UMIN-CTR Clinical Trial

Public title

Analysis of pathogenic role of soluble immune semaphorin in autoimmune diseases.

Acronym

Semaphorin in autoimmune diseases

Scientific Title

Analysis of pathogenic role of soluble immune semaphorin in autoimmune diseases.

Scientific Title:Acronym

Semaphorin in autoimmune diseases

Region

Japan

Condition

autoimmune diseases (including rheumatoid arthritis and osteoarticular diseases (including osteoarthritis and osteoporosis)

Classification by specialty

Clinical immunology

Orthopedics

Classification by malignancy

Others

Genomic information

NO

Narrative objectives1

Analysis of semaphorin status during conventional and biologics treatment in autoimmune and osteoarticular diseases

Basic objectives2

Others

Basic objectives -Others

To establish the significance of semahorin as a new pharmacometrics method in the autoimmune and osteoarticular diseases

Trial characteristics_1

Exploratory

Trial characteristics_2

Explanatory

Developmental phase

Not applicable

Primary outcomes

-disease activity scores (DAS28, -CDAI/SDAI, CRP, MMP3 in RA)
-Semahorins (Sema3A, Sema4A, Sema4D)
-bone turnover markers
-cytokines and proteases

Key secondary outcomes

To evaluate efficacy of conventional and biologics treatment

Study type

Observational

Basic design

Randomization

Randomization unit

Blinding

Control

Stratification

Dynamic allocation

Institution consideration

Blocking

Concealment

No. of arms

Purpose of intervention

Type of intervention

Interventions/Control_1

Interventions/Control_2

Interventions/Control_3

Interventions/Control_4

Interventions/Control_5

Interventions/Control_6

Interventions/Control_7

Interventions/Control_8

Interventions/Control_9

Interventions/Control_10

Age-lower limit

20

years-old

<=

Age-upper limit

Not applicable

Gender

Male and Female

Key inclusion criteria

Males and females diagnosed autoimmune and osteoarticular diseases including rheumatoid arthritis, osteoarthritis, osteporosis) must
-be more than 20 years old
-be informed and will give written informed consent

Key exclusion criteria

-complicated with active infectious diseases
-The patients who the doctors in charge consider should not enter this study.

Target sample size

100

Name of lead principal investigator

1st name
Middle name
Last name	Atsushi Ogata

Organization

Osaka University Graduate School of Medicine

Division name

Department of Respiratory Medicine, Allergy and Rheumatic Diseases

Zip code

Address

2-2, Yamadaoka, Suita, Osaka Japan 565-0871

TEL

06-6879-3833

Email

ogata@imed3.med.osaka-u.ac.jp

Name of contact person

1st name
Middle name
Last name	Atsushi Ogata

Organization

Osaka University Graduate School of Medicine

Division name

Department of Respiratory Medicine, Allergy and Rheumatic DIseases

Zip code

Address

2-2, Yamadaoka, Suita, Osaka Japan 565-0871

TEL

06-6879-3833

Homepage URL

Email

ogata@imed3.med.osaka-u.ac.jp

Institute

Osaka University Graduate School of Medicine

Institute

Department

Personal name

Organization

Osaka University Graduate School of Medicine

Organization

Division

Category of Funding Organization

Other

Nationality of Funding Organization

Co-sponsor

Name of secondary funder(s)

Organization

Address

Tel

Email

Secondary IDs

NO

Study ID_1

Org. issuing International ID_1

Study ID_2

Org. issuing International ID_2

IND to MHLW

Institutions

Date of disclosure of the study information

2014

Year

02

Month

10

Day

URL releasing protocol

Publication of results

Partially published

URL related to results and publications

http://onlinelibrary.wiley.com/

Number of participants that the trial has enrolled

Results

Levels of sSema4D were elevated in RA patients, and disease activities were correlated with serum levels of sSema4D. Treatment with an anti-Sema4D antibody suppressed arthritis in CIA.
Levels of sSema4D were elevated in ANCA associated vasculitis patients. Neutrophil surface Sema4D functions as a negative regulator of neutrophil activation. Proteolytic cleavage of Sema4D as observed in patients with AAV may amplify neutrophil-mediated inflammatory responses.

Results date posted

Results Delayed

Results Delay Reason

Date of the first journal publication of results

Baseline Characteristics

Participant flow

Adverse events

Outcome measures

Plan to share IPD

IPD sharing Plan description

Recruitment status

Completed

Date of protocol fixation

2013

Year

04

Month

01

Day

Date of IRB

Anticipated trial start date

2013

Year

04

Month

01

Day

Last follow-up date

2017

Year

08

Month

13

Day

Date of closure to data entry

2017

Year

08

Month

13

Day

Date trial data considered complete

2017

Year

08

Month

13

Day

Date analysis concluded

2017

Year

08

Month

13

Day

Other related information

Yoshida Y, Ogata A, Kang S, Ebina K, Shi K, Nojima S, Kimura T, Ito D, Morimoto K, Nishide M, Hosokawa T, Hirano T, Shima Y, Narazaki M, Tsuboi H, Saeki Y, Tomita T, Tanaka T, Kumanogoh A.Semaphorin 4D Contributes to Rheumatoid Arthritis by Inducing Inflammatory Cytokine Production: Pathogenic and Therapeutic Implications. Arthritis Rheumatol. 2015 Jun;67(6):1481-90.
Nishide M, Nojima S, Ito D, Takamatsu H, Koyama S, Kang S, Kimura T, Morimoto K, Hosokawa T, Hayama Y, Kinehara Y, Kato Y, Nakatani T, Nakanishi Y, Tsuda T, Park JH, Hirano T, Shima Y, Narazaki M, Morii E, Kumanogoh A. Semaphorin 4D inhibits neutrophil activation and is involved in the pathogenesis of neutrophil-mediated autoimmune vasculitis. Ann Rheum Dis. 2017 Aug;76(8):1440-1448.

Registered date

2014

Year

02

Month

05

Day

Last modified on

2018

Year

08

Month

11

Day

Link to view the page

Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000015256