New Insights on the Emerging Genomic Landscape of CXCR4 in Cancer: A Lesson from WHIM

Scala, Stefania; D’Alterio, Crescenzo; Milanesi, Samantha; Castagna, Alessandra; Carriero, Roberta; Farina, Floriana Maria; Locati, Massimo; Borroni, Elena Monica

doi:10.3390/vaccines8020164

Cited by 9 publications

(12 citation statements)

References 171 publications

(240 reference statements)

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“…These somatic mutations are primarily subclonal, and almost always associated with the MYD88 L265P mutation, the first identified recurring mutation in almost 67-90% of non-IgM secreting WM patients [6]. All 17 CXCR4 heterozygous mutations identified so far in WM span in the C-ter of the receptor, and closely resemble the already documented germline mutations of CXCR4 C-ter occurring in heterozygosis in WHIM syndrome [9]. Although their relevance for clinical presentation and overall survival, as well as their relationship with resistance to chemotherapy are still unsolved issues [26][27][28], several studies reported that patients with CXCR4 mutations present a significantly lower rate of adenopathy, and those with CXCR4 nonsense mutations have an increased BM disease burden, serum IgM levels, and/or risk of symptomatic hyperviscosity [29].…”

Section: Waldenstrom's Macroglobulinaemiasupporting

confidence: 53%

“…At least 20 different WHIM/WHIM-like mutations have been described so far in the genomic region of chromosome 2q21 that encodes the C-ter of CXCR4 [9,29] (Figure 1). Interestingly, these mutations occur in the context of a gene that is highly conserved across species and span in a genomic region that is even more highly conserved than the gene as a whole [32].…”

Section: Genetic Barcode Of Whim Mutationsmentioning

confidence: 99%

“…Acquired CXCR4 WHIM-like mutations, are present in up to 40% of patients with WM and are nearly always observed in conjunction with the MYD88 L265P mutation [29]. CXCR4 mutations are essentially unique to WM, as they have not been described so far in other malignancies, except for several cases of patients affected by follicular lymphoma [9,22]. Among the different CXCR4 mutations observed, 5 are NS and 12 FS [34].…”

Section: Genetic Barcode Of Whim Mutationsmentioning

confidence: 99%

“…Since CXCR4 is an attractive target for diverse diseases and is considered as one of the best potential targets in hematological tumors, several efforts are currently ongoing aimed at developing specific inhibitors including small molecules, peptides, antibodies, and siRNA that abrogate receptor activity [8]. Of note, several clinical trials proposed CXCR4 inhibitors for treatment of hematological tumors alone or in combination with chemotherapy or biological agents [9]. Although the CXCR4 antagonist Plerixafor (also known as AMD3100) is an Food and Drug Administration (FDA)-approved drug and represents a valid therapeutic approach in both WHIM and WM, the complexity of its use in clinical practice indicates the need to develop new strategies.…”

Section: Introductionmentioning

confidence: 99%

“…Although the CXCR4 antagonist Plerixafor (also known as AMD3100) is an Food and Drug Administration (FDA)-approved drug and represents a valid therapeutic approach in both WHIM and WM, the complexity of its use in clinical practice indicates the need to develop new strategies. Other CXCR4 antagonists such as Mavorixafor (also known as AMD11070) the humanized IgG blocking monoclonal antibody BMS-936564 (also known as Ulocuplumab) are currently tested in clinical trials for WHIM and WM and showed promising results [9]. Targeting the other part of the axis, CXCL12, also represents an attractive alternative approach that may facilitate regulation rather than the abrogation of receptor activity, although the extremely high evolutionary conservation of this chemokine gets the generation of efficacious antibodies complicated.…”

Section: Introductionmentioning

confidence: 99%

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Aberrant CXCR4 Signaling at Crossroad of WHIM Syndrome and Waldenstrom’s Macroglobulinemia

Milanesi

Locati

Borroni

2020

IJMS

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Given its pleiotropic functions, including its prominent role in inflammation, immune responses and cancer, the C-X-C chemokine receptor type 4 (CXCR4) has gained significant attention in recent years and has become a relevant target in drug development. Although the signaling properties of CXCR4 have been extensively studied, several aspects deserve deeper investigations. Mutations in the C-term tail of the CXCR4 gene cause WHIM syndrome, a rare congenital immunodeficiency associated by chronic leukopenia. Similar mutations have also been recently identified in 30% of patients affected by Waldenstrom’s macroglobulinaemia, a B-cell neoplasia with bone marrow accumulation of malignant cells. An ample body of work has been generated to define the impact of WHIM mutations on CXCR4 signaling properties and evaluate their role on pathogenesis, diagnosis, and response to therapy, although the identity of disease-causing signaling pathways and their relevance for disease development in different genetic variants are still open questions. This review discusses the current knowledge on biochemical properties of CXCR4 mutations to identify their prototypic signaling profile potentially useful to highlighting novel opportunities for therapeutic intervention.

