MANAGEMENT OF CHEMOTHERAPY INDUCED NAUSEA AND VOMITING

1. MANAGEMENT OF CHEMOTHERAPY INDUCED NAUSEA AND VOMITING

3. Aim-complete control of N/V • MULTIDISPLINARY MGT • GENERAL CONSIDERATIONS-R/o Medical causes,Adequate Hydration, Correct Metab disturb,Diet, Anxiety • Appropriate Pharm Intervention • Patient Support,Educatn,Tech Expertise • Behavioural/Psychotherapeutic interventn. • Emetic Classif-High’ Intermediate and Low

4. Surgical / Other Mgt • Thermal Ablation of Area Pastrema-CTZ • Use of Bioband and Relband • Use of Acupuncture • Psychotherapeutic Intervention-Hypnosis, Mind diversion,Systemic desensitization

5. Pharmacological mgt • Most common intervention in CINV. • Based on Neurochemical control of Vom. • MOA-Competitive blockade of Receptors; Serotonin-5HT3,Dopamine-D2,Histamine H1,H2,Opoids,Acetylcholine,Substance P –NK1(Neurokinin type 1) • Mainstay of CINV prevention • Single or Combination Therapy

6. Phenothiazines-1950 • MOA= #Dopamine D2 R[CTZ,CNS,?PNS] • Aliphatic P-Chlorpromazine,Methotrimeprazine. >Autonomic/Anticholin Effects • Piperazine P- >Antiemetic Axn Prochlorperazine,Fluphenazine,Perphenazine. >Extrapyramidal Rxn[dystonia etc] • Prochlorp-10-15%,limited role.

7. Butyrophenones –Haloperidol/Droperidol • D2 R Antagonist. • Struct and Pharm similar PTZ • Superior to PTZ • ADR –Sedation, Extrap Rxn

8. Corticosteroids-Dexamethasone/ Methylprednisolone • MOA- ? # Brain Prostaglandin synthesis • Low and Interm emetogenic regimen • ADR –Euphoria,insomnia,Fluid retention

9. Cannabinoids;-Levonantradol Tetrahydrocannabinol, Nabilone. • MOA = ? CNS depression • Limited to oral admin • ADR -Sedation, Orth Hypotention,Ataxia • Superior to Ptz,low dose Metoc and Halop • Synthetics for investig use only

10. Substituted Benzamides-Metoclopramide • MOA -D2 R Antagonist CNS • -5HT3 R Antagonist[weak] • -Periph Axn >Gastric Emptying and direct smooth msl and cholinomimetic axn • Most effective against Acute vomiting. • High dose>40% Efficacy. Cheap • ADR–Sedation,Diarrhoea,Extrapyram Rxn

11. Benzodiazepines-Diazepam/Lorazepam • MOA-Anxiolytic,Sedative, Amnesic CNS effect • Major use=Adjunct to other antiemetics • Prev/Treat of ANV and Anxiety • ADR –Sedation,Amnesia,Hypotention

12. Antihistamines-[H1H2] Promethazine,Chlorpheniramine • Effective for Vestibular mediated N/V • No effect on CINV • Prevents Extrapyramidal Rxn of Antiemetics • ADR –Sedation, Anticholinergic effects

13. 5HT3[5 Hydroxytryptamine type 3] /Serotonin Rec Antagonists- • Granisetron,Ondansetron,Dolasetron,Tropisetron. • MOA-# 5HT3 R Centrally and Peripherally • 40-60%. Most Effective single agent • For Highly Emetogenic Chemotherapy • ADR –Headache,Transaminase elevat • Expensive,??Delayed emesis

14. Substance P Antagonist-NK1 R [Neurokinin] Aprepitant[Emend] • MOA- # NK I R in CNS • Especially Acute/Delayed Emesis • 5HT3 Ant + CORTIC + Aprep DOC –A Em • MISCELLANEOUS AGENTS= ACTH,BARBITURATES,SCOPOLAMINE,DOMPERIDONE .

15. Combination Therapy • Standard of care for control of CINV • MOA –Several sites and MOA • High therapeutic index >75%. < Drug ADR • D2 R Ant + Corticost/ + Benzodiaz • 5HT3 R Ant + Corticost + NKI R Ant • 5HT3 R Ant + Corticosteroid • Route,Dose and Schedule=Antiem Select

16. Acute and Delayed Emesis • Patient Counseling • Prophylactic Combination Antiemetic therapy. High to Moderate Emetogenic drug • Continue Antiemetics for 4-7days after

17. Anticipatory N/V • Refractory to std antiemetics • Best approach –Prevention using pharm agent from initiation of Chemotherapy • Benzodiazepine[Lorazepam] -Prevention • Psychotherapy –Hypnosis,Mind diversion,Systemic desensitization

18. Conclusion • Prevention and control of N/V are paramount in the treatment of cancer patients b/c of the various complication and withdrawal from useful and curative antineoplastic treatment.

19. STOP NAUSEA AND VOMITING! • THANK YOU