A Study to Determine the Safety and the Efficacy of Fasinumab Compared to Placebo and Naproxen for Treatment of Adults With Pain From Osteoarthritis of the Knee or Hip

Osteoarthritis, Knee Clinical Trial

— FACT OA1  

Official title:

A Phase 3 Randomized, Double-blind, Multi-dose, Placebo and Naproxen-Controlled Study to Evaluate the Efficacy and Safety of Fasinumab in Patients With Pain Due to Osteoarthritis of the Knee or Hip

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT03161093
• Other study ID #: R475-OA-1611
• Secondary ID: 2016-005020-29
• Status: Completed
• Phase: Phase 3
• Start date: August 17, 2017
• Est. completion date: August 27, 2021

Study information

• Verified date: October 2022
• Source: Regeneron Pharmaceuticals
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

The primary objective of the study is to evaluate the efficacy of fasinumab compared with placebo, when administered for up to 16 weeks in patients with pain due to osteoarthritis (OA) of the knee or hip. The secondary objectives of the study are: 1. To evaluate the efficacy of fasinumab compared with naproxen, when administered for up to 16 weeks in patients with pain due to OA of the knee or hip 2. To evaluate the efficacy of fasinumab compared with placebo, when administered for up to 44 weeks in patients with pain due to OA of the knee or hip 3. To assess the safety and tolerability of fasinumab compared with naproxen, when administered for up to 16 weeks in patients with pain due to OA of the knee or hip 4. To assess the safety and tolerability of fasinumab compared with naproxen, when administered for up to 52 weeks in patients with pain due to OA of the knee or hip 5. To assess the safety and tolerability of fasinumab compared with naproxen, when administered for up to 104 weeks in patients with pain due to OA of the knee or hip 6. To evaluate the pharmacokinetic (PK) profile of fasinumab administered to patients with pain due to OA of the knee or hip for up to 52 weeks 7. To evaluate the PK profile of fasimumab administered to patients with pain due to OA of the knee or hip for up to 104 weeks 8. To evaluate the immunogenicity of fasinumab administered to patients with pain due to OA of the knee or hip for up to 52 weeks 9. To evaluate the immunogenicity of fasinumab administered to patients with pain due to OA of the knee or hip for up to 104 weeks 10. To evaluate the efficacy of fasinumab compared with naproxen, when administered for up to 44 weeks in patients with pain due to OA of the knee or hip

Recruitment information / eligibility

• Status: Completed
• Enrollment: 3307
• Est. completion date: August 27, 2021
• Est. primary completion date: September 9, 2019
• Accepts healthy volunteers: No
• Gender: All
• Age group: 18 Years and older

Eligibility

Inclusion Criteria include, but are not limited to, the following:

Year 1:

1. Male and female patients, at least 18 years of age, at screening

2. A clinical diagnosis of OA of the knee or hip based on the American College of Rheumatology criteria with radiologic evidence of OA (K-L score =2 for the index joint) at the screening visit

3. Moderate to severe pain in the index joint defined at both the screening and randomization visits

4. Willing to discontinue current pain medications and to adhere to study requirements for rescue treatments (acetaminophen/paracetamol) to be taken as needed with a maximum daily dose of 2500 mg (countries where 500 mg strength tablets/capsules are available) or 2600 mg (countries where 325 mg strength tablets/capsules are available)

5. A history of at least 12 weeks of analgesics use for pain due to OA of the knee or

hip, as defined by:

1. Inadequate pain relief from acetaminophen/paracetamol AND

2. Intolerance to or inadequate pain relief from opioid or tramadol therapy, unwillingness to take opioid or tramadol therapy for a medically acceptable reason, or lack of access to an opioid or to tramadol

6. Currently using a stable dose of NSAID.

7. Willing to discontinue glucosamine sulfate and chondroitin sulfate treatments during the initial 16 weeks of treatment

8. Stable treatment with glucosamine sulfate and chondroitin sulfate treatments must be stopped during the pre-randomization period

9. Consent to allow all radiographs and medical/surgical/hospitalization records of care received elsewhere prior to and during the study period to be shared with the investigator

10. Willing to maintain current activity and exercise levels throughout the study

11. Willing and able to comply with clinic visits and study-related procedures and willing to provide follow-up information related to any JR surgery that occurs within the period of time covered by their intended participation in the study

12. Able to understand and complete study-related questionnaires Year 2: Note: Any Year 1 patient attending their week 52 visit on or after 26 March 2020 will no longer have the option to enroll into Year 2.

