ANTIMICROBIAL DRUGS ADVISORY COMMITTEE MEETING BRIEFING BOOK Study Drug: Plazomicin NDA Number: 210303 Sponsor: Achaogen, Inc. 1 Tower Place, Suite 300 South San Francisco, CA 94080 Meeting Date: 2 May 2018 ADVISORY COMMITTEE BRIEFING MATERIALS: AVAILABLE FOR PUBLIC RELEASE Achaogen, Inc.—plazomicin AMDAC Meeting Briefing Book (30 March 2018) Page 1 of 171 TABLE OF CONTENTS Page 1.  Executive Summary ..........................................................................................................13  1.1  Proposed Indications ..............................................................................................13  1.2  Unmet Medical Need .............................................................................................13  1.3  Regulatory Pathway ...............................................................................................16  1.4  Overview of the Plazomicin Development Program .............................................17  1.4.1  Product Characteristics ...........................................................................18  1.4.2  Summaries of Microbiology and Clinical Pharmacology ......................19  1.4.2.1  Microbiology ........................................................................19  1.4.2.2  Clinical Pharmacology .........................................................23  1.4.3  Overview of Efficacy in the Complicated Urinary Tract and Bloodstream Infection Indications ..................................................29  1.4.3.1  Efficacy in the Phase 3 Complicated Urinary Tract Infection Study (Study ACHN-490-009) .............................29  1.4.3.2  Efficacy in Bloodstream Infections ......................................32  1.4.4  Overview of Safety Experience with Plazomicin ..................................36  1.4.4.1  Safety in the Pooled Phase 2 and 3 Complicated Urinary Tract Infection Studies (Studies ACHN-490-002 and ACHN-490-009) ...................37  1.4.4.2  Safety in the Phase 3 Study in Patients With Serious Infections Due to Carbapenem-Resistant Enterobacteriaceae (Study ACHN-490-007) .......................38  1.4.4.3  Aminoglycoside Class-Associated Toxicities in the Phase 2 and 3 Clinical Development Program ...............39  1.5  Overall Summary and Proposed Role for Plazomicin in the Treatment of cUTI and BSI in Patients with Limited or No Alternative Treatment Options .....42  2.  Clinical Development Plan Overview ..............................................................................45  3.  Regulatory History ............................................................................................................46  4.  Microbiology ....................................................................................................................48  4.1  Mechanisms of Action and Resistance ..................................................................48  4.2  Spectrum of Activity ..............................................................................................50  4.3  In Vitro Pharmacodynamics ..................................................................................52  4.4  In Vivo Pharmacodynamics ...................................................................................53  4.5  Potential for Plazomicin Resistance Development ................................................54  4.6  Clinical Microbiology ............................................................................................56  4.7  Pharmacokinetics/Pharmacodynamics Targets and Probability of Target Attainment Analyses .....................................................57  Achaogen, Inc.—plazomicin 2/AMDAC Meeting Briefing Book (30 March 2018) Page 2 of 171 TABLE OF CONTENTS (CONT’D) Page 5.  Efficacy in Complicated Urinary Tract Infection .............................................................60  5.1  Efficacy in Phase 3 Complicated Urinary Tract Infection Study (Study ACHN-490-009).........................................................................................60  5.1.1  Study Design ..........................................................................................60  5.1.1.1  Key Eligibility Criteria .........................................................61  5.1.1.2  Choice of Comparator ..........................................................61  5.1.1.3  Statistical Analysis ...............................................................62  5.1.2  Patient Disposition .................................................................................63  5.1.3  Demographics and Other Baseline Characteristics ................................63  5.1.3.1  Demographics and Disease Characteristics ..........................63  5.1.3.2  Baseline Infecting Pathogens and Susceptibility .................65  5.1.4  Efficacy Results ......................................................................................67  5.1.4.1  Primary, Secondary, and Key Additional Efficacy Analyses ...............................................67  5.1.4.2  Efficacy in Important Subgroups and Patient Subpopulations ..................................................69  5.1.4.3  Additional Efficacy Analyses ...............................................72  5.2  Efficacy in Phase 2 Study (Study ACHN-490-002) ..............................................77  6.  