---
name: managing-chemotherapy-toxicity
language: en
description: Grades treatment toxicity using CTCAE v5.0 with dose modification and supportive care protocols. Use when grading chemo toxicity, applying CTCAE criteria, or managing treatment side effects.
tags:
  - management
  - oncology
  - treatment
metadata:
  author: casemark
  practice_areas:
    - Medical Oncology
    - Hematology-Oncology
    - Radiation Oncology
  document_types:
    - Management Report
  skill_modes:
    - Management
    - Coordination
---

# Managing Chemotherapy Toxicity

Grades treatment toxicity using CTCAE v5.0 with dose modification and supportive care protocols.

## Why This Skill Exists

Chemotherapy toxicity is the leading cause of treatment delays, dose reductions, and treatment discontinuation in oncology. The Common Terminology Criteria for Adverse Events (CTCAE) v5.0, published by NCI, is the universal grading system used across clinical practice, clinical trials, and quality reporting. Incorrect grading leads to inappropriate dose modifications — undergrating risks life-threatening toxicity continuation; overgrading results in unnecessary dose reductions that compromise efficacy.

ASCO/ONS Chemotherapy Administration Safety Standards require standardized toxicity assessment and documentation at every treatment cycle. QOPI measures track toxicity-related hospitalizations and emergency department visits. FDA post-marketing safety reporting (MedWatch) depends on accurate CTCAE grading. Institutions participating in NCI-sponsored clinical trials must grade adverse events per CTCAE to maintain protocol compliance and data integrity.

---

## Checkpoint A: Pre-Draft Intake (Mandatory)

1. What chemotherapy regimen is the patient receiving (specific agents, doses, schedule)? (Default: [VERIFY])
2. What cycle and day is the patient currently on? (Default: specify)
3. What specific adverse event(s) are being graded? (Default: list all active toxicities)
4. What were the baseline organ function values prior to treatment initiation? (Default: review baseline labs)
5. What is the patient's current ECOG performance status? (Default: last documented)
6. Has the patient experienced this toxicity in prior cycles? If yes, what was the prior grade and action taken? (Default: no prior episodes)
7. What supportive care medications are currently prescribed? (Default: document current regimen)
8. Is the patient on a clinical trial with protocol-specific dose modification rules? (Default: no)

### Documents to Request

- CTCAE v5.0 reference for the specific adverse event term
- Current and prior cycle lab results (CBC with differential, CMP, LFTs)
- Regimen-specific dose modification tables from the protocol or NCCN guidelines
- Nursing flow sheets with vital signs and symptom documentation
- Prior toxicity grading documentation from previous cycles
- Supportive care medication list with doses and schedule
- Relevant imaging if toxicity involves organ damage (e.g., chest CT for pneumonitis)
- Clinical trial protocol dose modification section if applicable

---

## Step 1: Grade the Adverse Event Using CTCAE v5.0

CTCAE v5.0 grades adverse events on a 1–5 scale:

| Grade | Severity | General Definition |
|-------|----------|-------------------|
| 1 | Mild | Asymptomatic or mild symptoms; clinical or diagnostic observations only; no intervention indicated |
| 2 | Moderate | Minimal, local, or noninvasive intervention indicated; limiting age-appropriate instrumental ADL |
| 3 | Severe | Severe or medically significant but not immediately life-threatening; hospitalization or prolongation of hospitalization indicated; disabling; limiting self-care ADL |
| 4 | Life-threatening | Life-threatening consequences; urgent intervention indicated |
| 5 | Death | Death related to adverse event |

**Critical grading examples for common toxicities:**

- **Neutropenia:** Grade 1 (ANC <LLN–1500), Grade 2 (1000–1500), Grade 3 (500–1000), Grade 4 (<500)
- **Thrombocytopenia:** Grade 1 (75,000–LLN), Grade 2 (50,000–75,000), Grade 3 (25,000–50,000), Grade 4 (<25,000)
- **Nausea:** Grade 1 (loss of appetite, intake preserved), Grade 2 (decreased oral intake), Grade 3 (inadequate caloric/fluid intake, hospitalization)
- **Peripheral neuropathy:** Grade 1 (asymptomatic, reflexes decreased), Grade 2 (moderate symptoms, limiting instrumental ADL), Grade 3 (severe, limiting self-care ADL)
- **Diarrhea:** Grade 1 (increase 4 stools/day over baseline), Grade 2 (increase 4–6 stools/day), Grade 3 (increase ≥7 stools/day, hospitalization), Grade 4 (life-threatening, urgent intervention)

Use the exact CTCAE v5.0 term — do not paraphrase or use institutional shorthand.