1. Completed the treatment period of Year 1

2. Did not permanently discontinue study drug during Year 1

3. Received no less than 10 of the 13 planned doses of SC study drug during the treatment period of Year 1

4. Provide informed consent for Year 2

5. Willing to continue to maintain current activity and exercise levels throughout Year 2

Exclusion Criteria include, but are not limited to, the following:

1. Non-compliance with the Numeric Rating Scale (NRS) recording during the pre-randomization period

2. History or presence at the screening visit of non-OA inflammatory joint disease, Paget's disease of the spine, pelvis or femur, neuropathic disorders, multiple sclerosis, fibromyalgia, tumors or infections of the spinal cord, or renal osteodystrophy

3. History or presence on imaging of arthropathy, neuropathic joint arthropathy, hip or knee dislocation, extensive subchondral cysts, significant bone collapse or bone loss, or pathologic fractures

4. Trauma to the index joint within 3 months prior to the screening visit

5. Signs or symptoms of carpal tunnel syndrome within 6 months of screening

6. Patient is not a candidate for MRI

7. Is scheduled for a JR surgery to be performed during the study period or who would be unwilling or unable to undergo JR surgery if needed

8. History or presence at the screening visit of autonomic or diabetic neuropathy, or other peripheral neuropathy, including reflex sympathetic dystrophy

9. History or diagnosis of chronic autonomic failure syndrome including pure autonomic failure, multiple system atrophy

10. History of naproxen intolerance, or existence of a medical condition that is high risk for naproxen-associated complications

11. Resting heart rate of <50 beats per minute (bpm) or >100 bpm at the screening or randomization visits

12. History or presence of 2nd or 3rd degree heart block, 1st degree heart block with abnormal Complex of Q, R, and S waves on an electrocardiogram (QRS) complex, or bifascicular block by ECG assessment at the screening visit

13. History or presence of orthostatic hypotension at the screening, prerandomization, or randomization visits

14. History of poorly controlled hypertension

15. Use of systemic corticosteroid within 30 days prior to the screening visit. Intra-articular corticosteroids in the index joint within 12 weeks prior to the screening visit, or to any other joint within 30 days prior to the screening visit

16. Exposure to an anti-Nerve growth factor (NGF) antibody prior to the screening visit or known sensitivity or intolerance to anti-NGF antibodies

Related Conditions & MeSH terms

• Osteoarthritis
• Osteoarthritis, Hip
• Osteoarthritis, Knee

Intervention

Drug:
• Fasinumab
Solution for injection in pre-filled syringe
• Naproxen
Pharmaceutical form: Capsule
• Fasinumab-matching placebo
Solution for injection in pre-filled syringe
• Naproxen-matching placebo
Capsule

