Anti-HIV Agent Trichosanthin Enhances the Capabilities of Chemokines to Stimulate Chemotaxis and G Protein Activation, and This Is Mediated through Interaction of Trichosanthin and Chemokine Receptors

doi:10.1084/jem.190.1.101

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© The Rockefeller University Press, 0022-1007/1999/7/101/ $5.00
The Journal of Experimental Medicine, Volume 190, Number 1, July 1, 1999 101-112

Original Article

Anti-HIV Agent Trichosanthin Enhances the Capabilities of Chemokines to Stimulate Chemotaxis and G Protein Activation, and This Is Mediated through Interaction of Trichosanthin and Chemokine Receptors

Jian Zhao^a, Li-Hong Ben^a, Ya-Lan Wu^a, Wei Hu^a, Kun Ling^a, Shun-Mei Xin^a, Hui-Ling Nie^a, Lan Ma^b, and Gang Pei^a

^a From the Shanghai Institute of Cell Biology and Shanghai Research Center of Life Sciences, Chinese Academy of Sciences, Shanghai 200031, People's Republic of China
^b National Laboratory of Medical Neurobiology, Shanghai Medical University, Shanghai 200032, People's Republic of China

Trichosanthin (TCS), an active protein component isolated froma traditional Chinese medicinal herb Trichosanthes kirilowii,has been shown to inhibit HIV infection and has been appliedin clinical treatment of AIDS. The recent development that chemokinesand chemokine receptors play important roles in HIV infectionled us to investigate the possible functional interaction ofTCS with chemokines and their receptors. This study demonstratedthat TCS greatly enhanced both RANTES (regulated upon activation,normal T cell expressed and secreted)– and stromal cell–derivedfactor (SDF)-1 ${alpha}$ –stimulated chemotaxis (EC₅₀ ${cong}$ 1 nM) in leukocytes(THP-1, Jurkat, and peripheral blood lymphocyte cells) and activationof pertussis toxin–sensitive G proteins (EC₅₀ ${cong}$ 20 nM).TCS also significantly augmented chemokine-stimulated activationof chemokine receptors CCR5 and CXCR4 as well as CCR1, CCR2B,CCR3, and CCR4 transiently expressed in HEK293 cells. A mutantTCS with 4,000-fold lower ribosome-inactivating activity showedsimilar augmentation activity as wild-type TCS. Moreover, flowcytometry demonstrated that the specific association of TCSto the cell membranes required the presence of chemokine receptors,and laser confocal microscopy reveals that TCS was colocalizedwith chemokine receptors on the membranes. The results fromTCS-Sepharose pull-down and TCS and chemokine receptor coimmunoprecipitationand cross-linking experiments demonstrated association of TCSwith CCR5. Thus, our data clearly demonstrated that TCS synergizesactivities of chemokines to stimulate chemotaxis and G proteinactivation, and the effects of TCS are likely to be mediatedthrough its interaction with chemokine receptors.

Key Words: chemokine receptors • trichosanthin • G proteins • chemotaxis • HIV

1used in this paper: DSS, disuccinimidyl suberate; FBS, fetalbovine serum; GPCR, G protein–coupled receptor; HA, hemagglutinin;HEK, human embryonic kidney; MCP, monocyte chemotactic protein;MIP, macrophage inflammatory protein; RANTES, regulated uponactivation, normal T cell expressed and secreted; RIP, ribosome-inactivatingprotein; SDF, stromal cell–derived factor; TCS, trichosanthin

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