Chemotherapy: How It Works, Side Effects, and What to Expect

Chemotherapy is the use of systemic drugs that kill rapidly dividing cells — including cancer cells — to treat malignancy. It remains one of the most widely used cancer treatments, both as a standalone modality and in combination with surgery, radiation, targeted therapy, and immunotherapy. Chemotherapy is fundamentally different from targeted therapy, which attacks specific molecular alterations driving a particular tumor’s growth. Chemotherapy, by contrast, acts broadly on all rapidly dividing cells — cancer cells divide faster than most normal cells, making them more vulnerable, but normal rapidly dividing tissues (bone marrow, gut epithelium, hair follicles) are also affected.

This guide covers what chemotherapy is, how each drug class disrupts cancer cell biology, which regimens are used for which cancers, how side effects are managed with modern supportive care, and what to expect during treatment. For a complete overview of all cancer treatment modalities, see the cancer treatment guide. For guidance on how to choose between chemotherapy and other options, see the cancer treatment options guide.

>90% Cure rate for Stage I–II testicular cancer with BEP chemotherapy (bleomycin + etoposide + cisplatin)

60–70% Cure rate for diffuse large B-cell lymphoma (DLBCL) with R-CHOP — one of oncology’s most effective regimens

10–14 days Nadir timing (lowest blood counts) after most chemotherapy cycles — the window of highest infection risk

31.3% vs. 17.4% 3-year overall survival: pembrolizumab + chemotherapy vs. chemotherapy alone for metastatic NSCLC (KEYNOTE-189)

How Chemotherapy Works — Drug Classes

Chemotherapy drugs disrupt cancer cell replication through several distinct mechanisms. Understanding these mechanisms helps explain both their effectiveness and their specific side effect profiles.

Alkylating Agents

Cross-link DNA strands → prevent replication. Non-cell-cycle-specific. Cisplatin, carboplatin, oxaliplatin, cyclophosphamide, temozolomide (TMZ for glioblastoma — activity predicted by MGMT methylation).

Antimetabolites

Block DNA building blocks. S-phase specific. 5-FU (TS inhibition; potentiated by leucovorin), capecitabine (oral 5-FU prodrug), pemetrexed (requires folic acid + B12 pre-medication), gemcitabine, methotrexate.

Anthracyclines

Intercalate DNA + inhibit topoisomerase II + generate ROS. Doxorubicin, epirubicin. Lifetime cumulative dose limit (doxorubicin ~500 mg/m²) due to irreversible cardiotoxicity. Backbone of R-CHOP and AC (breast).

Taxanes

Stabilize microtubules → G2/M arrest (opposite of vinca alkaloids). Paclitaxel (requires premedication for hypersensitivity), nab-paclitaxel (albumin-bound, no premedication), docetaxel. Key toxicity: cumulative peripheral neuropathy.

Vinca Alkaloids

Prevent microtubule polymerization → mitotic arrest. Vincristine (R-CHOP, ABVD; dose-limiting toxicity: neuropathy), vinblastine (ABVD for Hodgkin). Unlike taxanes — minimal myelosuppression with vincristine.

Topoisomerase Inhibitors

Irinotecan (topo I; FOLFIRI, FOLFIRINOX; UGT1A1*28 genotype → dose reduction), etoposide (topo II; BEP, carbo/etoposide in SCLC). S-phase active.

Key Mechanism Details

5-FU and leucovorin: 5-FU inhibits thymidylate synthase (TS), depleting thymidine for DNA synthesis. Leucovorin (folinic acid) stabilizes the 5-FU/TS inhibitory complex, making 5-FU significantly more effective — which is why FOLFOX, FOLFIRI, and FLOT always include leucovorin. Continuous IV infusion of 5-FU over 46 hours provides sustained TS inhibition superior to IV bolus. Capecitabine (Xeloda) is an oral prodrug converted to 5-FU preferentially within tumor tissue, allowing outpatient oral administration in place of IV infusion.

Temozolomide and MGMT: TMZ, the oral alkylator used in glioblastoma (Stupp protocol: concurrent RT + TMZ → adjuvant TMZ), methylates the O6 position of guanine. Tumors with MGMT promoter methylation cannot express the MGMT repair enzyme that reverses this damage — making them significantly more sensitive to TMZ. MGMT status is a key biomarker tested before glioblastoma treatment.