Locations

Country	Name	City	State
Denmark	CCBR Vejle	Vejle
Germany	Synexus Clinical Research GmbH	Berlin
Germany	Synexus Clinical Research GmbH	Bochum
Germany	Synexus Clinical Research GmbH	Frankfurt
Germany	Synexus Clinical Research GmbH	Leipzig	Sachsen
Hungary	Qualiclinic Kft.	Budapest
Hungary	Synexus Magyarorszag Kft	Budapest
Hungary	Synexus Magyarorszag Kft.	Debrecen
Hungary	Synexus Magyarorszag Kft.	Gyula
Hungary	BKS Research Kft.	Hatvan
Hungary	Hevizgyogyfurdo es Szent Andraes ReumaKorhaz	Hévíz
Hungary	Szabolcs-Szatmar-Bereg Megyei Korhazak es Egyetemi Oktato Korhazak Josa Andras Oktatokorhaza Klinikai Kutatasi Osztaly	Nyíregyháza
Hungary	Synexus Magyarorszag Egeszsegugyi Kft.	Zalaegerszeg
Lithuania	Hospital of Lithuanian University of Health Sciences Kaunas Clinics	Kaunas
Lithuania	Saules Seimos Medicinos Centras, Jsc	Kaunas
Lithuania	Republican Panevezys Hospital	Panevežys
Lithuania	Center Outpation Clinic, Public Institution	Vilnius
Poland	ClinicMed Daniluk, Nowak Sp.j.	Bialystok
Poland	Synexus Polska Sp. z o.o. Oddzial w Gdansku	Gdynia	Pomorskie
Poland	Synexus Polska Sp. z o.o. Oddzial w Gdyni	Gdynia	Pomorskie
Poland	MCBK Sc lwona Czajkowska Monika Barney	Grodzisk Mazowiecki	Mazowieckie
Poland	Synexus Polska Sp. z o.o. Oddzial w Katowicach	Katowice
Poland	Krakowskie Centrum Medyczne Sp. z o.o.	Kraków	Malopolskie
Poland	Malopolskie Centrum Kliniczne	Kraków
Poland	Specjalistyczny Osrodek Medycyny Wieku Dojrzalego Sp. z o.o. Jednostka 02 - SOMED - Lodzkie Centrum Osteoporozy	Lódz	Lodzkie
Poland	Synexus Polska Sp. z o.o Oddzial w Poznaniu	Poznan	Wielkopolskie
Poland	CLINMEDICA RESEARCH OMC, Spolka z Ograniczona Odpowiedzialnoscia Spolka Komandytowa	Skierniewice
Poland	Specjalistyczny Osrodek Medycyny Wieku Dojrzalego Sp. z o.o.	Warszawa	Mazowieckie
Poland	Synexus Polska Sp. z o.o. Oddzial w Warszawie	Warszawa	Mazowieckie
Poland	Synexus Polska Sp. z o.o. Oddzial we Wroclawiu	Wroclaw	Dolnoslaskie
Poland	Etg Zgierz	Zgierz
Romania	Clinica Medicala Synexus Ltd.	Bucharest
Romania	SC Policlinica CCBR SRL	Bucharest
Russian Federation	"SBEIHPE ""Kazan State Medical University"" of MHSD of Russia"	Kazan	Tatarstan Republic
Russian Federation	"CDCR ""Healthy Joints"" L.L.C."	Novosibirsk
Russian Federation	City Out-Patient Clinic #109	Saint Petersburg
Russian Federation	Samara Regional Clinical Hospital n.a.V.D.Seredavin	Samara
Russian Federation	"State Autonomous Healthcare Institution of Yaroslavl Oblast ""Clinical Hospital #3"""	Yaroslavl
South Africa	Mzansi Ethical Research Centre Cape Town	Cape Town
South Africa	TASK Applied Science	Cape Town
South Africa	Enhancing Care	Durban	KwaZulu-Natal
South Africa	Synapta Clinical Research Center	Durban	Kwa-Zulu Natal
South Africa	Newtown Clinical Research	Johannesburg
South Africa	Wits Clinical Research	Johannesburg	Gauteng
South Africa	Langeberg Medicross Medical Centre	Kraaifontein	Western Cape
South Africa	Mzansi Ethical Research Centre Middleburg	Middelburg	Mpumalanga
South Africa	Paarl Research Centre	Paarl	Western Cape
South Africa	Tread Research-Tygerberg Hospital	Parow	Cape Town
South Africa	Global Clinical Trials	Pretoria	Gauteng
South Africa	Synexus SA Stanza Clinical Research Centre	Pretoria	Gauteng
