Identification of Residues on CD40 and Its Ligand Which Are Critical for the Receptor-Ligand Interaction

Bajorath, Juergen; Chalupny, N. Jan; Marken, John S.; Siadak, Anthony W.; Skonier, John E.; Gordon, Marcia N.; Hollenbaugh, Diane; Noelle, Randolph J.; Ochs, Hans D.; Aruffo, Alejandro

doi:10.1021/bi00006a003

Cited by 72 publications

(83 citation statements)

References 31 publications

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“…Such structural restraint of the N terminus may also affect the way in which the ligand interacts with the receptor and explain the enhanced bioactivity. Site-directed mutagenesis has shown that Lys 143 and Tyr 145 are critical for CD40L interaction with CD40 (27). These residues are in close proximity to the N terminus.…”

Section: Discussionmentioning

confidence: 99%

Incorporation of an Isoleucine Zipper Motif Enhances the Biological Activity of Soluble CD40L (CD154)

Morris

Remmele

Klinke

et al. 1999

Journal of Biological Chemistry

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Recent progress in the understanding of immune function indicates that the interaction of CD40L with its receptor, CD40, plays a pivotal role in both humoral immunity and cell-mediated defense against pathogens. Functional studies of this interaction on both dendritic cells and malignant cells have demonstrated that CD40L also plays an important role in immune surveillance and anti-tumor immunity. CD40L exists in nature predominantly as a membrane-anchored molecule. To develop CD40L as a potential therapeutic, it is important to optimize soluble forms of this molecule that could be used in a clinical setting. Several reports have shown that soluble forms of CD40L, like CD40 antibodies, are biologically active. In the present report we demonstrate that the incorporation of an isoleucine zipper trimerization motif significantly enhances the biological activity of soluble CD40L.Interaction of CD40L (CD154) with its receptor, CD40, provides essential signals for the development of a protective humoral immune response and is a key mechanism in the regulation of defense against pathogenic assault (for review see Ref. 1). CD40, a 50-kDa transmembrane glycoprotein, is a member of the tumor necrosis factor (TNF) 1 receptor superfamily (for review see Refs. 2 and 3) and is expressed on antigen-presenting cells including dendritic cells, B cells, macrophages, follicular dendritic cells, and fibroblasts. CD40 is also expressed on a number of other cell types including endothelial cells and a significant proportion of carcinomas.CD40L is predominantly expressed on activated CD4 ϩ T cells, but variable expression has also been reported on CD8 ϩ T cells, mast cells, basophils, B cells, monocytes, NK cells, and activated platelets (1-4). Generally, CD40L does not exist naturally in a soluble form, although exceptions have been reported (5, 6). Initial studies focusing on the interaction of CD40L with its receptor on B cells show that CD40L is largely responsible for the helper T cell function that drives B cell proliferation and Ig class switching and protects B cells from apoptotic cell death. More recent studies on other cell types have indicated an important role for CD40L in the induction of T cell-mediated effector functions, antigen presentation, and costimulatory activity of antigen-presenting cells and in the production of many cytokines (for review see Ref. 1).CD40L is a type II membrane glycoprotein and is a member of the TNF superfamily. CD40L has an extracellular domain consisting of a 75-amino acid spacer region immediately adjacent to the membrane spanning region that is not shared by other family members and a receptor-binding domain that consists of two stacked ␤-sheets. The receptor-binding domain has low amino acid sequence homology with TNF family members (Ͻ30%) but has high structural homology (7). Soluble forms of CD40L have been expressed that are able to induce B cell proliferation, costimulate Ig class switching, and suppress the induction of apoptosis (8 -10). As with cell surface expressed CD40L, maxi...

