Major Histocompatibility Complex Haplotype Is Associated with Postherpetic Pain in Mice

Author:

Sato-Takeda Masako1,Takasaki Ichiro2,Takeda Kenji3,Sasaki Atsushi4,Andoh Tsugunobu5,Nojima Hiroshi6,Shiraki Kimiyasu7,Kuraishi Yasushi8,Hanaoka Kazuo9,Tokunaga Katsushi10,Yabe Toshio11

Affiliation:

1. Assistant Professor, Department of Anesthesiology, Graduate School of Medicine, University of Tokyo, Tokyo, Japan. Department of Research, Tokyo Metropolitan Red Cross Blood Center, Tokyo, Japan.

2. Assistant Professor, Division of Molecular Genetics Research, Life Science Research Center.

3. Assistant Professor, Department of Anesthesiology, Graduate School of Medicine, University of Tokyo.

4. Postgraduate Student.

5. Assistant Professor.

6. Associate Professor.

7. Professor, Department of Virology, Faculty of Medicine, University of Toyama.

8. Professor, Department of Applied Pharmacology, Faculty of Pharmaceutical Science, University of Toyama, Toyama, Japan.

9. Chairman, JR Tokyo General Hospital, Tokyo, Japan.

10. Professor, Department of Human Genetics, Graduate School of Medicine, University of Tokyo.

11. Research Fellow, Department of Research, Tokyo Metropolitan Red Cross Blood Center, Tokyo, Japan.

Abstract

Background Postherpetic neuralgia is one of the major complications of herpes zoster caused by the reactivation of varicella-zoster virus and is characterized by severe pain. The authors previously showed the association of a human major histocompatibility complex (MHC) haplotype with postherpetic neuralgia. This study was performed to experimentally confirm the role of MHC haplotype in the development of postherpetic pain using a mouse model of postherpetic pain, which corresponds to postherpetic neuralgia. Methods BALB/c mice (MHC haplotype: H-2), C57BL/6 mice (MHC haplotype: H-2), and BALB/b mice, a congenic BALB/c strain with H-2, were used. Herpes simplex virus type I was transdermally inoculated on the hind paw. Unilaterally zosteriform skin lesion and pain-related responses (acute herpetic pain) were caused, and some mice showed pain-related responses (postherpetic pain) after the cure of skin lesions. Herpes simplex virus type I antigen and CD3-positive cells were immunostained in the dorsal root ganglion in the acute phase. Results The incidence (78%) of postherpetic pain in C57BL/6 mice was significantly higher than that (35%) in BALB/c mice (P = 0.004, odds ratio = 6.7). Furthermore, the incidence of postherpetic pain in BALB/b (H-2) was similar to that in C57BL/6. Herpes simplex virus type I antigen-positive cells were less in the dorsal root ganglion of C57BL/6 mice than that of BALB/c mice. CD3-positive T cells were more in the dorsal root ganglion of C57BL/6 mice than BALB/c mice. Conclusions These results suggest that the MHC haplotype (H-2) is involved in the incidence of postherpetic pain, and CD3-positive T cells may play a role in its pathogenesis.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Anesthesiology and Pain Medicine

Reference42 articles.

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