Efficacy in Bloodstream Infection ....................................................................................79  6.1  Efficacy in the Phase 3 Study in Patients With Serious Infections Due to Carbapenem-Resistant Enterobacteriaceae (Study ACHN-490-007) ................79  6.1.1  Study Design ..........................................................................................79  6.1.1.1  Key Study Eligibility Criteria and Diagnosis Criteria .........82  6.1.1.2  Choice of Comparator ..........................................................84  6.1.1.3  Choice of Adjunctive Therapy .............................................84  6.1.1.4  Statistical Analysis ...............................................................85  6.1.2  Patient Disposition .................................................................................85  6.1.3  Demographics and Other Baseline Characteristics ................................87  6.1.3.1  Demographics and Disease Characteristics ..........................87  6.1.3.2  Baseline Infecting Pathogens and Susceptibility .................89  6.1.4  Efficacy Results for Cohort 1 .................................................................91  6.1.4.1  Primary Efficacy Analysis ...................................................91  6.1.4.2  Additional Analyses of the Primary Endpoint: Efficacy in Important Subgroups and Patient Subpopulations ...........94  6.1.4.3  Additional Efficacy Results .................................................95  Achaogen, Inc.—plazomicin 3/AMDAC Meeting Briefing Book (30 March 2018) Page 3 of 171 TABLE OF CONTENTS (CONT’D) Page 6.1.4.4  Microbiological Response Results .......................................95  6.1.4.5  Response by Baseline Infecting Pathogen ...........................97  6.1.5  Emergent Infections .............................................................................100  6.1.6  Impact of Non-Study Drug Therapy ....................................................100  6.1.7  Efficacy Results for Cohort 2 ...............................................................100  6.2  Efficacy Results in the Enterobacteriaceae Bacteremia Subgroup From Phase 3 Complicated Urinary Tract Infection Study (Study ACHN-490-009) ...101  6.2.1  Primary Endpoint Analysis in Enterobacteriaceae Bacteremia Subgroup ..............................................................................................101  6.2.2  Clearance of Blood Pathogens .............................................................101  6.3  Mouse Septicemia Study......................................................................................102  6.4  Summary of Efficacy in Bloodstream Infections .................................................102  7.  Safety ..............................................................................................................................104  7.1  Nonclinical Toxicology .......................................................................................104  7.2  Clinical Safety ......................................................................................................104  7.2.1  Safety Evaluations ................................................................................104  7.2.1.1  Specific Safety Assessments for Nephrotoxicity and Ototoxicity ..........................................105  7.2.2  Safety Analyses ....................................................................................106  7.2.2.1  Subgroups for Safety Analysis ...........................................106  7.2.3  Safety in the Pooled Phase 2 and 3 cUTI Studies ................................106  7.2.3.1  Disposition of Patients in the Safety Analysis ...................106  7.2.3.2  Demographics and Baseline Characteristics ......................107  7.2.3.3  All Adverse Events .............................................................109  7.2.3.4  Deaths and Other Serious Adverse Events .........................113  7.2.3.5  Clinical Laboratory Evaluations .........................................114  7.2.3.6  Vital Signs and Electrocardiograms ...................................114  7.2.3.7  Safety in Patients with Renal Impairment ..........................114  7.2.4  Safety in the Phase 3 Study in Patients With Serious Infection Due to Carbapenem-Resistant Enterobacteriaceae, Including Bloodstream Infection ..........................................................................116  7.2.4.1  Disposition of Patients in the Safety Analysis ...................116  7.2.4.2  Demographics and Baseline Characteristics ......................117  7.2.4.3  All Adverse Events .............................................................121  7.2.4.4  Adverse Events by Severity ...............................................122  Achaogen, Inc.