Inhibitory Effect of Afatinib on Platelet Activation and Apoptosis

Cao, Hang; Bhuyan, Abdulla Al Mamun; Umbach, Anja T.; Bissinger, Rosi; Gawaz, Meinrad; Läng, Florian

doi:10.1159/000484377

Cited by 6 publications

(20 citation statements)

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“…On the other hand, thrombin‐induced platelet responses were less strongly inhibited. Further investigation showed that the collagen‐induced phosphorylation of Akt was decreased by afatinib .…”

Section: Effects Of Tkis On Platelet Functionmentioning

confidence: 99%

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Tullemans

Heemskerk

Kuijpers

2018

Journal of Thrombosis and Haemostasis

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Platelets can contribute to tumor progression and metastasis. Cancer patients are at increased risk of thrombosis, and advanced stages of cancer are associated with thrombocytosis or increased platelet reactivity. Tyrosine kinase inhibitors (TKIs) are widely used as a targeted strategy for cancer treatment, with the aim of prolonging progression-free survival of the patients. Because of their broad kinase target spectrum, most TKIs inevitably have off-target effects. Platelets rely on tyrosine kinase activity for their activation. Frequently observed side effects are lowering of platelet count and inhibition of platelet functions, whether or not accompanied by an increased bleeding risk. In this review, we aim to give insights into: (i) 38 TKIs that are currently used for the treatment of different types of cancer, either on the market or in clinical trials; (ii) how distinct TKIs can inhibit activation mechanisms in platelets; and (iii) the clinical consequences of the antiplatelet effects of TKI treatment. For several TKIs, the knowledge on affinity for their targets does not align with the published effects on platelets and reported bleeding events. This review should raise awareness of the potential antiplatelet effects of several TKIs, which will be enhanced in the presence of antithrombotic drugs.

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Section: Effects Of Tkis On Platelet Functionmentioning

confidence: 99%

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Tullemans

Heemskerk

Kuijpers

2018

Journal of Thrombosis and Haemostasis

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“…Individual values (mean AE SD) of female and male WT and Ga i2 -deficient mice of annexin-V-binding, platelet volume, caspase-3-positive cells, ceramide abundance, P-selectin abundance and activated integrin a IIb b3 are displayed in Table 1A-D. No significant differences were observed between male and female WT or Ga i2 -deficient mice. Phosphatidylserine exposure, a hallmark of platelet apoptosis, was quantified by flow cytometry analysis using annexin-V-binding as described previously (Cao et al 2017). As illustrated in Figure 1A and D, the percentage of PS-positive platelets in untreated resting Ga i2 À/À and WT platelets was not significantly different.…”

Section: Resultsmentioning

confidence: 81%

“…Phosphatidylserine exposure, a hallmark of platelet apoptosis, was quantified by flow cytometry analysis using annexin‐V‐binding as described previously (Cao et al. ). As illustrated in Figure A and D, the percentage of PS‐positive platelets in untreated resting Gα i2 −/− and WT platelets was not significantly different.…”

Section: Resultsmentioning

confidence: 99%

“…Next, we explored whether G α i2 ‐mediated platelet apoptosis accompanies cell volume alterations (Cao et al. ). As depicted in Figure E and H, forward scatter, reflecting platelet volume, was not significantly different in resting platelets of either genotype but was significantly reduced following thrombin and CoRP treatment, an effect significantly less pronounced in Gα i2 −/− platelets than in WT platelets (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…We then sought to elucidate the mechanism(s) regulating Ga i2 -mediated apoptosis. To this end, we analyzed intracellular Ca 2+ levels [Ca 2+ ] i in murine platelets of either genotype using Fluo3 AM fluorescence as described previously (Cao et al 2017). As a result, prior to CoRP treatment, [Ca 2+ ] i in resting platelets was similar in Ga i2 À/À platelets (22.73 AE 0.69, a.u.…”

