Chemo Basics - Drug Dueling Cancers
- Primary Goal: Cytotoxic (kill) or cytostatic (halt growth) effects on cancer cells.
- Drug Categories:
- Cell Cycle Specific (CCS): Act on specific phases (e.g., S-phase: Antimetabolites; M-phase: Vincas, Taxanes).
- Cell Cycle Non-Specific (CCNS): Effective in all phases, including G0 (e.g., Alkylating agents).
- Therapeutic Intent:
- Adjuvant: Post-surgery/RT to eliminate micrometastases.
- Neoadjuvant: Pre-surgery/RT to shrink tumor.
- Combination Regimens: Standard to maximize kill, minimize resistance.
⭐ Most chemotherapy drugs target rapidly dividing cells, leading to common side effects like myelosuppression, mucositis, and alopecia.
Key Chemo Drugs - H&N Hitmen
- Platinum Agents: Crucial for H&N cancers.
- Cisplatin: Forms DNA cross-links. Toxicities: Severe Nausea/Vomiting, Nephrotoxicity (📌 Amifostine), Ototoxicity, Neuropathy.
- Carboplatin: DNA cross-links. Toxicities: Myelosuppression (dose-limiting), less nephro/ototoxic. Calvert formula.
- Antimetabolites:
- 5-Fluorouracil (5-FU): Inhibits thymidylate synthase $\rightarrow$ ↓DNA. Toxicities: Mucositis, Diarrhea, Myelosuppression.
- Methotrexate (MTX): DHFR inhibitor. Toxicities: Mucositis, Myelosuppression, Hepatotoxicity. (📌 Leucovorin rescue).
- Taxanes (Paclitaxel, Docetaxel):
- MOA: Stabilize microtubules $\rightarrow$ mitotic arrest.
- Toxicities: Myelosuppression, Neuropathy, Hypersensitivity.
- Targeted Therapy:
- Cetuximab: EGFR mAb. Toxicities: Acneiform rash, Hypomagnesemia, Infusion reactions.
⭐ Acneiform rash with Cetuximab often correlates with better treatment response.
- Cetuximab: EGFR mAb. Toxicities: Acneiform rash, Hypomagnesemia, Infusion reactions.
Targeted Therapy Intro - Precision Payloads
- Drugs engineered to interfere with specific molecules ("targets") vital for cancer cell growth & survival.
- Deliver "precision payloads" by selectively targeting cancer cells, reducing harm to normal tissues.
- Major classes:
- Monoclonal Antibodies (MAbs): Large proteins; bind extracellular targets (e.g., EGFR - Cetuximab). Suffix: "-mab".
- Small Molecule Inhibitors (TKIs): Oral; enter cells, block intracellular targets (e.g., BCR-ABL - Imatinib). Suffix: "-nib".

⭐ Biomarker testing (companion diagnostics) is often mandatory to identify patients benefiting from specific targeted therapies.
Star Targeted Agents - EGFR & Immune Boosters
-
EGFR Inhibitors:
- Cetuximab: mAb vs EGFR.
- Uses: LA HNSCC (w/ RT); R/M HNSCC (w/ chemo/alone).
- SEs: Acneiform rash (predicts response; 📌 C-rash = C-benefit), hypomagnesemia, infusion rxns.
- TKIs (Gefitinib, Erlotinib): Minor role HNSCC.
- Cetuximab: mAb vs EGFR.
-
Immune Checkpoint Inhibitors (ICIs) - "Immune Boosters":
- PD-1 Inhibitors: Nivolumab, Pembrolizumab.
- Mech: Blocks T-cell PD-1 → ↑anti-tumor activity.
- Uses: R/M HNSCC (post-platinum, or 1st line [Pembrolizumab +/- chemo for PD-L1+]).
- PD-L1 Inhibitors: Atezolizumab, Durvalumab.
- SEs (irAEs): Skin, gut, liver, lung, endocrine toxicities.
- PD-1 Inhibitors: Nivolumab, Pembrolizumab.
⭐ Pembrolizumab: 1st-line for metastatic/unresectable recurrent HNSCC if PD-L1 CPS ≥ 1 (alone/with chemo).
Regimens & Resistance - Combo Combat & Defenses
- Key Regimens:
- Induction (LA-SCCHN): TPF (Docetaxel, Cisplatin, 5-Fluorouracil) improves outcomes.
- Concurrent (CCRT): High-dose Cisplatin (100 mg/m² every 3 weeks) is standard with RT.
- Resistance Mechanisms:
- Drug efflux (e.g., MDR1/P-gp), target gene mutations, enhanced DNA repair, altered drug metabolism.
- Combat Strategies:
- Combination chemotherapy, sequential therapies, novel targeted agents.
⭐ Acquired resistance to Cisplatin often involves increased cellular detoxification via glutathione conjugation or enhanced DNA repair pathways like NER.
High‑Yield Points - ⚡ Biggest Takeaways
- Cisplatin is a cornerstone for HNSCC chemoradiation; key toxicities include nephrotoxicity and ototoxicity.
- Induction chemotherapy (e.g., TPF regimen) is used for locally advanced HNSCC to improve outcomes.
- Cetuximab (EGFR inhibitor) is crucial for HNSCC, especially HPV-negative cases; characteristic acneiform rash.
- Immunotherapy (e.g., Pembrolizumab, Nivolumab) is vital for recurrent or metastatic HNSCC.
- 5-Fluorouracil (5-FU) is often combined with cisplatin for synergistic antitumour activity in HNSCC.
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