South Africa	Synexus Watermeyer Clinical Research Centre	Pretoria	Gauteng
South Africa	University of Pretoria	Pretoria	Gauteng
South Africa	Roodepoort Medicross Clinical Research Centre	Roodepoort	Gauteng
South Africa	Synexus Helderberg Clinical Trial Centre	Somerset West	Western Cape
South Africa	Soweto Clinical Trials Centre (CTC)	Soweto	Johannesburg
South Africa	Aliwal Shoal Medical Centre	Umkomaas	Kwa-Zulu Natal
South Africa	Welkom Clinical trial Centre	Welkom	Free State
Spain	Complejo Hospitalario Universitario A Coruna	A Coruña
Spain	CETA Leganes	Leganés	Madrid
Spain	MeDiNova Investigacion y Desarrollo	Madrid
Spain	Centro De Investigacion Clinica En Enfermedades Cronicas - Cicec	Santiago De Compostela
Spain	Clínica Nuevas Tecnologias en Diabetes y Endocrinologia (NTDE)	Sevilla
Spain	Hospital Quiron Salud Infanta Luisa	Sevilla
Ukraine	"Municipal Establishment ""Cherkasy Regional Hospital of Cherkasy Oblast Council"""	Cherkasy
Ukraine	Kharkiv City Multispecialty Hospital #18	Kharkiv
Ukraine	"Kyiv Railway Clinical Hospital No.2 of branch ""Health Center "" of the PJSC ""Ukrainian Railway"""	Kyiv
Ukraine	"Subsidiary Company ""Medical Research and Practice Center Medbud of the Public Joint Stock ""Holding Company ""Kyivmiskbud"""	Kyiv
Ukraine	Medical center of Private High Educational Institute Institute of General Practice-Family Medicine	Kyiv
Ukraine	Lviv Regional Hospital for veterans of the war and former political prisoners	Lviv
United Kingdom	Synexus Midlands Clinical Research Centre	Birmingham	West Midlands
United Kingdom	Synexus Wales Clinical Research Centre	Cardiff
United Kingdom	Synexus Lancashire Clinical Research Centre	Chorley	Lancashire
United Kingdom	Synexus Scotland Clinical Research Centre	Glasgow	Lanarkshire
United Kingdom	Synexus North East Clinical Research Centre - Hexham General Hospital	Hexham	Northumberland
United Kingdom	Synexus Merseyside Clinical Research Centre	Liverpool
United Kingdom	Synexus Manchester Clinical Research Centre-Manchester Science Park	Manchester
United Kingdom	MediNova North London Dedicated Research Centre, Mount Vernon Hospital	Northwood	Middlesex
United Kingdom	Synexus Thames Valley Clinical Research Centre	Reading	Berkshire
United Kingdom	Medinova Research East London Clinical Studies Centre	Romford
United Kingdom	MeDiNova Research Yorkshire Clinical Studies Centre	Shipley
United Kingdom	MediNova South London Dedicated Research Centre	Sidcup
United States	Lovelace Scientific Resources, Inc.	Albuquerque	New Mexico
United States	Lynn Institute of Denver	Aurora	Colorado
United States	Arthritis and Rheumatic Disease Specialties	Aventura	Florida
United States	Rheumatology & Pulmonary Clinic	Beckley	West Virginia
United States	United Medical Associates	Binghamton	New York
United States	PMG Research of Raleigh, LLC d/b/a PMG Research of Cary	Cary	North Carolina
United States	Low Country Rheumatology, PA	Charleston	South Carolina
United States	DJL Clinical Research, PLLC	Charlotte	North Carolina
United States	Center for Arthritis and Rheumatic Diseases	Chesapeake	Virginia
United States	Medex Healthcare Research, Inc.	Chicago	Illinois