—plazomicin 4/AMDAC Meeting Briefing Book (30 March 2018) Page 4 of 171 TABLE OF CONTENTS (CONT’D) Page 7.2.4.5  Treatment-Emergent Adverse Events Resulting in Discontinuation of Intravenous Study Drug .......................123  7.2.4.6  Deaths and Other Serious Adverse Events .........................124  7.2.4.7  Clinical Laboratory Evaluations .........................................125  7.2.4.8  Vital Signs and Electrocardiograms ...................................125  7.2.4.9  Safety in Patients with Renal Impairment ..........................126  7.2.5  Aminoglycoside Class-Associated Adverse Events in the Clinical Development Program ..................................................126  7.2.5.1  Nephrotoxicity ....................................................................126  7.2.5.2  Ototoxicity ..........................................................................129  7.2.5.3  Neurotoxicity ......................................................................129  7.3  Postmarketing Experience ...................................................................................129  8.  Benefit–Risk Discussion .................................................................................................130  8.1  Nonclinical Benefits .............................................................................................130  8.2  Clinical Benefits ...................................................................................................131  8.3  Limitations and Risks ..........................................................................................132  9.  Conclusion ......................................................................................................................136  10.  References .......................................................................................................................137  LIST OF TABLES Table 1:  Summary of Pivotal Phase 3 Study Features ...................................................17  Table 2:  Proposed Dosing Regimens Based on Creatinine Clearance Categories .........26  Table 3:  Two Types of Therapeutic Drug Management ................................................27  Table 4:  Performance of AUC-Based Therapeutic Drug Management in a Simulated Population of BSI Patients as Reflected by Summary Statistics for AUC0–24h .....................................................................29  Table 5:  Composite of Microbiological and Clinical Cure at Day 5 (mMITT and ME-Day 5 Populations) and the Test-of-Cure Visit (mMITT and ME-TOC Populations) (Study ACHN-490-009) ......................................31  Table 6:  All-Cause Mortality at Day 28 or Significant Disease Related Complications—mMITT Population, Cohort 2 BSI Subgroup (Study ACHN-490-007)...................................................................................35  Table 7:  Overview of Treatment-Emergent Adverse Events and Deaths—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) ................37  Table 8:  Overview of Treatment-Emergent Adverse Events and Deaths—Safety Population (Study ACHN-490-007) ................................................................38  Achaogen, Inc.—plazomicin 5/AMDAC Meeting Briefing Book (30 March 2018) Page 5 of 171 TABLE OF CONTENTS (CONT’D) Page Table 9:  Treatment Emergent Adverse Events Related to Renal Function and Serum Creatinine Increases 0.5 mg/dL—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) ..................................40  Table 10:  Treatment Emergent Adverse Events Related to Renal Function and Serum Creatinine Increases 0.5 mg/dL—Safety Population (Study ACHN-490-007)...................................................................................41  Table 11:  Plazomicin Clinical Development Program—Completed Clinical Studies .....45  Table 12:  Plazomicin Activity Against Isogenic Escherichia coli Expressing Individual Aminoglycoside-Modifying Enzymes ............................................50  Table 13:  Antibacterial Activity of Plazomicin Against 2014 Through 2016 US Surveillance Isolates ..........................................................51  Table 14:  Plazomicin Efficacy in Animal Models Against Multidrug Resistant Enterobacteriaceae ..........................................................54  Table 15:  Emergence of Resistance in Patients from Study 009 .....................................56  Table 16:  Plazomicin PK/PD Targets Against Enterobacteriaceae .................................58  Table 17:  Study Disposition—ITT Population (Study ACHN-490-009) ........................63  Table 18:  Demographics and Baseline Characteristics— mMITT Population (Study ACHN-490-009) ..................................................64  Table 19:  Uropathogens Identified From Baseline Urine Cultures— mMITT Population (Study ACHN-490-009) ..................................................66  Table 20:  Composite of Microbiological Response and Clinical Response at Day 5 (mMITT and ME-Day 5 Populations) and the Test-of-Cure Visit (mMITT and ME–TOC Populations) (Study ACHN-490-009) ......................68  Table 21:  Clinical Response at Day 5 and the