Irinotecan and UGT1A1: Irinotecan is metabolized to its active form SN-38 by the UGT1A1 enzyme. Patients with the UGT1A1*28 polymorphism (the Gilbert syndrome genotype, ~10% of the population) metabolize SN-38 more slowly — accumulation leads to severe diarrhea and neutropenia at standard doses. UGT1A1 genotyping is recommended before irinotecan at doses ≥250 mg/m². For more on how targeted therapies differ mechanistically from chemotherapy, see the targeted therapy guide.

Common Chemotherapy Regimens by Cancer Type

Cancer Type	Key Regimens	Evidence / Notes
Breast cancer (early)	AC-T; dose-dense AC-T; TC; TNBC + carboplatin or pembrolizumab	CALGB 9741: dose-dense AC-T improved DFS/OS vs. q3w; KEYNOTE-522: pembro + chemo for TNBC
Colorectal cancer	FOLFOX; FOLFIRI; XELOX/CAPOX; FOLFOXIRI	FOLFOX adjuvant Stage III colon; TRIBE trial: FOLFOXIRI superior ORR for conversion to resection
Lung cancer (NSCLC)	Carboplatin + pemetrexed + pembrolizumab; carbo + paclitaxel ± pembro; cisplatin + vinorelbine (adjuvant)	KEYNOTE-189: 3-yr OS 31.3% vs. 17.4% (chemo alone); LACE meta-analysis: 5.4% 5-yr OS benefit adjuvant
Small cell lung (SCLC)	Carboplatin + etoposide ± atezolizumab (IMpower133) or durvalumab (CASPIAN)	IMpower133: OS 12.3 vs. 10.3 months with atezolizumab added
DLBCL (lymphoma)	R-CHOP × 6 cycles	60–70% cure rate; Coiffier et al., NEJM 2002
Hodgkin lymphoma	ABVD; BV-AVD (advanced HL)	ECHELON-1: BV-AVD superior modified PFS and OS vs. ABVD for advanced HL
Testicular cancer	BEP (3–4 cycles) or EP	>90% cure Stage I-II; ~80% Stage III — among highest cure rates in metastatic solid tumors
Pancreatic cancer	FOLFIRINOX; gemcitabine + nab-paclitaxel	PRODIGE 4: FOLFIRINOX 11.1 vs. 6.8 months OS; MPACT: gem + nab-pac 8.5 vs. 6.7 months OS
Gastric cancer	FLOT (perioperative); XELOX + nivolumab (metastatic)	FLOT4: 45% vs. 36% 5-yr OS; CHECKMATE-649: superior OS for nivolumab + chemo (CPS ≥5)
Ovarian cancer	Carboplatin + paclitaxel × 6; olaparib maintenance (BRCA1/2-mutated)	SOLO1: 60.4 months PFS with olaparib vs. 13.8 months placebo

The Chemotherapy Cycle — What Happens

A chemotherapy cycle is a scheduled treatment period followed by a recovery period, repeated until the planned number of cycles is complete. Recovery time allows the bone marrow to replenish blood cells before the next cycle — cancer cells, which repair less efficiently, have less opportunity to recover.

Common cycle lengths:

Every 2 weeks (q2w): FOLFOX, FOLFIRI, FOLFIRINOX (treatment day + 46h 5-FU pump = 3 days, then 11 days off)
Every 3 weeks (q3w): AC (breast cancer), BEP (testicular), carboplatin/paclitaxel
Every 4 weeks: Many oral regimens (capecitabine: 14 days on, 7 days off)

What happens at each cycle visit:

Pre-cycle bloodwork: CBC (ANC ≥1,500/μL required; platelets ≥100,000/μL); CMP (creatinine for carboplatin Calvert formula: Dose mg = Target AUC × [CrCl + 25]; bilirubin for irinotecan risk)
Nursing assessment: Weight, symptom review, performance status
Pre-medications: Antiemetics before chemotherapy starts; dexamethasone + antihistamine for taxane hypersensitivity prevention; G-CSF counseling
Chemotherapy infused: Via peripheral vein, PICC line, or implanted port (port preferred for multi-cycle regimens — preserves peripheral veins)
5-FU pump (if applicable): Patient goes home with a portable pump; 46-hour continuous 5-FU infusion; pump disconnected at day 3

The nadir: Blood counts reach their lowest point — the nadir — approximately 10–14 days after chemotherapy for most agents (carboplatin nadir: ~21 days). This is the window of highest infection risk. Patients should check their temperature daily during the nadir and know clearly: fever ≥38.3°C (100.4°F) = go to the ER immediately. For a comprehensive list of questions to ask your team before starting chemotherapy, see the cancer diagnosis questions guide.

chemotherapy blood test CBC monitoring nadir — Blood tests before each chemotherapy cycle confirm white blood cell and platelet counts are safe to proceed.