United States	Northwestern University	Chicago	Illinois
United States	Sterling Research Group, Ltd.	Cincinnati	Ohio
United States	Lynn Institute of the Rockies	Colorado Springs	Colorado
United States	Medvin Clinical Research	Covina	California
United States	Klein & Associates, MD PA	Cumberland	Maryland
United States	Pioneer Research Solutions, Inc.	Cypress	Texas
United States	Altoona Center for Clinical Research	Duncansville	Pennsylvania
United States	TriWest Research Associates, LLC	El Cajon	California
United States	Regional Clinical Research, Inc.	Endwell	New York
United States	Healthcare Research Network II, LLC	Flossmoor	Illinois
United States	Clinical Research Solutions	Franklin	Tennessee
United States	Panorama Orthopedics & Spine Center	Golden	Colorado
United States	Klein & Associates, MD, PA	Hagerstown	Maryland
United States	Hickory Family Practice Associates	Hickory	North Carolina
United States	Peters Medical Research LLC	High Point	North Carolina
United States	Clinical Neuroscience Solutions, Inc.	Jacksonville	Florida
United States	Jacksonville Center for Clinical Research	Jacksonville	Florida
United States	The Center for Pharmaceutical Research	Kansas City	Missouri
United States	PMG Research of Knoxville	Knoxville	Tennessee
United States	BioSolutions Clinical Research	La Mesa	California
United States	Physician Research Collaboration, LLC	Lincoln	Nebraska
United States	Baptist Health Center for Clinical Research	Little Rock	Arkansas
United States	Pacific Arthritis Care Center	Los Angeles	California
United States	Clinical Neuroscience Solutions, Inc.	Memphis	Tennessee
United States	Advanced Clinical Research	Meridian	Idaho
United States	Arizona Arthritis & Rheumatology Research, PLLC	Mesa	Arizona
United States	Southwest Rheumatology Research, LLC	Mesquite	Texas
United States	PMG Research of Charleston, LLC	Mount Pleasant	South Carolina
United States	Medex Healthcare Research	New York	New York
United States	Sensible Healthcare	Ocoee	Florida
United States	Hillcrest Clinical Research	Oklahoma City	Oklahoma
United States	Buffalo Rheumatology and Medicine, PLLC	Orchard Park	New York
United States	Orchard Park Family Practice	Orchard Park	New York
United States	Clinical Neuroscience Solutions, Inc.	Orlando	Florida
United States	Jewett Orthopaedic Clinic	Orlando	Florida
United States	Arizona Research Center	Phoenix	Arizona
United States	Medex Healthcare Research, Inc.	Saint Louis	Missouri
United States	Sundance Clinical Research, LLC	Saint Louis	Missouri
United States	PMG Research of Salisbury, LLC	Salisbury	North Carolina
United States	Artemis Institute for Clinical Research	San Diego	California
United States	Artemis Clinical Research	San Marcos	California
United States	Meridian Clinical Research	Savannah	Georgia
United States	Tucson Orthopaedic Research Center	Tucson	Arizona
United States	Lovelace Scientific Resources	Venice	Florida
United States	Integrated Clinical Trial Services, Inc.	West Des Moines	Iowa
United States	The Center for Rheumatology and Bone Research	Wheaton	Maryland
United States	PMG Research of Winston-Salem, LLC	Winston-Salem	North Carolina
United States	Clinical Pharmacology Study Group	Worcester	Massachusetts