End-of-Intravenous-Therapy and Test-of-Cure Visits—mMITT Population (Study ACHN-490-009) ...............72  Table 22:  Per-Patient Microbiological Response at Day 5 and the End-of-Intravenous-Therapy and Test-of-Cure Visits— mMITT Population (Study ACHN-490-009) ..................................................73  Table 23:  Per-Pathogen Microbiological Eradication Rates at the Test-of-Cure Visit by Baseline Uropathogen—mMITT Population (Study ACHN-490-009) ......74  Table 24:  Patients with Superinfections and/or New Infections— mMITT Population (Study ACHN-490-009) ..................................................76  Table 25:  Microbiological Response at the Test-of-Cure Visit— MITT and ME Populations (Study ACHN-490-002) ......................................78  Table 26:  Diagnosis Criteria for Bloodstream Infection ..................................................83  Table 27:  Patient Demographics and Baseline Disease Characteristics— mMITT Population, BSI Subgroup (Study ACHN-490-007) .........................88  Table 28:  Baseline Pathogens Based on Study-Qualifying Cultures— mMITT Population, BSI Subgroup (Study ACHN-490-007) .........................90  Achaogen, Inc.—plazomicin 6/AMDAC Meeting Briefing Book (30 March 2018) Page 6 of 171 TABLE OF CONTENTS (CONT’D) Page Table 29:  All-Cause Mortality at Day 28 or Significant Disease-Related Complications—mMITT Population, Cohort 1 BSI and HABP/VABP Patients (Study ACHN-490-007) .............................................92  Table 30:  All-Cause Mortality at Day 28 or Significant Disease-Related Complications—mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007)...................................................................................93  Table 31:  All-Cause Mortality at Day 28 or Significant Disease-Related Complications by Subgroup—mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007) ...........................................................94  Table 32:  Per-Patient Microbiological Response at EOT and TOC— mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007) ..........96  Table 33:  Documented Clearance of CRE Bacteremia—mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007) ............................................97  Table 34:  Per-Pathogen Favorable Microbiological Response at Test of Cure by Baseline Pathogen and Pathogen Category—mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007) ........................98  Table 35:  Per-Pathogen Favorable Microbiological Response at Test of Cure by Plazomicin MIC to Each Baseline Pathogen and Pathogen Category— mMITT Population, Cohort 1 BSI Subgroup (Study ACHN-490-007) ..........99  Table 36:  Demographics and Baseline Characteristics—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) ................................107  Table 37:  Treatment-Emergent Adverse Events Reported in at Least 2% of Patients in the Pooled Plazomicin Group—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) ..............................................110  Table 38:  Incidence of Severe or Worse Treatment-Emergent Adverse Events by Preferred Term—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) .....................................................................................110  Table 39:  Adverse Events Leading to Premature Discontinuation of Intravenous Study Drug—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) .....................................................................................112  Table 40:  Incidence of Serious Adverse Events by Preferred Term—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) ..............113  Table 41:  Risk Factors for Potential Nephrotoxicity .....................................................115  Table 42:  Patient Disposition—Intent-to-Treat Population (Study ACHN-490-007) ...116  Table 43:  Patient Demographics and Baseline Disease Characteristics— Safety Population (Study ACHN-490-007) ...................................................118  Table 44:  Treatment-Emergent Adverse Events With at Least 5% Incidence in the Combined Plazomicin Group—Safety Population (Study ACHN-490-007) ....122  Achaogen, Inc.—plazomicin 7/AMDAC Meeting Briefing Book (30 March 2018) Page 7 of 171 TABLE OF CONTENTS (CONT’D) Page Table 45:  Incidence of Grade 3 Treatment-Emergent Adverse Events Occurring in 2 Patients in Any Cohort 1 or Cohort 2 Treatment Group—Safety Population (Study ACHN-490-007) ..............................................................123  Table 46:  Incidence of Serious Adverse Events Occurring in 2 Patients in Any Cohort 1 or Cohort 2 Treatment Group—Safety Population (Study ACHN-490-007).................................................................................125  Table 47:  Patients With Any Serum Creatinine Increase of 0.5 mg/dL or Greater Above Baseline—Safety Population (Pooled Studies ACHN-490-002 and ACHN-490-009) .....................................................................................127  Table 48:  Patients With Any Serum Creatinine Increase of 0.5 mg/dL or Greater Above Baseline—Safety Population (Study