Nursing Oncology

Nursing Pharmacology Chapter 33-34: Anticancer Drugs

Alkylating Agents:

Classification: Platinum Analogs:

Oxaliplatin (Eloxatin): Overview
- Oxaliplatin is a third-generation platinum analogue (diaminocyclohexene).³
  - However, with respect to mechanism of action and clinical pharmacology this agent appears identical to cisplatin and carboplatin.
  - Importantly, however, some tumors resistant to cisplatin or carboplatin, due to mismatch repair defects, do not show cross-resistance to oxaliplatin.
    - This finding may be the basis of the clinical observation that oxaliplatin exhibits activity in colorectal cancer.³
- Initial approval of oxaliplatin was as a second-line treatment in combination with 5-FU (fluoropyrimidine 5-fluorouracil) and leukovorin for metastatic colon cancer.³
  - This protocol was referred to as the FOLFOX regimen.³
    - In various formulations of FOLFOX, this intervention is a first-line treatment for advanced colorectal cancer.
      - The regimen is also important in stage III colon cancer in an adjuvant role as well as in high-risk stage II colon cancer.
      - Oxaliplatin exhibits clinical activity another gastrointestinal cancers such as pancreatic.
    - The primary dose-limiting toxicities neurotoxicity presenting as peripheral sensory neuropathy.³
      - The neurotoxicity presents both as an acute form which is worse and then triggered by cold exposure and a chronic form that appears dose-dependent.³
Mechanism of Action:
- Cisplatin (Platinol), as well as carboplatin and oxaliplatin initiate their cytotoxic activity by first entering cells by means of a high affinity Cu²⁺ CTR1 transporter.¹
  - Degraded transporter activity is associated with transporting these agents.
  - The compounds are extruded from cells by other copper transporters, in this case exporters.¹
    - Clinical resistance to the action of these platinum-based antineoplastic drugs depends in part on the expression level of these transporters.
  - Once inside the cell, specific ligands associated with the platinum drugs are displaced by water which results in a positively charged molecule, highly reactive with DNA and proteins.¹
    - Cisplatin is perhaps the most prominent organoplatinum anticancer agent.
  - Formation of DNA-platinum adducts inhibits both transcription and replication.¹
    - Adduct formation between DNA diguanosine dinucleotides and oxaliplatin appears structurally i.e. conformationally different from adducts formed with cisplatin or carboplatin. ⁷
    - These adducts induce single-and double-stranded breaks as well as miscoding.
    - If the adducts in DNA are so recognized by p53 and other checkpoint proteins, programmed cell death or apoptosis is induced.
  - Various platinum analogues are different with respect to adduct configuration and adduct effects on DNA structure and function.¹
    - For example, carboplatin (Paraplatin) and oxaliplatin (Eloxatin) form adducts more slowly compared to cisplatin.
Absorption, distribution, Metabolism Excretion:
- Oxaliplatin exhibits a relatively short t_1/2 in plasma (initial t_1/2is about 15 min.).¹
  - Both chemical reactivity and tissue uptake of oxaliplatin contribute to the short t1/2.¹
  - Oxaliplatin volume of distribution (V_d) is about 440 L.⁹
    - This drug is extensively protein-bound (>90%) mainly with albumin and gamma globulin.
    - Oxaliplatin is sensitive to rapid and extensive nonenzymatic metabolism which results in both inactive and active derivatives.
    - About 50% of the platinum is excreted in the urine (approximately 2%).⁹
Some Clinical Uses:
- Oxaliplatin exhibits antitumor activity including colorectal and gastric cancer which is different from other platinum drugs.
  - Effectiveness in colorectal cancer may be due to its MMR-and HMG-(Mismatch Repair; High Mobility Group) independent effects.
  - Oxaliplatin also suppresses thymidylate synthase (TS) which is the target enzyme of the antineoplastic agent 5-fluorouracil (5-FU).
  - Oxaliplatin in combination with 5-FU, has been approved for therapy of patients with colorectal cancer.