Sponsors (2)

Lead Sponsor	Collaborator
Regeneron Pharmaceuticals	Teva Pharmaceutical Industries, Ltd.

Countries where clinical trial is conducted

United States,  Denmark,  Germany,  Hungary,  Lithuania,  Poland,  Romania,  Russian Federation,  South Africa,  Spain,  Ukraine,  United Kingdom, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Change in the WOMAC Pain Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg SC Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Primary	Change in the WOMAC Physical Function Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Primary	Change in the WOMAC Pain Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg SC Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Primary	Change in the WOMAC Physical Function Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in the Patient Global Assessment (PGA) Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Placebo	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 16
Secondary	Change in the PGA Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Naproxen	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 16
Secondary	Change In The PGA Scores From Baseline To Week 44 In Participants Treated With Fasinumab 1mg Q4W Compared With That Of Participants Treated With Placebo	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 44
Secondary	Percentage Of Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Placebo, Who Had A Response At Week 16, With Response Defined As An Improvement By =30% In The WOMAC Pain Subscale Scores	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Percentage of Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Naproxen, Who Had A Response At Week 16, With Response Defined As An Improvement By =30% In The WOMAC Pain Subscale Scores	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Week 16
Secondary	Change in WOMAC Pain Subscale Scores From Baseline to Week 16 In Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in WOMAC Pain Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change in WOMAC Pain Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1 mg Q4W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to the Average Score Across Weeks 4, 8, 12 and 16, in Participants Treated With Fasinumab 1 mg Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 4, 8, 12 and 16
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to the Average Score Across Weeks 36, 40 and 44 in Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 36, 40 and 44
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1mg Q4W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change In WOMAC Pain Subscale Scores From Baseline To The Average Score Across Weeks 4, 8, 12 And 16, in Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 4, 8, 12 and 16
Secondary	Change in WOMAC Pain Subscale Scores From Baseline To The Average Score Across Weeks 36, 40 And 44 In Participants Treated With Fasinumab 1mg Q4W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 36, 40 and 44
Secondary	Change in the Patient Global Assessment (PGA) Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q8W Compared With That of Participants Treated With Placebo	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 16
Secondary	Change in the PGA Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1 mg Q8W Compared With That of Participants Treated With Naproxen	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 16
Secondary	Change In The PGA Scores From Baseline To Week 44 In Participants Treated With Fasinumab 1mg Q8W Compared With That Of Participants Treated With Placebo	The Patient Global Assessment of OA (PGA) is a patient-rated assessment of current disease state on a 5-point Likert scale (1 = very good; 2 = good; 3 = fair; 4 = poor; and 5 = very poor).	Baseline to Week 44
Secondary	Change in WOMAC Pain Subscale Scores From Baseline to Week 16 In Participants Treated With Fasinumab 1mg Q8W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in WOMAC Pain Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1mg Q8W, Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to the Average Score Across Weeks 4, 8, 12 and 16, in Participants Treated With Fasinumab 1 mg Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 4, 8, 12 and 16
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to the Average Score Across Weeks 36, 40 and 44 in Participants Treated With Fasinumab 1mg Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 36, 40 and 44
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to Week 16 in Participants Treated With Fasinumab 1mg Q8W, Compared With That of Participants Treated With Naproxen	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in WOMAC Physical Function Subscale Scores From Baseline to Week 44 in Participants Treated With Fasinumab 1mg Q8W, Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 44
Secondary	Change In WOMAC Pain Subscale Scores From Baseline To The Average Score Across Weeks 4, 8, 12 And 16, in Participants Treated With Fasinumab 1mg Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 4, 8, 12 and 16
Secondary	Percentage Of Participants Treated With Fasinumab 1mg Q8W, Compared With That of Participants Treated With Placebo, Who Had A Response At Week 16, With Response Defined As An Improvement By =30% In The WOMAC Pain Subscale Scores	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to Week 16
Secondary	Change in WOMAC Pain Subscale Scores From Baseline To The Average Score Across Weeks 36, 40 And 44 In Participants Treated With Fasinumab 1mg Q8W Compared With That of Participants Treated With Placebo	The WOMAC index is comprised of 24 parameters grouped in 3 subscales (pain-5 questions, physical function -17 questions and stiffness - 2 questions), with 0-10 grading of each question. The scores for each subscale are summed up, divided by number of questions, and each subscale is reported using Numerical Rating Scale score of 0-10. In addition to subscales, a total score is provided as the sum of normalized subscale scores divided by three, and reported using a Numerical Rating Scale score of 0-10. Higher scores indicate worse pain, stiffness and functional limitations.	Baseline to average score across weeks 36, 40 and 44
Secondary	Number of Participants With Adjudicated Arthropathy (AA) (as Confirmed by Adjudication) - Year 1		Baseline to Week 52
Secondary	Number of Participants With AA (as Confirmed by Adjudication) - Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of Participants With AA (as Confirmed by Adjudication) - Year 1 and Year 2		Day 1 through week 104E (Extension)
Secondary	Number of Participants With Destructive Arthropathy (DA) (as Confirmed by Adjudication) - Year 1		Baseline to Week 52
Secondary	Number of Participants With DA (as Confirmed by Adjudication) - Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of Participants With DA (as Confirmed by Adjudication) - Year 1 and Year 2		Day 1 through week 104E
Secondary	Number of Treatment Emergent Adverse Events (TEAEs) - Year 1		Baseline to Week 52
Secondary	Number of TEAEs - Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of TEAEs - Year 1 and Year 2		Day 1 through week 104E
Secondary	Number of Participants With at Least 1 Sympathetic Nervous System (SNS) Dysfunction Adverse Event of Special Interest (AESI) - Year 1		Baseline to Week 52
Secondary	Number of Participants With at Least 1 Sympathetic Nervous System (SNS) Dysfunction Adverse Event of Special Interest (AESI) - Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of Participants With at Least 1 Sympathetic Nervous System (SNS) Dysfunction Adverse Event of Special Interest (AESI) - Year 1 and Year 2		Day 1 through week 104E
Secondary	Number of Participants With at Least 1 Peripheral Sensory Neuropathy AESI That Require a Neurology or Other Specialty Consultation - Year 1		Baseline to Week 52
Secondary	Number of Participants With at Least 1 Peripheral Sensory Neuropathy AESI That Require a Neurology or Other Specialty Consultation - Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of Participants With at Least 1 Peripheral Sensory Neuropathy AESI That Require a Neurology or Other Specialty Consultation - Year 1 and Year 2		Day 1 through week 104E
Secondary	Number of Participants With Any Type of All-Cause Joint Replacement (JR) in Year 1		Baseline to Week 52
Secondary	Number of Participants With Any Type of All-Cause JR in Year 2		First dose of study drug in Year 2 through week 104E
Secondary	Number of Participants With Any Type of All-Cause Joint Replacement (JR) - Year 1 and Year 2		Day 1 through week 104E