Managing Chemotherapy Side Effects

Myelosuppression and Febrile Neutropenia

Febrile Neutropenia = Medical Emergency

Fever ≥38.3°C (100.4°F) during the nadir window (days 7–14 after chemotherapy) requires immediate emergency department evaluation. IV antibiotics must begin within 60 minutes of triage. Do not wait — untreated febrile neutropenia can progress to sepsis within hours.

Chemotherapy suppresses the bone marrow’s production of all blood cells:

Neutropenia: ANC nadir 10–14 days post-treatment; febrile neutropenia (FN) occurs when ANC <500/μL + fever ≥38.3°C
Thrombocytopenia: Most pronounced with carboplatin and oxaliplatin; platelet transfusion threshold typically <10,000/μL
Anemia: Iron supplementation if iron-deficient; transfusion for symptomatic severe anemia

G-CSF (Granulocyte Colony-Stimulating Factor) prevents FN by stimulating neutrophil production from bone marrow:

Filgrastim (Neupogen): Daily subcutaneous injections, started 24–72 hours after chemotherapy completion
Pegfilgrastim (Neulasta): Single injection per cycle — equivalent efficacy; preferred for dose-dense every-2-week regimens

G-CSF is required when FN risk ≥20% (dose-dense AC-T, FOLFOXIRI, ABVD in elderly) and strongly considered for 10–20% risk with patient risk factors (age >65, PS ≥2, prior FN, no previous G-CSF).

Nausea and Vomiting (CINV)

CINV is the most feared chemotherapy side effect — and now the most reliably prevented with modern antiemetics. The key rule: take antiemetics before chemotherapy starts, not after nausea begins.

Emetogenic Category	Examples	Required Antiemetics
Highly emetogenic (HEC, ≥90%)	Cisplatin, AC-based regimens, FOLFIRINOX	NK1 RA (aprepitant) + 5-HT3 RA (palonosetron) + dexamethasone + olanzapine (for delayed)
Moderately emetogenic (MEC, 30–90%)	Carboplatin, oxaliplatin, irinotecan, doxorubicin, cyclophosphamide	5-HT3 RA (palonosetron preferred) + dexamethasone ± NK1 RA
Low emetogenic (10–30%)	Taxanes, pemetrexed, gemcitabine, etoposide, 5-FU	Single agent (dexamethasone or prochlorperazine)
Minimal (<10%)	Vincristine, bleomycin, capecitabine	As needed only

Olanzapine 10 mg added to standard antiemetic regimens for HEC significantly improves complete CINV control — endorsed by MASCC/ESMO guidelines. Palonosetron (second-generation 5-HT3 receptor antagonist with 40-hour half-life) is preferred over first-generation agents (ondansetron, granisetron) for both acute and delayed CINV prevention.

Peripheral Neuropathy

Oxaliplatin: Causes acute cold-related dysesthesia — tingling in fingertips and throat triggered by cold exposure (ice, cold drinks, cold surfaces) lasting ~1 week after each infusion. Patients must avoid cold during this window. Cumulative sensorimotor neuropathy develops with successive cycles and may persist after treatment ends.
Paclitaxel: Cumulative distal sensory neuropathy — numbness and tingling beginning in fingertips and toes, progressing proximally with each cycle. May be dose-limiting.
Vincristine: Peripheral and autonomic neuropathy (constipation, foot drop); does not cause myelosuppression.

Management: Dose reduction is the primary intervention. Duloxetine (SNRI antidepressant) has ASCO-endorsed moderate evidence for established oxaliplatin or paclitaxel neuropathy — the only pharmacologic intervention with randomized trial support (Smith EM et al., JAMA 2013).

