![Platelet FXIII-A is not synthesized during activation of human platelets. (A-C) Washed human platelets were unstimulated (Unstim) or stimulated with thrombin (IIa), CVX plus IIa, or A23187. The platelet pellet (P) and releasate (R) were separated by centrifugation. FXIII-A was visualized by immunoblotting and quantified by densitometry. (A) Representative immunoblots of FXIII-A from the pellet (1.5 × 105 platelets) or releasate (7.5 × 105 platelets). (B-C) Quantification of total FXIII-A in the pellet and releasate, respectively (mean ± SEM; n = 5 separate donors; same symbols in both panels; P values vs unstimulated platelets at the same time point are indicated). (D-F) Washed human platelets were unstimulated (Unstim) or stimulated with CVX plus IIa in the presence of cycloheximide (cyclo) or vehicle (Veh [ethanol]). Samples were processed as those in panels A-C. (D) Representative immunoblots of FXIII-A. For analysis of the pellet, proteins from ∼2 × 105 platelets were loaded. For analysis of the releasate, supernatant from 1 × 106 platelets were loaded. (E-F) Quantification of total FXIII-A in the pellet and releasate, respectively (mean ± SEM; n = 6 separate donors; same symbols in both panels; P = .05 vs convulxin plus thrombin in the absence of cycloheximide at the same time point; the slight increase in FXIII-A in the pellet in the absence of cycloheximide at 30 minutes is likely an artifact because this is too short of a time frame for significant protein synthesis). For both immunoblots, rhFXIII-A is recombinant human FXIII-A loading control, and the band in the MWM lane indicates 100 kDa. FXIII-A species are labeled on the right of the immunoblot as (O) (representing zymogen FXIII-A or nonproteolytically activated FXIII-A°) and ∗ (representing FXIII-A∗).](https://ash.silverchair-cdn.com/ash/content_public/journal/bloodadvances/8/19/10.1182_bloodadvances.2024012979/1/blooda_adv-2024-012979-gr2.jpeg?Expires=1730446353&Signature=32ZDDFCA4t5PfAC7R00ENMi-c-Kji8o~5KDGdoOqrME0r4fhQA14hxRrV1lo9bpJVtwSEjIl1vMoy9PUt7EIUUk9H5oho2YjhJk8BcNmgRpGsxJunAbVfXmWu1xrtQHAIOqauKz7P8GIBVgTa6ZLuD1~21BiOVFfBS~NTE0Sb6Joq5yHrdq5bVTFqFLeNrajeP6uCIuhgep58da-yVtMfVSDvcMz9DRsjKlZKJri-XooccFXmdhdD1r0nmpp6REdbjUqznWmC7bFJ83ue~qd3HN7r10w3QrMxGT8yJcxeAaZT8r9zHt3l5c0YQNTyQJDqNBisyRT~7CzYaWhOod4Sw__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
Platelet FXIII-A is not synthesized during activation of human platelets. (A-C) Washed human platelets were unstimulated (Unstim) or stimulated with thrombin (IIa), CVX plus IIa, or A23187. The platelet pellet (P) and releasate (R) were separated by centrifugation. FXIII-A was visualized by immunoblotting and quantified by densitometry. (A) Representative immunoblots of FXIII-A from the pellet (1.5 × 105 platelets) or releasate (7.5 × 105 platelets). (B-C) Quantification of total FXIII-A in the pellet and releasate, respectively (mean ± SEM; n = 5 separate donors; same symbols in both panels; P values vs unstimulated platelets at the same time point are indicated). (D-F) Washed human platelets were unstimulated (Unstim) or stimulated with CVX plus IIa in the presence of cycloheximide (cyclo) or vehicle (Veh [ethanol]). Samples were processed as those in panels A-C. (D) Representative immunoblots of FXIII-A. For analysis of the pellet, proteins from ∼2 × 105 platelets were loaded. For analysis of the releasate, supernatant from 1 × 106 platelets were loaded. (E-F) Quantification of total FXIII-A in the pellet and releasate, respectively (mean ± SEM; n = 6 separate donors; same symbols in both panels; P = .05 vs convulxin plus thrombin in the absence of cycloheximide at the same time point; the slight increase in FXIII-A in the pellet in the absence of cycloheximide at 30 minutes is likely an artifact because this is too short of a time frame for significant protein synthesis). For both immunoblots, rhFXIII-A is recombinant human FXIII-A loading control, and the band in the MWM lane indicates 100 kDa. FXIII-A species are labeled on the right of the immunoblot as (O) (representing zymogen FXIII-A or nonproteolytically activated FXIII-A°) and ∗ (representing FXIII-A∗).
