Effects of histatin-1 peptide on human corneal epithelial cells

Shah, Dhara; Ali, Mohsin; Shukla, Deepak; Jain, Sandeep; Aakalu, Vinay K.

doi:10.1371/journal.pone.0178030

Cited by 26 publications

(41 citation statements)

References 23 publications

(44 reference statements)

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“…However, due to the large variety of biomaterials, there is still an apparent great need for broadly applicable approaches to promote cell spreading on biomaterials. Previously, we and others showed that Hst1 promoted adhesion, spreading, and migration of various epithelial cells from different origins, such as mucosa , gingiva , cornea , and skin , endothelial cells , and osteogenic cells . All together, these findings underline a non‐cell type‐specific character of Hst1 rendering a promising application potential for tissue engineering purposes.…”

Section: Resultssupporting

confidence: 52%

“…A promising candidate cell‐targeting agent to promote cell–substrate interactions is histatin‐1 (Hst1), a member of a large histidine‐rich salivary peptide family. Our previous findings show that Hst1 can significantly promote the attachment, spreading, and migration of various cell types including epithelial, endothelial, and osteogenic cells . Our recent data confirm that Hst1 can promote the spreading of osteogenic cells on both bio‐inert glass and titanium surface , which suggests a promising application potential of Hst1 in the cell‐based bone tissue engineering.…”

supporting

confidence: 65%

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All‐trans retinoic acid and human salivary histatin‐1 promote the spreading and osteogenic activities of pre‐osteoblasts in vitro

Sun

Shi

et al. 2020

FEBS Open Bio

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Cell‐based bone tissue engineering techniques utilize both osteogenic cells and biomedical materials, and have emerged as a promising approach for large‐volume bone repair. The success of such techniques is highly dependent on cell adhesion, spreading, and osteogenic activities. In this study, we investigated the effect of co‐administration of all‐trans retinoic acid (ATRA) and human salivary peptide histatin‐1 (Hst1) on the spreading and osteogenic activities of pre‐osteoblasts on bio‐inert glass surfaces. Pre‐osteoblasts (MC3T3‐E1 cell line) were seeded onto bio‐inert glass slides in the presence and absence of ATRA and Hst1. Cell spreading was scored by measuring surface areas of cellular filopodia and lamellipodia using a point‐counting method. The distribution of fluorogenic Hst1 within osteogenic cells was also analyzed. Furthermore, specific inhibitors of retinoic acid receptors α, β, and γ, such as ER‐50891, LE‐135, and MM‐11253, were added to identify the involvement of these receptors. Cell metabolic activity, DNA content, and alkaline phosphatase (ALP) activity were assessed to monitor their effects on osteogenic activities. Short‐term (2 h) co‐administration of 10 μm ATRA and Hst1 to pre‐osteoblasts resulted in significantly higher spreading of pre‐osteoblasts compared to ATRA or Hst1 alone. ER‐50891 and LE‐135 both nullified these effects of ATRA. Co‐administration of ATRA and Hst1 was associated with significantly higher metabolic activity, DNA content, and ALP activity than either ATRA or Hst1 alone. In conclusion, co‐administration of Hst1 with ATRA additively stimulated the spreading and osteogenicity of pre‐osteoblasts on bio‐inert glass surfaces in vitro.

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Section: Resultssupporting

confidence: 52%

supporting

confidence: 65%

All‐trans retinoic acid and human salivary histatin‐1 promote the spreading and osteogenic activities of pre‐osteoblasts in vitro

Sun

Shi

et al. 2020

FEBS Open Bio

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“…Comparable cell activating effects for Hst1 and Hst2 have also been found on endothelial cells, fibroblasts and osteogenic cells [5,12]. Hst1 also stimulates cell metabolic activity [13] and maintains cell viability under various adverse conditions, such as the presence of zoledronic acid [14] or ultraviolet radiation [15]. Interestingly, Hst1 and Hst2 are internalized in epithelial cells [2,7] in contrast to the D-enantiomer of Hst2 (D-Hst2), which can not promote the migration of epithelial cells and neither is internalized by the cells [3].…”

Section: Introductionmentioning

confidence: 88%

“…From the above described results it may be deducted that the absence of amino sequences 1-11 in Hst2 and 23-38 in Hst5 (compared to Hst1) dramatically compromised their uptake rates. Consequently, we assessed the uptake dynamics and subcellular targets of truncated variants, F-Hst1 1-11 , F-Hst1 [12][13][14][15][16][17][18][19][20][21][22] and F-Hst1 [23][24][25][26][27][28][29][30][31][32][33][34][35][36][37][38] to explore their role in the cellular uptake of Hst1, Hst2 and Hst5. CLSM images revealed that the uptake of the truncated variants F-Hst1 1-11 , F-Hst1 12-22 and F-Hst1 [23][24][25][26][27][28][29][30][31][32][33][34][35][36][37][38] was much lower than that of the whole molecule F-Hst1 ( Figure 7A-D).…”