Additional Side Effects

Alopecia: Expected with anthracyclines, taxanes, irinotecan, and cyclophosphamide — hair loss typically begins 2–3 weeks after the first cycle. Scalp cooling (DigniCap, Paxman — FDA-cleared) reduces alopecia in 50–66% of breast cancer patients receiving taxane-based therapy. Not appropriate for hematologic malignancies.

Mucositis: Painful mouth sores and GI inflammation with 5-FU-based regimens, high-dose methotrexate, and cytarabine. Prevention: meticulous oral hygiene, avoidance of alcohol-containing mouthwash, and palifermin (approved for mucositis in hematologic malignancy high-dose regimens).

Cardiotoxicity (anthracyclines): Baseline ECHO or MUGA scan required; monitor during treatment at cumulative dose thresholds (doxorubicin ~250 mg/m², ~400 mg/m²). Avoid concurrent anthracycline + trastuzumab — dramatically increased cardiotoxicity risk.

Cisplatin nephrotoxicity: Dose-dependent renal tubular damage; requires aggressive pre-hydration (1–2L IV saline + mannitol before and after). Carboplatin (dosed by Calvert formula based on renal function) is far less nephrotoxic and preferred when eGFR is borderline.

Hemorrhagic cystitis (ifosfamide, high-dose cyclophosphamide): Caused by acrolein metabolite; MESNA uroprotection is mandatory with each ifosfamide dose.

Oral Chemotherapy: Same Precautions Apply

Capecitabine (Xeloda) and temozolomide are chemotherapy drugs dispensed as pills — not “just oral medications.” They carry the same risks of myelosuppression, CINV, hand-foot syndrome (capecitabine), and nadir-related infection risk as intravenous chemotherapy. The same blood count monitoring, antiemetic use, and fever vigilance are required.

Bloodwork and Monitoring During Chemotherapy

Standard labs before each cycle confirm it is safe to proceed:

CBC with differential: ANC ≥1,500/μL; platelets ≥100,000/μL; hemoglobin for transfusion threshold
Creatinine/eGFR: Critical for carboplatin Calvert formula dosing; cisplatin typically avoided if eGFR <50 mL/min
LFTs and bilirubin: Elevated bilirubin signals reduced irinotecan metabolism → SN-38 accumulation → dose reduction required
Magnesium: Cisplatin causes renal magnesium wasting; monitor and replace to prevent hypomagnesemia-related arrhythmias
UGT1A1 genotype: Before high-dose irinotecan; *28/*28 homozygotes require dose reduction
Cardiac monitoring: Baseline ECHO before anthracyclines; repeat at cumulative dose thresholds

Understanding cancer stage is prerequisite to most chemotherapy decisions — stage determines intent (curative vs. palliative), regimen intensity, and planned number of cycles. According to the NCCN Patient Guidelines, chemotherapy regimen selection should be reviewed by a multidisciplinary oncology team including medical oncologist, pharmacist, and oncology nurse coordinator.

Frequently Asked Questions

What is chemotherapy and how does it work?

Chemotherapy is the use of systemic drugs that kill rapidly dividing cells — primarily cancer cells, but also normal rapidly dividing tissues including bone marrow, gut epithelium, and hair follicles. Different drug classes disrupt different steps: alkylating agents (cisplatin, cyclophosphamide) form crosslinks that prevent DNA from being copied; antimetabolites (5-FU, pemetrexed) block the building blocks needed for DNA synthesis; anthracyclines (doxorubicin) intercalate into DNA and inhibit topoisomerase II; taxanes (paclitaxel) stabilize microtubules to arrest cell division in G2/M. According to the NCI, chemotherapy may be given to cure cancer, control growth, relieve symptoms, or sensitize tumors to radiation — and the goal affects which regimen and schedule is chosen.

What is the difference between chemotherapy and targeted therapy?

Chemotherapy kills all rapidly dividing cells — cancer cells and normal rapidly dividing tissues alike. Targeted therapy attacks specific molecular targets present in cancer cells — EGFR mutations, HER2 amplification, BCR-ABL fusion, BRAF V600E — causing far less damage to normal cells that don’t carry those alterations. Side effect profiles differ substantially: targeted therapies cause rash, diarrhea, and organ-specific toxicities; chemotherapy causes myelosuppression, nausea, alopecia, and neuropathy. Many regimens combine both: KEYNOTE-189 uses carboplatin + pemetrexed (chemotherapy) with pembrolizumab (immunotherapy) for NSCLC. See the targeted therapy guide for a detailed comparison of mechanisms and applications.