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Section: Waldenstrom's Macroglobulinaemiasupporting

confidence: 53%

Section: Genetic Barcode Of Whim Mutationsmentioning

confidence: 99%

Section: Genetic Barcode Of Whim Mutationsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Aberrant CXCR4 Signaling at Crossroad of WHIM Syndrome and Waldenstrom’s Macroglobulinemia

Milanesi

Locati

Borroni

2020

IJMS

Self Cite

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Chemokines as possible therapeutic targets in metastatic melanoma

et al. 2023

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Background Cutaneous melanoma is a relentless form of cancer which continues to rise in incidence. Currently, cutaneous melanoma is the leading cause of skin cancer‐related mortality, which can mainly be attributed to its metastatic potential. The activation of chemokine axes is a major contributor to melanoma metastasis through its involvement in promoting tumour cell migration, proliferation, survival, and adhesion. This review will focus on the role of chemokines in melanoma and possible therapeutic strategies to alter chemokine activation and subsequently inhibit the activation of signalling cascades that may promote metastasis. Methods A literature review was conducted to evaluate chemokines as possible therapeutic targets in metastatic melanoma. Results The crosstalk between signalling pathways and immune responses in the melanoma microenvironment resembles a complex and dynamic system. Therefore, the involvement of governing chemokine axes in the promotion of cutaneous and metastatic melanoma demands a proper understanding of the tumour microenvironment in order to identify possible targets and develop appropriate treatments against melanoma. Conclusion Even though chemokine axes are regarded as promising therapeutic targets, it has become increasingly evident that chemokines can play a critical role in both tumour inhibition and promotion. The inhibition of chemokine axes to inhibit signalling cascades in target cells that regulate metastasis should, therefore, be carefully approached.

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Sevoflurane but not propofol enhances ovarian cancer cell biology through regulating cellular metabolic and signaling mechanisms

Wang²,

Liu³

et al. 2022

Cell Biol Toxicol

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Perioperative risk factors, including the choice of anesthetics, may influence ovarian cancer recurrence after surgery. Inhalational anesthetic sevoflurane and intravenous agent propofol might affect cancer cell metabolism and signaling, which, in turn, may influence the malignancy of ovarian cancer cells. The different effects between sevoflurane and propofol on ovarian cancer cell biology and underlying mechanisms were studied. Cultured ovarian cancer cells were exposed to 2.5% sevoflurane, 4 μg/mL propofol, or sham condition as the control for 2 h followed by 24-h recovery. Glucose transporter 1 (GLUT1), mitochondrial pyruvate carrier 1 (MPC1), glutamate dehydrogenase 1 (GLUD1), pigment epithelium-derived factor (PEDF), p-Erk1/2, and hypoxia-inducible factor 1-alpha (HIF-1α) expressions were determined with immunostaining and/or Western blot. Cultured media were collected for 1H-NMR spectroscopy-based metabolomics analysis. Principal component analysis (PCA) and orthogonal projections to latent structures discriminant analysis (OPLS-DA) were used to analyze metabolomics data. Sevoflurane increased the GLUT1, MPC1, GLUD1, p-Erk1/2, and HIF-1α expressions but decreased the PEDF expression relative to the controls. In contrast to sevoflurane, propofol decreased GLUT1, MPC1, GLUD1, p-Erk1/2, and HIF-1α but increased PEDF expression. Sevoflurane increased metabolite isopropanol and decreased glucose and glutamine energy substrates in the media, but the opposite changes were found after propofol treatment. Our data indicated that, unlike the pro-tumor property of sevoflurane, propofol negatively modulated PEDF/Erk/HIF-1α cellular signaling pathway and inhibited ovarian cancer metabolic efficiency and survival, and hence decreased malignancy. The translational value of this work warrants further study. Graphical abstract • Sevoflurane promoted but propofol inhibited ovarian cancer cell biology. • Sevoflurane upregulated but propofol downregulated the GLUT1, MPC1, and GLUD1 expressions of ovarian cancer cells. • Sevoflurane enhanced but propofol inhibited ovarian cancer cellular glucose. metabolism and glutaminolysis. • Sevoflurane downregulated PEDF but upregulated the Erk pathway and HIF-1α, while propofol had the adverse effects on ovarian cancer cells.

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New Insights on the Emerging Genomic Landscape of CXCR4 in Cancer: A Lesson from WHIM

Cited by 9 publications

References 171 publications

Aberrant CXCR4 Signaling at Crossroad of WHIM Syndrome and Waldenstrom’s Macroglobulinemia

Aberrant CXCR4 Signaling at Crossroad of WHIM Syndrome and Waldenstrom’s Macroglobulinemia

Chemokines as possible therapeutic targets in metastatic melanoma

Sevoflurane but not propofol enhances ovarian cancer cell biology through regulating cellular metabolic and signaling mechanisms

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