12/23/2016 Antibiotic Update Prepared by: Leany Capote University of Miami Health System PGY-1 January 2017 Goals and Objectives Discuss the mechanism of action, pharmacodynamics, and pharmacokinetics of novel antibiotics Summarize FDA-approved indications for these novel antibiotics Compare and contrast these novel antibiotics and traditional agents Abbreviations  ESKAPE: Enterobacter  VABP: Ventilator Associated species, Klebsiella, Bacterial Pneumonia Pseudomonas, E. coli  PNA: Pneumonia  GAIN: Generating Antibiotic  cIAI: Complicated intra- Incentives Now abdominal infections  QIDP: Qualified Infectious  ctrUaTcIt: i nCfoemctpiolincsa ted urinary Disease Products  MSSA: Methicillin susceptible  ABSSSI: Acute bacterial skin staphylococcus aureus and skin structural infections  MRSA: Methicillin resistant  cSSSI: Complicated skin and staphylococcus aureus skin structural infections  VRSA: Vancomycin resistant  CAP: Community Acquired staphylococcus aureus Pneumonia  VRE: Vancomycin resistant  HABP: Hospital Acquired enterococcus Bacterial Pneumonia  MOA: Mechanism of action 1 12/23/2016 Abbreviations  DI: Drug Interactions  MAOI: Monoamine oxidase  PO: oral, IV: Intravenously inhibitor  RCT: Randomized controlled  Amp-c: Beta lactamase gene trial  KPCs: Klebsiella pneumoniae  ITT: Intended to treat group carbapenamases  ME/CE: Experimental group  CRE: Carbapenem resistant  n: Sample Size Enterobacteriaceae  Crcl: Creatinine Clearance  CC: Chief Complaint  CI: Confidence interval  HTN: Hypertension  PT: Prothrombin time  BP: Blood Pressure  INR: International  HR: Heart Rate normalization ratio  Temp: Temperature  aPPT: Activated partial  MDR: Multi drug resistant thromboplastin time  ESBL: Extended spectrum beta  QTc: QT-interval lactamase  CI: Contraindicated  GNR: gram negative rods  HNPEK: H, influenza, Neisseria, Proteus, E. coli, Klebsiella Background FDA Approved Antibiotics Boucher et al. Clinical Infectious Diseases 2013 Antibiotic Resistance Seeing is Believing Harvard Medical School andTechnion-Israel Institute of Technology; Sept 2016 2 12/23/2016 Background  Infections secondary to antibiotic-resistant bacteria are on the rise  Gram negative bacilli, Klebsiella pneumoniae, Acinetobacter baumannii, Pseudomonas aeruginosa and Enterobacter species (ESKAPE)  Innovation Act: GAIN; July 9, 2012  Extends exclusivity to 5 years for new antibiotics to treat serious or life-threatening infections (targeted indications)  Qualified Infectious Disease Products (QIDP) gain fast track and priority review status GAIN: Generating Antibiotic Incentives Now ESKAPE Organisms Bad Bugs, No Drugs: No ESKAPE! EE SS KK AA PP EE Enterobacter species -Klebsiella –Acinetobacter –Pseudomonas -E.coli Qualified Infectious Disease Products  Acinetobacter species  Streptococcus pyogenes  Enterobactericaceae  Aspergillus species species  Burkholderia cepacia  Pseudomonas species complex  Campylobacter species  Coccidoides species  Candida species  Crytococcus species  Clostridium difficile  Helicobacter pylori  Enterococcus species  Neisseria meningitides  M. tuberculosis complex  Non-tuberculous Mycobacteria  Neisseria gonorrhoeae  Staphylococcus aureus  Staphylococcus agalactiae  Streptococcus pneumoniae  Vibrio cholera Bold: ESKAPE; Underlined: QIDP All listed organisms are on the Center of Disease Control (CDC) urgent threat list 3 12/23/2016 Targeted Indications  Acute bacterial skin and skin structural infections (aSSTI)  Hospital acquired pneumonia/ventilator associated pneumonia (HAP/VAP)  Complicated intra-abdominal infections (cIAI)  Complicated urinary tract infections (cUTI) FDA Approved Antibiotics Timeline Telavancin Oritavancin September 11, 2009 August 6, 2014 GAIN 2012 Dalbavancin Ceftolozane/ May 23, 2014 Tazobactam December 19, 2014 Ceftazidime/ Tedizolid Avibactam June 20, 2014 February 25, 2015 Emerging Antibiotics Meropenem + RPX7009 (Carbavance) Imipenem/Relebactam (MK7655) Plazomicin (ACHN-4901)  All cover Qualified Infectious Disease Products (QIDP) 4 12/23/2016 Telavancin (Vibativ®)  September 11, 2009  Coverage: Gram Positives  Staphylococcus aureus •Methicillin susceptible staphylococcus aureus + Methicillin resistant staphylococcus aureus (MSSA + MRSA)  Streptococcus pyogenes  Streptococcus agalactiae  Streptococcus anginosus group  Enterococcus faecalis •Vancomycin resistant enterococcus (VRE) Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Pharmacology and Pharmacokinetics  Class: Synthetic lipoglycopeptide  Mechanism of Action (MOA):Interferes with cell wall synthesis and depolarizes the bacterial membrane  Metabolites: None detectable  Metabolism: Non-significant  Excretion: Kidney (76% excreted in urine)  Half-life: ~8 hours  Drug interactions: Non-significant Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Trials Two Phase 3 Trials Design Sample Intervention Infections RCT 1867 - Telavancin10 mg/kg IV Cellulitis,major every 24 hours abscesses, wound - Vancomycin1000 mg IV infections, burn and every 12 hours ulcer Clinical Response Rates in ABSSSI Trials using Responders at 48- 72 Hours after Initiation of Therapy Trial VIBATIV Vancomycin Difference n/N% n/N (%) 95%CI 1: ITT 72.5% (309/426) 71.6% (307/429) 0.9 (-5.3, 7.2) 1:CE 84.3% (289/343) 82.8% (288/348) 1.5 (-4.3, 7.3) 2: ITT 74.7% (342/458) 74.0% (356/481) 0.7 (-5.1, 6.5) 2:CE 83.9% (302/360) 87.7% (315/359) -3.8 (-9.2, 1.5) Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 5 12/23/2016 Telavancin Trials Two Phase 3 Trials All-Cause Mortality at Day 28 in Patients with at least One Baseline Gram-Positive Pathogen Trial VIBACTIV Vancomycin Difference 95%CI 1 28.7% (n= 187) 24.3 (n=180) 4.4% (-4.71, 13.5% ) CrCl ≤ 50 41.8% (n=63) 35.4% (n=68) 6.4% (-10.4-23.2%) CrCl > 50 22.0% 17.6% (n=112) 4.4% (-5.9-14.7%) 2 24.3% (n=22) 22.3% (n=206) 2.0% (-6.1%, 10%) CrCl ≤ 50 43.9% (n=53) 29.6% (n=58) 14.3% (-3.6, 32.2) CrCl > 50 18.2% (n=171) 19.3% (n=148) -1.1% (-9.8, 7.6) Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Indications and Dosages  Complicated skin and skin structure infection (CSSSI)  10 mg/kg IV over 60 minutes every 24 hours for 14 days  HABP/VABP  10 mg/kg IV over 60 minute every 24 hours for 21 days  Renal or hepatic dose adjustments:  Renal adjustment is required once CrCl < 50 mL/min  Formulations:  Solution for injection •750 mg/vial Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Adverse Events, Warnings and Precautions  Adverse Events:  Taste disturbance (33%)  Nausea (5-27%)  Vomiting (5-14%)  Foamy urine (13%)  Diarrhea (7%)  Contraindications:  Hypersensitivity to telavancin •Potential to cross-react with vancomycin Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 6 12/23/2016 Telavancin Adverse Events, Warnings and Precautions  Warning and Precautions:  Decreased efficacy in moderate/severe pre-existing renal impairment  Hypersensitivity reactions  Infusion-related reactions •To avoid “Red-man syndrome”: Administer over 60 minutes  Clostridium difficile-associated diarrhea  Coagulation test interference •Falsely elevates PT, INR, aPPT  QTc prolongation Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Adverse Events, Warnings and Precautions  Black Box Warning:  Use in moderate/severe renal impairment (CrCl < 50 ml/min) should only be considered if benefit outweighs risk •Increased mortality observed  Nephrotoxicity  Avoid use in pregnancy •Pregnancy test should be administered prior to initiation •Potential fetal risk  REMS program  Requires a medication guide and communication plan REMS: Risk Evaluation and Mitigation Strategies Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 Telavancin Advantages and Disadvantages Advantages: Disadvantages  Effective against  Only available as IV lung infections  More nephrotoxic  Less monitoring  