ACHN-490-007)......................128  LIST OF FIGURES Figure 1:  Kaplan-Meier Curve of Overall Mortality through Day 60— mMITT Population, BSI Subgroup (Study ACHN-490-007) .........................34  Figure 2:  Documented Clearance of Blood Pathogens in cUTI Patients with Concurrent Enterobacteriaceae Bacteremia—mMITT Population (Study ACHN-490-009)...................................................................................36  Figure 3:  The Plazomicin Chemical Structure and Common Sites of Aminoglycoside Modification by Aminoglycoside-Modifying Enzymes .......49  Figure 4:  MIC Distribution of Plazomicin Against Enterobacteriaceae Isolates Nonsusceptible to Amikacin, Gentamicin, or Tobramycin (2014-2016 US Surveillance) ......................................................51  Figure 5:  MIC Distribution of Plazomicin Against Carbapenem-Resistant Enterobacteriaceae and ESBL Enterobacteriaceae Isolates .............................52  Figure 6:  Plazomicin Exhibits Rapid Bactericidal Activity in Time-Kill Studies ..........53  Figure 7:  Plazomicin Suppresses Resistance Outgrowth in an In Vitro Chemostat Model ...............................................................................55  Figure 8:  Probability of Plazomicin Stasis Target Attainment Overlaid on the MIC Distributions of cUTI/AP Baseline Enterobacteriaceae From Study 009 and UTI Enterobacteriaceae from 2014-2016 US Surveillance .....59  Figure 9:  Probability of Plazomicin 1-log10 Kill Target Attainment Overlaid on the MIC Distributions of BSI Baseline Enterobacteriaceae From Study 007 and BSI Enterobacteriaceae from 2014-2016 US Surveillance ......59  Figure 10:  Study Design Schema and Overview of Study Schedule for Study ACHN-490-009 ................................................................60  Figure 11:  Composite Cure by Study Day—mMITT Population (Study ACHN-490-009) ................................................................69  Figure 12:  Composite Cure at the Test-of-Cure Visit by Subgroup— mMITT Population (Study ACHN-490-009) ..................................................71  Achaogen, Inc.—plazomicin 8/AMDAC Meeting Briefing Book (30 March 2018) Page 8 of 171 TABLE OF CONTENTS (CONT’D) Page Figure 13:  Study Design Schema and Overview of Study Schedule for Study ACHN-490-007 ................................................................80  Figure 14:  Disposition Flow Diagram for Study ACHN-490-007 ....................................86  Figure 15:  Kaplan-Meier Survival Curve of Plazomicin Monotherapy vs Untreated Control Over 96 Hours in a Mouse Model of Septicemia .............................102 LIST OF APPENDICES Appendix 1:  Tabular Overview of Completed Clinical Studies .........................................144  Appendix 2:  Population Pharmacokinetics Analysis Population Demographics ...............150  Appendix 3:  Therapeutic Drug Management Procedures ...................................................151  Appendix 4:  Additional Information on Statistical Analyses for Study ACHN-490-007 ...................................................................................153  Appendix 5:  Summary of Key Program and Regulatory Milestones for Plazomicin......................................................................................................155  Appendix 6:  Animal Models Used in Plazomicin Efficacy Studies ...................................158  Appendix 7:  Eligibility Criteria for Phase 3 Studies ..........................................................161 Appendix 7.1: Eligibility Criteria for Study ACHN-490-009 ...............................................161  Appendix 7.2: Eligibility Criteria for Study ACHN-490-007 ...............................................165  Achaogen, Inc.—plazomicin 9/AMDAC Meeting Briefing Book (30 March 2018) Page 9 of 171 List of Abbreviations Abbreviation Definition 16S RMTase 16S ribosomal ribonucleic acid methyltransferase AAC aminoglycoside acetyltransferase ACE angiotensin-converting enzyme ACM all-cause mortality AE adverse event AME aminoglycoside-modifying enzyme ANT aminoglycoside nucleotidyltransferase AP acute pyelonephritis APACHE II Acute Physiology and Chronic Health Evaluation II APH aminoglycoside phosphotransferase ARDS acute respiratory distress syndrome ASHA American Speech-Language-Hearing Association AUC area under the concentration-time curve from time zero to 24hours 0–24h BL/BLI -lactam/-lactamase inhibitor BMI body mass index BSI bloodstream infection CBA colistin base activity CFU colony-forming unit CLcr creatinine clearance CLSI Clinical and Laboratory Standards Institute CMS colistimethate sodium CRE carbapenem-resistant Enterobacteriaceae CRRT continuous renal replacement therapy CSR Clinical Study Report CT computerized tomography CTCAE Common Terminology Criteria for Adverse Events cUTI complicated urinary tract infection DDI drug–drug interaction ECG electrocardiogram eCRF electronic case report form ELF epithelial lining fluid ENG electronystagmography EOIV end of intravenous therapy Achaogen, Inc.—plazomicin 10/AMDAC Meeting Briefing Book (30 March 2018) Page 10 of 171