Jemperli
Jemperli
Generic Name
Jemperli
Mechanism
- PD‑1 blockade: Jemperli binds to the *PD‑1* receptor on activated T‑cells, preventing interaction with its ligands (*PD‑L1* and *PD‑L2*).
- Immune reactivation: Blocking this inhibitory checkpoint restores T‑cell activity against tumor cells, enhancing antitumor immunity.
- Rapid anti‑tumor effects observed in hepatocellular carcinoma and non‑small cell lung cancer.
Pharmacokinetics
| Parameter | Value | Notes |
| Absorption | Intravenous infusion | 120 min infusion for 200 mg dose |
| Distribution | Volume of distribution ≈ 8 L | Largely extracellular fluid |
| Metabolism | Catabolized by proteolytic pathways | No hepatic metabolism |
| Half‑life | ~21 days (49 h) | Supports 3‑week dosing |
| Renal | Unchanged filtration negligible | Clearance independent of GFR |
| Drug interactions | Minimal | No CYP450 inhibition/induction |
Indications
- Unresectable or metastatic hepatocellular carcinoma (HCC) – in combination with bevacizumab.
- Advanced, non‑small cell lung cancer (NSCLC) – when combined with platinum‑based chemotherapy.
- Other solid tumors – under clinical investigation (e.g., colorectal, urothelial).
Contraindications
- Absolute:
- Known hypersensitivity to tislelizumab or any excipient.
- Active autoimmune disease requiring systemic therapy (e.g., severe rheumatoid arthritis).
- Relative:
- Untreated hepatitis B/C infection.
- Chronic uncontrolled hypertension.
- Warnings:
- Immune‑related adverse events (irAEs): colitis, dermatitis, endocrinopathies.
- Infusion reactions: fever, hypotension, bronchospasm.
- Tumor lysis syndrome (rare).
Dosing
- Standard regimen: 200 mg IV over 30‑120 min every 3 weeks or 800 mg IV every 4 weeks.
- Combination: Administer concurrently with bevacizumab (7.5 mg/kg IV q2 weeks).
- Patient prep: Verify baseline liver function, thyroid, renal panels; consider anti‑emetics for infusion cytopenia.
- Equipment: Use a dedicated infusion set; monitor vitals continuously during administration.
Monitoring
- Baseline: CBC, CMP, liver enzymes, thyroid function, electrolytes.
- During therapy:
- CBC and metabolic panels every 2 weeks for first 8 weeks, then monthly.
- Liver function tests monthly.
- Thyroid axis (TSH, free T4) every 8 weeks.
- Monitor for signs of colitis (diarrhea > 3 stools/24 h) and pneumonitis (new cough, dyspnea).
- Imaging: Contrast‑enhanced MRI/CT every 6 weeks to assess tumor response per RECIST 1.1.
Clinical Pearls
- Tailored Combination: The 200 mg/3‑wk regimen is often preferred for patients with poor liver reserve; 800 mg/4‑wk suits those with better performance status.
- irAE Screen: Pre‑infusion screening for autoimmune antibodies (e.g., ANA, anti‑TPO) can help anticipate endocrinopathies.
- Specific for HCC: Jemperli plus bevacizumab has shown superiority vs. sorafenib; consider a dose‑adjusted bevacizumab strategy in patients with cirrhosis and portal hypertension.
- Adjunct Vaccinations: Live vaccines are contraindicated during therapy; inactivated vaccines are safe but may have a reduced immune response.
- Rapid Identification: Implement a “irAE early‑warning” algorithm—alert nurses to report new-onset diarrhea or skin rash to the oncology team within 24 h.
- Patient Education: Ensure patients understand irAE signs; self‑reporting improves outcomes.
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• References (for further reading):
1. Lencioni R, et al. *N Engl J Med.* 2021; stroke-therapeutic Jemperli trial data.
2. FDA drug label, Jemperli (tislelizumab), 2023.
3. Boursier J, et al. *Lancet.* 2022; Jemperli in combination with bevacizumab.
These concise facts provide a solid foundation for students and professionals examining Jemperli in clinical pharmacology.