Adverse Effects:

Peripheral neuropathy represents the dose-limiting oxaliplatin toxic effect.¹

One form develops acutely, triggered by cold liquids, and presents as parasthesias and dysesthesias in the mouth, throat and upper and lower limbs.

The other manifestation develops with cumulative dose and exhibits features comparable to that observed with cisplatin neuropathology.

These features include a progressive sensory neurotoxicity including dysesthesias, extremity numbness and ataxia.

**Adjuvant treatment for colon cancer (Oxaliplatin and 5-FU (5-fluorouracil): How to treat a stage III colon cancer? (Reducing Neuropathic Toxicities)**

Attribution: Cervantes A Adjuvant treatment for colon cancer: How to treat a stage III colon cancer" https://www.youtube.com/watch?v=zjJiUS6sH64 ESMD (European Society for Medical Oncology) Youtube Channel: https://www.youtube.com/channel/UC7SPyIzaAkrzTS1hmQoa-1g

Oxaliplatin is associated with mild to moderate hematological toxicity with the exception of rare immune system mediated cytopenias.¹
In the long-term oxaliplatin administration may cause leukemia and pulmonary fibrosis in a time frame extending months to years after drug administration.

Acute allergic responses to oxaliplatin include hypotension, bronchoconstriction, and hives.¹

**"Reducing the neurotoxic side effects of adjuvant chemotherapy for colon cancer"⁹**

Attribution: Arkenau H-T Reducing the neurotoxic side effects of adjuvant chemotherapy for colon cancer. https://www.youtube.com/watch?v=QN5oZgZogss (6/2017) VJOncology Youtube Channel https://www.youtube.com/channel/UCn3u5oMgE00_qIex2IzGjYg

References
Wellstein A Giaccone G Atkins MB Sausville Chapter 66: Cytotoxic Drugs in Goodman & Gilman's: The Pharmacological Basis of Therapeutics, 13e, Brunton LL Hilal-Dandan R Knollmann BC, eds) 2018. Sausville EA Longo DL Chapter 103e Principles of Cancer Treatment, in Harrison's Online (Dennis L. Kasper, Anthony S. Fauci, Stephen L. Hauser, Dan L. Longo, J. Larry Jameson, Joseph Loscalzo, Eds.), Harrison's Principles of Internal Medicine, 19th edition, The McGraw-Hill Companies, Inc. 2015. Chu E Cancer Chemotherapy Chapter 54 in Basic & Clinical Pharmacology, 14 e (Katzung BG The McGraw-Hill Companies, 2018 (on-line edition) Tew KD Chapter 17: Alkylating Agents in Principles & Practice of Oncology (DeVita, JR VT Lawrence TS Rosenberg SA, eds) 10e Wolters Kluwer Health 2015. Collins JM Cancer Pharmacology Chapter 29 in Abeloff's Clinical Oncology (Niederhuber JE Armitage JO Doroshow JH Kastan MB Tepper JE, eds) 5e Elsevier Churchill Livingstone, Philadelphia, PA 2014. SEER Training Modules, National Cancer Institute, Types of Chemotherapy Drugs: Alkylating agents http://training.seer.cancer.gov/treatment/chemotherapy/types.html accessed April 10, 2016. Roche VF Cancer and Chemotherapy Chapter 37: Therapeutic Classes of Anticancer Drugs-Nitrogen Mustards and Aziridine-Mediated Alkylators. in Foye's Priniciples of Medicinal Chemistry (Lemke TL Williams DA, eds; associate eds, Roche VF Zito SW) 7e Lippinoctt, Williams & Wilkins, a Wolters Kluwer business, 2013. O'Dwyer PJ Calvert AH Chapter 18: Platinum Analogs in Principles & Practice of Oncology (DeVita, JR VT Lawrence TS Rosenberg SA, eds) 10e Wolters Kluwer Health 2015. Oxaliplatin Drugs.com (Access Medicine) Arkenau H-T Reducing the neurotoxic side effects of adjuvant chemotherapy for colon cancer. Published June 20, 2017 https://www.youtube.com/watch?v=QN5oZgZogss
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