QTc Prolongation required  CI in pregnancy  Acodvdeitriaogneal MRSA  Coagulation test interference Telavancin [package insert] San Francisco, CA; Theravance Biopharma antibiotics INC; 2009 7 12/23/2016 Comparator Considerations Telavancin Vancomycin Coverage • MRSA, VRE • MRSA Side Effects • BBW: nephrotoxic, • Nephrotoxic contraindicated in pregnancy • QTc Prolongation AWP/day • $449.93 (75 kg) • $9.12 (75 kg) • (10 mg/kg) • (15 mg/kg) Other • Less monitoring • More monitoring • Only indicated for • Additional indications SSTI and for PNA , endocarditis, nosocomial PNA osteomyelitis, • Coagulation test septicemia interference AWP: Average wholesale price Dalbavancin (Dalvance®)  Approved May 23, 2014  Coverage: Gram Positives  Staphylococcus aureus (MSSA + MRSA)  Streptococcus anginosus  Streptococcus pyogenes  Streptococcus agalactiae Dalbavancin [package insert] Chicago,IL;Durata therapeutics INC;2014 Dalbavancin Pharmacology and Pharmacokinetics  Class: Semisynthetic lipoglycopeptide  Mechanism of Action: Disrupts cell wall synthesis by binding D-alanyl-D-alanine terminus of peptidoglycan  Excretion: Evenly excreted in urine (30%) and feces (20%)  Minor metabolite excreted in urine  Half-life: ~346 hours (~2 weeks)  Drug Interactions (DI): Non-significant Dalbavancin [package insert] Chicago,IL;Durata therapeutics INC;2014 8 12/23/2016 Dalbavancin Trials Two Phase 3 Trials Design Sample Intervention Infections Randomized 1312 - Dalbavancin1000 mg IV x 1, then Cellulitis, major control trial 500 mg IV x 1 7 days later abscesses and (RCT) - Vancomycin1000 mg or 15 mg/kg wound infections IV q12h x 3 days then switched to linezolid 600mg PO q12h Clinical Response Rates in ABSSSI Trials at 48-72 Hours after Initiation of Therapy Trial DALVANCE Vancomycin/Linezolid Difference n/N (%) n/N (%) 95%CI 1 240/288 (83.3%) 233/285 (81.8%) 1.5% (-4.6. 7.9) 2 285/371 (76.8%) 288/368 (78.3%) -1.5% (-7.4, 4.6) Dalbavancin [package insert] Chicago,IL;Durata therapeutics INC;2014 Dalbavancin Indications and Dosages  Acute bacterial skin and skin structure infections (ABSSSI)  Regimen: •1000 mg IV over 30 minutes one time then •500 mg IV over 30 minutes one time  Administered one week after first infusion  Dalbavancin 1500mg delivered as a single dose was noninferior to a 2-dose regimen  Renal Adjustment •Renal adjustment is required once CrCl < 30 mL/min  Formulations  Solution for injection (500 mg/vial) Dalbavancin [package insert] Chicago, IL; Durata therapeutics INC;2014 Dunne, M. Clinical Infectious Diseases, 62(5), 545-551; 2016 Dalbavancin Adverse Events, Warning and Precautions  Adverse Events  Headache (3.8-4.7%)  Diarrhea (3.4-4.4%)  Nausea (2.0-5.5%)  Hypersensitivity Reactions  Cross-sensitivity with other glycopeptides  Infusion-related reactions (<2%)  Hepatic effects (<2%)  Clostridium difficile associated diarrhea Dalbavancin [package insert] Chicago,IL;Durata therapeutics INC;2014 9 12/23/2016 Dalbavancin Advantages and Disadvantages Advantages Disadvantages Commonly used Lacks   Minimal drug Enterococcus sp.  interactions coverage  Dosing regimen  Hepatic impairment Reduced  nephrotoxicity  Only available IV Dalbavancin [package insert] Chicago,IL;Durata therapeutics INC;2014 Comparator Considerations Dalbavancin Vancomycin Coverage • MRSA • MRSA • Enterococcus sp. Side Effects • Hepatic impairment • More nephrotoxic • Nephrotoxic AWP/week • $5,364 • $63.84 (75kg) Other • Simple dosing • More monitoring regimen • Additional indications • Only indicated for for PNA, endocarditis, SSTIs osteomyelitis, septicemia AWP: Average wholesale price Tedizolid (Sivextro®)  Approved June 20, 2014  Coverage: Gram Positives  Staphylococcus aureus (MSSA + MRSA)  Streptococcus anginosus  Streptococcus pyogenes  Streptococcus agalactiae  Enterococcus faecalis and faecium (VRE) Tedizolid [package insert] Ferentino, Italy; Merck and CO; 2014 10