All-trans Retinoic Acid Potentiates the Ability of Interferon Beta-1b to Augment Suppressor Cell Function in Multiple Sclerosis

doi:10.1001/archneur.55.3.315

You are seeing this message because your Web browser does not support basic Web standards. Find out more about why this message is appearing and what you can do to make your experience on this site better.

Welcome | My Account | E-mail Alerts | Access Rights | Sign In

Vol. 55 No. 3, March 1998

Archives
	•	Online Features

Original Contribution

This Article
•	Full text
•	PDF
•	Reply to article
•	Send to a friend
•	Save in My Folder
•	Save to citation manager
•	Permissions

Citing Articles
•	Citation map
•	Citing articles on HighWire
•	Citing articles on ISI (15)
•	Contact me when this article is cited

Related Content
•	Similar articles in this journal

Topic Collections
•	Immunologic Disorders
•	Multiple Sclerosis/ Demyelinating Disease
•	Alert me on articles by topic

All-trans Retinoic Acid Potentiates the Ability of Interferon Beta-1b to Augment Suppressor Cell Function in Multiple Sclerosis

Zhi Xiang Qu, PhD; Amit Dayal; Mark A. Jensen, PhD; Barry G. W. Arnason, MD

Arch Neurol. 1998;55:315-321.

Objective To determine the effects of combination all-transretinoic acid (RA) and interferon beta-1b therapy on immunesystem functions potentially relevant to multiple sclerosis(MS).

Design Interferon gamma–secreting cells, T suppressorcell function, and lymphocyte proliferative responses were assayedusing peripheral blood mononuclear cells from patients withMS and control subjects under control conditions and in thepresence of interferon beta-1b, RA, and the 2 combined.

Setting A university hospital MS clinic.

Participants Seventeen patients with secondarily progressiveMS and 25 control subjects.

Results Interferon beta-1b use increased interferon gamma–secretingcell counts, augmented T suppressor cell function, and inhibitedT-cell proliferation. Therapy with RA decreased interferon gamma–secretingcell counts, had a minimal positive effect on T suppressor cellfunction, and had no effect on T-cell proliferation. When RAand interferon beta-1b were combined, the inhibitory effectof RA on interferon gamma–secreting cells predominated,T suppressor cell function increased synergistically over theincrement observed with interferon beta-1b use alone, and theinhibitory effect of interferon beta-1b alone on T-cell proliferationremained unchanged.

Conclusions Treatment with interferon beta-1b partiallyrestores defective T suppressor cell function in patients withMS. This potentially beneficial action is synergistically potentiatedby RA. Interferon beta-1b increases the number of interferongamma–secreting cells in the circulation when treatmentis initiated. A similar increment in interferon gamma-secretingcells is observed when interferon beta-1b is added to culturalperipheral blood mononuclear cells in vitro. This potentiallydeleterious action of interferon beta-1b is reversed by RA.Interferon beta-1b inhibits lymphocyte proliferation modestlybut reproducibly. This action of interferon beta-1b is unalteredby RA. These data provide a rationale for a trial of combinationtreatment with interferon beta-1b and RA in patients with MS.

From the Department of Neurology and the Brain Research Institute, University of Chicago, Chicago, Ill.

THIS ARTICLE HAS BEEN CITED BY OTHER ARTICLES

Concomitant therapy for multiple sclerosis
Stuart and Vermersch
Neurology 2004;63:S28-S34.
ABSTRACT | FULL TEXT

Retinol measurements and retinoid receptor gene expression in patients with multiple sclerosis
Royal et al.
Mult Scler 2002;8:452-458.
ABSTRACT

Etretinate Augments Interferon Beta-1b Effects on Suppressor Cells in Multiple Sclerosis
Qu et al.
Arch Neurol 2001;58:87-90.
ABSTRACT | FULL TEXT

| | |