What is a chemotherapy cycle and how long does treatment last?

A chemotherapy cycle is a scheduled treatment period followed by a recovery period, allowing the bone marrow to replenish blood cells before the next course. Cycle length varies: FOLFOX and FOLFIRI cycles are 14 days; most anthracycline-based regimens (AC, R-CHOP) are 21 days; capecitabine is typically 28-day cycles. Total treatment duration ranges widely: 4 cycles of AC-T for breast cancer takes about 12 weeks; 6 cycles of R-CHOP takes about 18 weeks; adjuvant FOLFOX for colon cancer (12 cycles) takes 6 months. Metastatic disease may involve continuous cycling until disease progression or unacceptable toxicity. FOLFOX patients receive a portable 5-FU pump for 46 hours after each clinic visit — treatment continues at home.

What side effects does chemotherapy cause?

Side effects depend on the specific drugs used. The most common across many regimens are myelosuppression (low blood counts — the most serious manifestation is febrile neutropenia), nausea and vomiting (now largely preventable with modern antiemetics), fatigue, and alopecia (hair loss with anthracyclines and taxanes). Specific toxicities by drug: oxaliplatin → peripheral neuropathy and cold dysesthesia; cisplatin → nephrotoxicity (requires IV hydration); doxorubicin → cumulative cardiotoxicity (lifetime dose limit); ifosfamide → hemorrhagic cystitis (requires MESNA); bleomycin → pulmonary fibrosis (lung function monitoring required). According to the American Cancer Society, most chemotherapy side effects are temporary and resolve after treatment ends, though neuropathy and cardiotoxicity may persist.

What is febrile neutropenia and why is it a medical emergency?

Febrile neutropenia (FN) occurs when chemotherapy has suppressed neutrophil production enough that the ANC drops below 500/μL AND the patient develops a fever ≥38.3°C (100.4°F). At this neutrophil level, the immune system cannot fight bacterial infection effectively — without rapid IV antibiotics, patients can develop sepsis and die within hours. FN requires immediate emergency department evaluation; IV antibiotics must begin within 60 minutes of triage. The nadir window — typically days 7–14 after chemotherapy — is when patients must check their temperature daily and have a clear instruction: fever during the nadir = go directly to the ER. Do not wait for the fever to resolve on its own, and do not take acetaminophen to mask it before being evaluated.

Can chemotherapy cure cancer?

Yes — in several cancer types, chemotherapy achieves cure, particularly with curative-intent regimens. The most dramatic examples: BEP chemotherapy (bleomycin + etoposide + cisplatin) cures >90% of Stage I–II testicular germ cell tumors; R-CHOP cures 60–70% of patients with diffuse large B-cell lymphoma; ABVD cures approximately 80% of Hodgkin lymphoma. Childhood ALL has a >90% cure rate with modern intensive chemotherapy. For many solid tumors (colon, lung, breast), chemotherapy is given adjuvantly after surgery to reduce recurrence risk, improving the probability that the surgery was curative. In metastatic solid tumors, chemotherapy generally controls disease and extends survival rather than achieving cure — with notable exceptions like testicular cancer and Hodgkin lymphoma at any stage.

National Cancer Institute — Chemotherapy to Treat Cancer
American Cancer Society — Chemotherapy for Cancer
Chemocare.com — Patient Drug Information
Conroy T et al. — PRODIGE 4 (FOLFIRINOX vs. gemcitabine in pancreatic cancer); NEJM 2011
Gandhi L et al. — KEYNOTE-189 (pembrolizumab + chemo for NSCLC); NEJM 2018
Citron ML et al. — CALGB 9741 (dose-dense AC-T); JCO 2003
Coiffier B et al. — R-CHOP for DLBCL; NEJM 2002
Connors JM et al. — ECHELON-1 (BV-AVD vs. ABVD in advanced HL); NEJM 2018
Smith EM et al. — Duloxetine for chemotherapy-induced neuropathy; JAMA 2013
Moore K et al. — SOLO1 (olaparib maintenance in ovarian cancer); NEJM 2018

This article is for educational purposes only and does not constitute medical advice. Discuss all chemotherapy decisions with your oncology care team.