---

## Step 2: Apply Dose Modification Rules

Standard dose modification framework (apply protocol-specific rules when available):

| Toxicity Grade | Standard Action |
|---------------|----------------|
| Grade 1 | Continue current dose; increase monitoring frequency |
| Grade 2 | Consider dose reduction (typically one level, 25% reduction); hold until Grade ≤1 for certain toxicities |
| Grade 3 | Hold treatment until Grade ≤1; resume at reduced dose (one or two dose levels); discontinue the offending agent for specific toxicities (e.g., Grade 3 peripheral neuropathy from platinum) |
| Grade 4 | Hold treatment; consider permanent discontinuation of offending agent; resume only after resolution and at reduced dose with documented clinical justification |

**Agent-specific dose modification highlights:**
- Capecitabine: reduce to 75% for Grade 2 hand-foot syndrome, hold for Grade 3
- Cisplatin: hold for CrCl <60 mL/min; no dose reduction — discontinue and substitute carboplatin if nephrotoxicity persists
- Anthracyclines: monitor cumulative dose (doxorubicin max 450–550 mg/m²); hold for LVEF drop >15% from baseline or LVEF <45%
- Taxanes: hold for ANC <1500; reduce one dose level for Grade 3 neuropathy

---

## Step 3: Implement Supportive Care Interventions

**Hematologic toxicity management:**
- G-CSF (filgrastim, pegfilgrastim) for febrile neutropenia risk >20% or secondary prophylaxis after prior febrile neutropenia episode
- Platelet transfusion threshold: <10,000 for prophylaxis, <50,000 for active bleeding or procedures
- Erythropoiesis-stimulating agents (ESAs) only for chemotherapy-induced anemia with Hgb <10, palliative intent

**Gastrointestinal toxicity management:**
- Antiemetic regimen per NCCN emetogenic risk (high: NK1 antagonist + 5-HT3 + dexamethasone ± olanzapine; moderate: 5-HT3 + dexamethasone; low: dexamethasone or 5-HT3 alone)
- Loperamide for uncomplicated diarrhea; octreotide for Grade 3–4 or persistent diarrhea
- Mucositis: cryotherapy during bolus 5-FU; palifermin for autologous SCT conditioning with TBI

**Neurotoxicity management:**
- Duloxetine for established chemotherapy-induced peripheral neuropathy (CIPN) — the only agent with ASCO Level 1 evidence
- Dose modification is the primary prevention strategy for CIPN
- No evidence supports calcium/magnesium infusions for oxaliplatin CIPN prevention

---

## Step 4: Document and Communicate Toxicity Management Decisions

For each graded adverse event, document:
1. CTCAE v5.0 term and grade
2. Date of onset and current status (improving, stable, worsening)
3. Relationship to treatment (definite, probable, possible, unlikely)
4. Action taken (dose held, reduced, discontinued, supportive care added)
5. New dose level if modified (document in mg/m² and absolute dose)
6. Plan for reassessment prior to next cycle
7. Communication to referring providers and primary care

---

## Checkpoint B: Post-Draft Alignment (Mandatory)

1. Is each adverse event graded using the exact CTCAE v5.0 term and grade definition?
2. Do dose modifications follow protocol-specific rules (or standard guidelines if no protocol)?
3. Is supportive care aligned with NCCN supportive care guidelines for the specific toxicity?
4. Are cumulative dose limits tracked for agents with lifetime maximums (anthracyclines, bleomycin)?
5. Is the plan for next-cycle reassessment clearly documented?

---

## Quality Audit

- [ ] CTCAE v5.0 version explicitly referenced (not v4.03 or earlier)
- [ ] Each adverse event uses the correct MedDRA preferred term from CTCAE
- [ ] Grade assignment matches the v5.0 grading criteria verbatim
- [ ] Dose modification level documented in both percentage and absolute dose
- [ ] Baseline values available for comparison (labs, imaging, symptoms)
- [ ] G-CSF use aligned with NCCN Hematopoietic Growth Factors guideline
- [ ] Antiemetic regimen matches NCCN Antiemesis emetogenic risk category
- [ ] Cumulative anthracycline dose tracked against maximum
- [ ] Attribution (relationship to treatment) documented for each event
- [ ] Clinical trial protocol-specific rules applied when applicable
- [ ] Patient education on expected toxicities documented
- [ ] Communication with referring providers documented
- [ ] Follow-up plan and timeline for reassessment specified

---

## Guidelines

- Use CTCAE v5.0 exactly — grading definitions changed between v4.03 and v5.0 for several common terms
- Grade at the worst severity within the reporting period, not at the time of assessment
- Never reduce dose for Grade 1 toxicity unless protocol-specifically mandated
- Febrile neutropenia (ANC <500 + fever ≥38.3°C single or ≥38.0°C sustained) is always at minimum Grade 3 and requires immediate intervention
- Dose re-escalation after reduction is generally not recommended — maintain reduced dose for subsequent cycles
- Track total number of dose reductions; more than two reductions for the same toxicity typically warrants regimen change discussion
- Document patient-reported outcomes alongside clinician-graded CTCAE — they frequently diverge
- Immune-related adverse events from checkpoint inhibitors use CTCAE grading but require separate management algorithms (see managing-immunotherapy-protocols skill)