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Section: Discussionmentioning

confidence: 99%

Incorporation of an Isoleucine Zipper Motif Enhances the Biological Activity of Soluble CD40L (CD154)

Morris

Remmele

Klinke

et al. 1999

Journal of Biological Chemistry

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“…Similar trees were obtained using maximum parsimony analyses and by systematically adding or removing sequences from the phylogenetic analyses. (22). A potential glycosylation site (Asn 240 ) described in human CD40L is indicated ( ‡) (22).…”

Section: Phylogenetic Analysis Of Teleost Tnfsf Membersmentioning

confidence: 99%

“…(22). A potential glycosylation site (Asn 240 ) described in human CD40L is indicated ( ‡) (22). Abbreviations: Hs, Homo sapiens; Mm, Mus musculus; Xt, X. tropicalis; Om, O. mykiss; Tn, T. nigroviridis.…”

Section: Phylogenetic Analysis Of Teleost Tnfsf Membersmentioning

confidence: 99%

“…Through single and double amino acid substitutions, five amino acids (Gln 220 , Arg 203 , Lys 143 , Tyr 145 , and Tyr 146 ) have been found to be important for CD40L-CD40 binding in mammals (22). None of these residues were found to be conserved in alignment analysis of teleost O. mykiss, S. salar, Tetraodon nigroviridis, Fugu rubripes, D. rerio, P. olivaceus, and G. aculeatus CD40L sequences (Fig.…”

Section: Cd40l (Tnfsf 5)mentioning

confidence: 99%

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Early Diversification of the TNF Superfamily in Teleosts: Genomic Characterization and Expression Analysis

Glenney

Wiens

2007

The Journal of Immunology

108

121

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The TNF superfamily (TNFSF) of proteins are cytokines involved in diverse immunological and developmental pathways. Little is known about their evolution or expression in lower vertebrate species. Bioinformatic searches of Zebrafish, Tetraodon, and Fugu genome and other teleost expressed sequence tag databases identified 44 novel gene sequences containing a TNF homology domain. This work reveals the following: 1) teleosts possess orthologs of BAFF, APRIL, EDA, TWEAK, 4-1BBL, Fas ligand, LIGHT, CD40L, RANKL, and possibly TL1A; 2) the BAFF-APRIL subfamily is enriched by a third member, BALM, unique to fish; 3) orthologs of lymphotoxins ␣ and ␤ were not clearly identified in teleosts and are substituted by a related ligand, TNF-New; 4) as many as four TRAIL-like genes are present in teleosts, as compared with only one in mammals; and 5) T cell activation ligands OX40L, CD27L, CD30L, and GITRL were not identified in any fish species. Finally, we characterize mRNA expression of TNFSF members CD40L, LIGHT, BALM, APRIL, Fas ligand, RANKL, TRAIL-like, and TNF-New in rainbow trout, Oncorhynchus mykiss, immune and nonimmune tissues. In conclusion, we identified a total of 14 distinct TNFSF members in fishes, indicating expansion of this superfamily before the divergence of bony fish and tetrapods, ϳ360 -450 million years ago. Based on these findings, we extend a model of TNFSF evolution and the coemergence of the vertebrate adaptive immune system.

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“…With the TNF-␤/TNF receptor interaction in mind, Bajorath et al (29) have identified the CD40 and CD154 residues that are ؉ BJAB cells. BJAB (A) or U937 (B) cell lines were stimulated at 37°C with 250 ng of sCD154WT or each of its mutants for the indicated time points.…”

Section: Discussionmentioning

confidence: 99%

Functional Interaction of CD154 Protein with α5β1 Integrin Is Totally Independent from Its Binding to αIIbβ3 Integrin and CD40 Molecules

Fakhry

Alturaihi

Yacoub

et al. 2012

Journal of Biological Chemistry

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Identification of Residues on CD40 and Its Ligand Which Are Critical for the Receptor-Ligand Interaction

Cited by 72 publications

References 31 publications

Incorporation of an Isoleucine Zipper Motif Enhances the Biological Activity of Soluble CD40L (CD154)

Incorporation of an Isoleucine Zipper Motif Enhances the Biological Activity of Soluble CD40L (CD154)

Early Diversification of the TNF Superfamily in Teleosts: Genomic Characterization and Expression Analysis

Functional Interaction of CD154 Protein with α5β1 Integrin Is Totally Independent from Its Binding to αIIbβ3 Integrin and CD40 Molecules

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