in Special Populations - Golden Years, New Leases

Eligibility: Chronological age (e.g., >65 yrs) less critical than physiological age & comorbidities.
Key Challenges:
- ↑ Comorbidities (cardiac, diabetes, prior malignancy).
- Immunosenescence: may ↓ rejection but ↑ infection/malignancy risk.
- Polypharmacy & frailty assessment crucial.
Evaluation: Comprehensive Geriatric Assessment (CGA) vital.
Immunosuppression: Tailored regimens to balance efficacy against infection risk.
Donor Considerations: Often utilize Expanded Criteria Donors (ECD).
Outcomes: Good quality of life achievable; higher risk of infection, cardiovascular events.

⭐ Despite immunosenescence potentially reducing acute rejection, elderly transplant recipients face increased mortality from infections and cardiovascular events.

Geriatric patient discusses transplant options

Transplantation in Special Populations - Viral Hurdles, Hopeful Horizons

HIV+ Recipients:
- Criteria: CD4 >200 cells/µL (some protocols >100), undetectable viral load (<50 copies/mL) for ≥6 months.
- HAART essential; watch for drug interactions (CNIs, mTOR inhibitors).
HIV+ Donors (e.g., HOPE Act principles):
- Permitted for HIV+ recipients under specific research protocols and consent.
Hepatitis B (HBV):
- Recipients: Lifelong antiviral prophylaxis (e.g., Entecavir/Tenofovir) ± HBIG post-transplant.
- HBcAb+ (core antibody positive) donors: Risk of de novo HBV in recipient; recipient requires prophylaxis.
Hepatitis C (HCV):
- Recipients: Direct-Acting Antivirals (DAAs) achieve Sustained Virologic Response (SVR) >95%. Treat pre or post-transplant. Untreated risks fibrosing cholestatic hepatitis.
- HCV NAT+ donors: Increasingly used for HCV+ recipients; also for HCV- if DAAs are assured post-transplant.

⭐ HIV+ patients on stable HAART with an undetectable viral load and adequate CD4 count (typically >200 cells/µL) have post-transplant outcomes comparable to HIV-negative recipients.

HCV-viremic kidney transplant outcomes

Transplantation in Special Populations - Fertile Futures, Careful Crafting

Pregnancy Post-Transplant:
- High-risk; requires multidisciplinary care.
- Optimal: 1-2 years post-transplant, stable graft, maintenance immunosuppression.
Immunosuppression (Pregnancy):
- AVOID: Mycophenolate (MMF/MPA) 📌 MMF = My Fetus Fails. Switch to Azathioprine (AZA) ≥6 weeks pre-conception.
- USE: Tacrolimus (preferred CNI), low-dose Prednisolone.
- CONTRAINDICATED: Sirolimus, Everolimus.
Risks:
- Maternal: Pre-eclampsia, gestational diabetes, infection, rejection.
- Fetal: Prematurity, IUGR.
Male Fertility: CNIs generally safe; Sirolimus/MMF may impair.
Breastfeeding: Generally not advised; specialist consultation.

⭐ Mycophenolate (MMF/MPA) is highly teratogenic; switch to Azathioprine ≥6 weeks before conception.

High‑Yield Points - ⚡ Biggest Takeaways

Pregnancy post-transplant is possible; avoid Mycophenolate Mofetil (MMF) and Sirolimus.

Elderly recipients face ↑ infection and ↑ malignancy risks; cardiac fitness is crucial.

Pediatric transplants risk growth issues and PTLD; non-adherence is a concern.

HIV+ patients can be transplanted with undetectable viral load and good CD4 counts.

HCV+ recipients can receive HCV+ organs; DAAs improve outcomes significantly.

ABO-incompatible & highly sensitized patients: Transplant possible with desensitization protocols (e.g., IVIG, Rituximab).

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