Section: Uptake Dynamics and Subcellular Target Of Truncated F-hsts mentioning

confidence: 99%

“…At 60 min post-incubation Hst1 showed a mean fluorescence of 2.00 ± 0.15 × 10 6 AFU, which was significantly higher than that of F-Hst1 12-22 (0.25 ± 0.03 × 10 6 AFU), F-Hst1 1-11 (0.07 ± 0.00 × 10 6 AFU) and F-Hst1 23-38 (0.07 ± 0.00 × 10 6 AFU) ( Figure 7F). F-Hst1 [12][13][14][15][16][17][18][19][20][21][22] mainly co-localized with the lysosomal marker (P coloc value of 0.55 ± 0.12, not with markers for the mitochondria or the ER or Golgi (Figure 8). Figure 7.…”

Section: Uptake Dynamics and Subcellular Target Of Truncated F-hsts mentioning

confidence: 99%

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Salivary Histatin 1 and 2 Are Targeted to Mitochondria and Endoplasmic Reticulum in Human Cells

Sun

Nazmi

et al. 2020

Cells

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Human salivary histatin 1 (Hst1) and Hst2 exhibit a series of cell-activating properties (e.g., promoting adhesion, spreading, migration and metabolic activity of mammalian cells). In contrast, Hst5 shows an anti-fungal property but no cell-activating properties. Previous findings suggest that their uptake and association with subcellular targets may play a determinant role in their functions. In this study, we studied the uptake dynamics and subcellular targets of Hst1, Hst2 and Hst5 in epithelial cells (HO1N1 human buccal carcinoma epithelial cell line). Confocal laser scanning microscopy (CLSM) revealed that fluorescently labeled Hst1 (F-Hst1) was taken up into the intracellular space of epithelial cells. Then, 60 min post-incubation, the total fluorescence of cell-associated F-Hst1, as measured using flow cytometry, was significantly higher compared to those of F-Hst2 and F-Hst5. In contrast, virtually no association occurred using the negative control—scrambled F-Hst1 (F-Hstscr). CLSM images revealed that F-Hst1, 2 and 5 co-localized with mitotrackerTM-labeled mitochondria. In addition, F-Hst1 and F-Hst2 but neither F-Hst5 nor F-Hst1scr co-localized with the ER-trackerTM-labeled endoplasmic reticulum. No co-localization of Hst1, 2 and 5 with lysosomes or the Golgi apparatus was observed. Furthermore, Hst1 and Hst2 but not Hst5 or Hst1scr significantly promoted the metabolic activity of both human epithelial cell lines, HaCaT human keratinocytes and primary human gingival fibroblasts.

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Human salivary histatin‐1 (Hst1) promotes bone morphogenetic protein 2 (BMP2)‐induced osteogenesis and angiogenesis

et al. 2020

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Large‐volume bone defects can result from congenital malformation, trauma, infection, inflammation and cancer. At present, it remains challenging to treat these bone defects with clinically available interventions. Allografts, xenografts and most synthetic materials have no intrinsic osteoinductivity, and so an alternative approach is to functionalize the biomaterial with osteoinductive agents, such as bone morphogenetic protein 2 (BMP2). Because it has been previously demonstrated that human salivary histatin‐1 (Hst1) promotes endothelial cell adhesion, migration and angiogenesis, we examine here whether Hst1 can promote BMP2‐induced bone regeneration. Rats were given subcutaneous implants of absorbable collagen sponge membranes seeded with 0, 50, 200 or 500 μg Hst1 per sample and 0 or 2 μg BMP2 per sample. At 18 days postsurgery, rats were sacrificed, and implanted regional tissue was removed for micro computed tomography (microCT) analyses of new bone (bone volume, trabecular number and trabecular separation). Four samples per group were decalcified and subjected to immunohistochemical staining to analyze osteogenic and angiogenic markers. We observed that Hst1 increased BMP2‐induced new bone formation in a dose‐dependent manner. Co‐administration of 500 μg Hst1 and BMP2 resulted in the highest observed bone volume and trabecular number, the lowest trabecular separation and the highest expression of osteogenic markers and angiogenic markers. Our results suggest that coadministration of Hst1 may enhance BMP2‐induced osteogenesis and angiogenesis, and thus may have potential for development into a treatment for large‐volume bone defects.

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Effects of histatin-1 peptide on human corneal epithelial cells

Cited by 26 publications

References 23 publications

All‐trans retinoic acid and human salivary histatin‐1 promote the spreading and osteogenic activities of pre‐osteoblasts in vitro

All‐trans retinoic acid and human salivary histatin‐1 promote the spreading and osteogenic activities of pre‐osteoblasts in vitro

Salivary Histatin 1 and 2 Are Targeted to Mitochondria and Endoplasmic Reticulum in Human Cells

Human salivary histatin‐1 (Hst1) promotes bone morphogenetic protein 2 (BMP2)‐induced osteogenesis and angiogenesis

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