Section: Resultsmentioning

confidence: 99%

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Heterotrimeric G-protein subunit Gα _i2 contributes to agonist-sensitive apoptosis and degranulation in murine platelets

et al. 2018

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Gα i2, a heterotrimeric G‐protein subunit, regulates various cell functions including ion channel activity, cell differentiation, proliferation and apoptosis. Platelet‐expressed Gα i2 is decisive for the extent of tissue injury following ischemia/reperfusion. However, it is not known whether Gα i2 plays a role in the regulation of platelet apoptosis, which is characterized by caspase activation, cell shrinkage and cell membrane scrambling with phosphatidylserine (PS) translocation to the platelet surface. Stimulators of platelet apoptosis include thrombin and collagen‐related peptide (CoRP), which are further known to enhance degranulation and activation of α II b β3‐integrin and caspases. Using FACS analysis, we examined the impact of agonist treatment on activation and apoptosis in platelets drawn from mice lacking Gα i2 and their wild‐type (WT) littermates. As a result, treatment with either thrombin (0.01 U/mL) or CoRP (2 μg/mL or 5 μg/mL) significantly upregulated PS‐exposure and significantly decreased forward scatter, reflecting cell size, in both genotypes. Exposure to CoRP triggered a significant increase in active caspase 3, ceramide formation, surface P‐selectin, and α II b β3‐integrin activation. These molecular alterations were significantly less pronounced in Gα i2‐deficient platelets as compared to WT platelets. In conclusion, our data highlight a previously unreported role of Gα i2 signaling in governing platelet activation and apoptosis.

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Platelet C3G: a key player in vesicle exocytosis, spreading and clot retraction

Fernández-Infante,

Hernández-Cano,

Herranz

et al. 2024

Cell. Mol. Life Sci.

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C3G is a Rap1 GEF that plays a pivotal role in platelet-mediated processes such as angiogenesis, tumor growth, and metastasis by modulating the platelet secretome. Here, we explore the mechanisms through which C3G governs platelet secretion. For this, we utilized animal models featuring either overexpression or deletion of C3G in platelets, as well as PC12 cell clones expressing C3G mutants. We found that C3G specifically regulates α-granule secretion via PKCδ, but it does not affect δ-granules or lysosomes. C3G activated RalA through a GEF-dependent mechanism, facilitating vesicle docking, while interfering with the formation of the trans-SNARE complex, thereby restricting vesicle fusion. Furthermore, C3G promotes the formation of lamellipodia during platelet spreading on specific substrates by enhancing actin polymerization via Src and Rac1-Arp2/3 pathways, but not Rap1. Consequently, C3G deletion in platelets favored kiss-and-run exocytosis. C3G also controlled granule secretion in PC12 cells, including pore formation. Additionally, C3G-deficient platelets exhibited reduced phosphatidylserine exposure, resulting in decreased thrombin generation, which along with defective actin polymerization and spreading, led to impaired clot retraction. In summary, platelet C3G plays a dual role by facilitating platelet spreading and clot retraction through the promotion of outside-in signaling while concurrently downregulating α-granule secretion by restricting granule fusion.

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Inhibitory Effect of Afatinib on Platelet Activation and Apoptosis

Cited by 6 publications

References 58 publications

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Heterotrimeric G-protein subunit Gα _i2 contributes to agonist-sensitive apoptosis and degranulation in murine platelets

Platelet C3G: a key player in vesicle exocytosis, spreading and clot retraction

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Inhibitory Effect of Afatinib on Platelet Activation and Apoptosis

Cited by 6 publications

References 58 publications

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Acquired platelet antagonism: off‐target antiplatelet effects of malignancy treatment with tyrosine kinase inhibitors

Heterotrimeric G-protein subunit Gα i2 contributes to agonist-sensitive apoptosis and degranulation in murine platelets

Platelet C3G: a key player in vesicle exocytosis, spreading and clot retraction

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Heterotrimeric G-protein subunit Gα _i2 contributes to agonist-sensitive apoptosis and degranulation in murine platelets