A Point Mutation That Confers Constitutive Activity to CXCR4 Reveals That T140 Is an Inverse Agonist and That AMD3100 and ALX40-4C Are Weak Partial Agonists

Zhang, Wenbo; Navenot, Jean-Marc; Haribabu, Bodduluri; Tamamura, Hirokazu; Hiramatu, Kenichi; Omagari, Akane; Pei, Gang; Manfredi, John P.; Fujii, Nobutaka; Broach, James R.; Peiper, Stephen C.

doi:10.1074/jbc.m200889200

Cited by 236 publications

(249 citation statements)

References 38 publications

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“…14 Comparative studies between T-140 and AMD3100 found that each of these agents inhibited CXCR4 through different mechanisms. 11,12,14 Analysis of antagonists revealed that exposure to AMD3100 induced G protein activation by CXCR4, whereas T-140 decreased autonomous signaling. 12 Therefore, AMD3100 was defined to have a weak partial agonist activity, whereas T-140 functions as an inverse agonist.…”

Section: Discussionmentioning

confidence: 99%

“…11,12,14 Analysis of antagonists revealed that exposure to AMD3100 induced G protein activation by CXCR4, whereas T-140 decreased autonomous signaling. 12 Therefore, AMD3100 was defined to have a weak partial agonist activity, whereas T-140 functions as an inverse agonist. In our current work, we found that SDF-1a at high levels, as well as T140, but not AMD3100, similarly affect the proliferation and differentiation of progenitors, granulocytes and erythroblasts when co-cultured with stromal cells.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, it was suggested that T140 acts as an inverse agonist, and AMD3100 acts as a weak partial agonist when the coupling of CXCR4 to Ga subunits in mammalian cells was assayed by [35S]GTPgS binding. 12 Indeed, blocking the CXCR4 receptor with antagonists, such as T140 or AMD3100, results in the mobilization of HPCs, including neutrophils. 13,14 Moreover, combination of these two antagonists with granulocyte colony-stimulating factor (G-CSF) has an additive effect.…”

Section: Introductionmentioning

confidence: 99%

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The CXCR4 antagonist 4F-benzoyl-TN14003 stimulates the recovery of the bone marrow after transplantation

Abraham¹,

Beider²,

Wald³

et al. 2009

Leukemia

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Cytopenia represents a significant complication after chemotherapy, irradiation before bone marrow (BM) transplantation or as a therapy for cancer. The mechanisms that determine the pace of BM recovery are not fully understood. During the recovery phase after chemotherapy or irradiation, the signals for retention of white blood cells within the BM increase significantly. This leads to a delay in the release of WBC, which can be overcome by targeting the CXCR4 axis with the antagonist 4F-benzoyl-TN14003 (T140). The delay in the release of WBC is also accompanied by suppression in the production of progenitor cells and mature cells by the BM stroma. Administration of T140 to mice transplanted with BM cells stimulates the production of all types of progenitors and mature cells, and increases the exit of mature cells to the periphery. Moreover, addition of T140, but not AMD3100, to BM stromal cultures stimulates the production of mature cells and progenitors from all lineages. The unique ability of the CXCR4 antagonist, T140 to stimulate the production and exit of WBC cells may be used as a novel therapeutic approach to overcome cytopenia associated with treatments for cancer and BM transplantation.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The CXCR4 antagonist 4F-benzoyl-TN14003 stimulates the recovery of the bone marrow after transplantation

Abraham¹,

Beider²,

Wald³

et al. 2009

Leukemia

View full text Add to dashboard Cite

show abstract

“…71 Also, in a series of experiments to elucidate the mechanism of CXCR4 signaling, it was noticed that T140 decreased autonomous CXCR4 signaling in CXCR4 wild-type or constitutively active CXCR4 mutants, characterizing T140 as an inverse CXCR4 agonist, whereas AMD3100 and ALX40-4C displayed partial agonist activity in this study. 72 Clinical trials will help to determine whether this characteristic of CXCR4 peptide antagonists correlates with a profile of activities and/or side effects that is distinct from AMD3100.…”

Section: Small Peptide Antagonist Of Cxcr4mentioning

confidence: 99%

CXCR4 antagonists: targeting the microenvironment in leukemia and other cancers

Burger

Peled²

2008

Leukemia

414

316

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“…AMD3100 was withdrawn from clinical trials in patients with HIV-1 infections because of cardiac toxicity. 2 The mechanism of antagonist action has been determined using human CXCR4 mutants with constitutive activity derived in yeast strains expressing the receptor functionally coupled to the pheromone response pathway (10). AMD3100 and ALX40-4C demonstrated weak partial agonist activity (10).…”

mentioning

confidence: 99%

Lipid Bilayer Simulations of CXCR4 with Inverse Agonists and Weak Partial Agonists

Trent

Wang

Murray

et al. 2003

Journal of Biological Chemistry

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111

120

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CXCR4 is a G protein-coupled receptor (GPCR) that has multiple critical functions in normal and pathologic physiology that include regulation of the metastatic behavior of mammary carcinoma, and utilization as a coreceptor for infection by T-tropic strains of human immunodeficiency virus-1. Molecular dynamic simulations of the rhodopsin-based homology model of CXCR4 were performed in a solvated lipid bilayer to reproduce the microenvironment of this integral membrane protein.The amino acids in CXCR4 necessary for interaction with an inverse agonist, T140, and a weak partial agonist, AMD3100, identified by alanine scanning mutants, were spatially consistent when computationally docked. Whereas T140 binds residues in extracellular domains and regions of the hydrophobic core proximal to the cell surface, amino acids in the central hydrophobic core are critical to binding of AMD3100. The physical localization of T140 binding to CXCR4 by biochemical analyses corroborated the molecular and computational approaches. The structural basis for the interaction of T140 and AMD3100 with CXCR4 confirms that the mechanisms used by these agents are different. This complementary utilization of molecular, physical, and computation analysis provides a powerful approach to elucidate GPCR conformation.

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A Point Mutation That Confers Constitutive Activity to CXCR4 Reveals That T140 Is an Inverse Agonist and That AMD3100 and ALX40-4C Are Weak Partial Agonists

Cited by 236 publications

References 38 publications

The CXCR4 antagonist 4F-benzoyl-TN14003 stimulates the recovery of the bone marrow after transplantation

The CXCR4 antagonist 4F-benzoyl-TN14003 stimulates the recovery of the bone marrow after transplantation

CXCR4 antagonists: targeting the microenvironment in leukemia and other cancers

Lipid Bilayer Simulations of CXCR4 with Inverse Agonists and Weak Partial Agonists

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