Kindlin-3 Deficiency leads to Impaired Erythropoiesis and Erythrocyte Cytoskeleton

Authors

Chloe Turpin, Case Western Reserve University
Utku Goreke, Case Western Reserve University
Utku Goreke, Case Western Reserve University
Katarzyna Bialkowska, Case Western Reserve UniversityFollow
Kamila M. Bledzka, Case Western Reserve UniversityFollow
Dmitriy Verbovetskiy, Case Western Reserve University
Umut A. Gurkan, Case Western Reserve UniversityFollow
Jun Qin, Case Western Reserve UniversityFollow
Edward F. Plow, Case Western Reserve UniversityFollow
Elzbieta Pluskota, Case Western Reserve UniversityFollow

Document Type

Article

Publication Date

4-27-2023

Abstract

Kindlin-3 (K3) is critical for the activation of integrin adhesion receptors in hematopoietic cells. In humans and mice, K3 deficiency is associated with impaired immunity and bone development, bleeding, and aberrant erythrocyte shape. To delineate how K3 deficiency (K3KO) contributes to anemia and misshaped erythrocytes, mice deficient in erythroid (K3KO\EpoR-cre) or myeloid cell K3 (K3KO\Lyz2cre), knockin mice expressing mutant K3 (Q597W598 to AA) with reduced integrin-activation function (K3KI), and control wild-type (WT) K3 mice were studied. Both K3-deficient strains and K3KI mice showed anemia at baseline, reduced response to erythropoietin stimulation, and compromised recovery after phenylhydrazine (PHZ)-induced hemolytic anemia as compared with K3WT. Erythroid K3KO and K3 (Q597W598 to AA) showed arrested erythroid differentiation at proerythroblast stage, whereas macrophage K3KO showed decreased erythroblast numbers at all developmental stages of terminal erythroid differentiation because of reduced erythroblastic island (EBI) formation attributable to decreased expression and activation of erythroblast integrin α4β1 and macrophage αVβ3. Peripheral blood smears of K3KO\EpoRcre mice, but not of the other mouse strains, showed numerous aberrant tear drop–shaped erythrocytes. K3 deficiency in these erythrocytes led to disorganized actin cytoskeleton, reduced deformability, and increased osmotic fragility. Mechanistically, K3 directly interacted with F-actin through an actin-binding site K3-LK48. Taken together, these findings document that erythroid and macrophage K3 are critical contributors to erythropoiesis in an integrin-dependent manner, whereas F-actin binding to K3 maintains the membrane cytoskeletal integrity and erythrocyte biconcave shape. The dual function of K3 in erythrocytes and in EBIs establish an important functional role for K3 in normal erythroid function.

Language

English

Publication Title

Blood Advances

Grant

HL HL096062

Rights

© 2023 by The American Society of Hematology. This is an open access article under the CC BY-NC-ND license (https://creativecommons.org/licenses/BY-NC-ND/4.0/), which permits non-commercial copying and redistribution of the material in any medium or format, provided the original work is not changed in any way and is properly cited.

Creative Commons License

This work is licensed under a Creative Commons Attribution-NonCommercial-No Derivative Works 4.0 International License.

Recommended Citation

Dorota Szpak, Chloe Turpin, Utku Goreke, Katarzyna Bialkowska, Kamila M. Bledzka, Dmitriy Verbovetskiy, Narla Mohandas, Umut A. Gurkan, Jun Qin, Edward F. Plow, Elzbieta Pluskota; Kindlin-3 deficiency leads to impaired erythropoiesis and erythrocyte cytoskeleton. Blood Adv 2023; 7 (9): 1739–1753. doi: https://doi.org/10.1182/bloodadvances.2022008498