Selection and identification of a novel bone-targeting peptide for biomedical imaging of bone

Bang, Jinho; Park, Hee Sun; Yoo, Jin‐Hong; Lee, Dong-Hyun; Choi, Won Il; Lee, Jin Hyung; Lee, Young Ran; Kim, Chungho; Koo, Heebeom; Kim, Sung-Hyun

doi:10.1038/s41598-020-67522-4

Cited by 9 publications

(3 citation statements)

References 39 publications

(36 reference statements)

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“…have also discussed the role of noncollagenous proteins enriched with acidic and phosphorylated amino acid in regulating the nucleation and growth of HAp for bone mineralization. Bang et al have compared the HAp binding affinities of a set of peptides with positive (basic amino acids) and negative charge (acidic amino acids) and illustrated that the positively charged peptides (KNFQSRSH) exhibited better binding with HAp . Gungormus et al also reported the ionic interaction of positively charged, histidine-binding peptides with phosphates of HAp .…”

Section: Resultsmentioning

confidence: 99%

Investigating the Role of Amino Acids in Short Peptides for Hydroxyapatite Binding and Osteogenic Differentiation of Mesenchymal Stem Cells to Aid Bone Regeneration

Halder,

Singh,

Negi

et al. 2024

Biomacromolecules

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Bone defects show a slow rate of osteoconduction and imperfect reconstruction, and the current treatment strategies to treat bone defects suffer from limitations like immunogenicity, lack of cell adhesion, and the absence of osteogenic activity. In this context, bioactive supramolecular peptides and peptide gels offer unique opportunities to develop biomaterials that can play a dominant role in the biomineralization of bone tissues and promote bone formation. In this article, we have demonstrated the potential of six tetrapeptides for specific binding to hydroxyapatite (HAp), a major inorganic component of the bone, and their effect on the growth and osteogenic differentiation of mesenchymal stem cells (MSCs). We adopted a simplistic approach of rationally designing amphiphilic peptides by incorporating amino acids, Ser, pSer, Pro, Hyp, Asp, and Glu, which are present in either collagenous or noncollagenous proteins and render properties like antioxidant,

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Section: Resultsmentioning

confidence: 99%

Investigating the Role of Amino Acids in Short Peptides for Hydroxyapatite Binding and Osteogenic Differentiation of Mesenchymal Stem Cells to Aid Bone Regeneration

Halder,

Singh,

Negi

et al. 2024

Biomacromolecules

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“…As revealed using the fourth Garnier–Osguthorpe–Robson algorithm (GOR4), out of the entire AP-2 family, AP-2δ has the largest number of extended strands but the smallest of random coils ( Figure 2 E). Bang et al suggested that binding affinity could be elevated with the increase of extended strands in secondary structure [ 38 ]. Particular attention was also given to the amino acids preceding the conserved “TF_AP-2” domain; these were evaluated for their similarity, physicochemical properties, and structural characteristics ( Figure 3 ).…”

Section: Resultsmentioning

confidence: 99%

AP-2δ Is the Most Relevant Target of AP-2 Family-Focused Cancer Therapy and Affects Genome Organization

Kołat

Zhao

Kciuk

et al. 2022

Cells

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Formerly hailed as “undruggable” proteins, transcription factors (TFs) are now under investigation for targeted therapy. In cancer, this may alter, inter alia, immune evasion or replicative immortality, which are implicated in genome organization, a process that accompanies multi-step tumorigenesis and which frequently develops in a non-random manner. Still, targeting-related research on some TFs is scarce, e.g., among AP-2 proteins, which are known for their altered functionality in cancer and prognostic importance. Using public repositories, bioinformatics tools, and RNA-seq data, the present study examined the ligandability of all AP-2 members, selecting the best one, which was investigated in terms of mutations, targets, co-activators, correlated genes, and impact on genome organization. AP-2 proteins were found to have the conserved “TF_AP-2” domain, but manifested different binding characteristics and evolution. Among them, AP-2δ has not only the highest number of post-translational modifications and extended strands but also contains a specific histidine-rich region and cleft that can received a ligand. Uterine, colon, lung, and stomach tumors are most susceptible to AP-2δ mutations, which also co-depend with cancer hallmark genes and drug targets. Considering AP-2δ targets, some of them were located proximally in the spatial genome or served as co-factors of the genes regulated by AP-2δ. Correlation and functional analyses suggested that AP-2δ affects various processes, including genome organization, via its targets; this has been eventually verified in lung adenocarcinoma using expression and immunohistochemistry data of chromosomal conformation-related genes. In conclusion, AP-2δ affects chromosomal conformation and is the most appropriate target for cancer therapy focused on the AP-2 family.

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“…In another example, Bang et al identified a supposedly highly specific HA-binding peptide via phage display and combined it with the fluorescent Cy5.5 dye. 180 During in vivo real-time wholebody imaging, the conjugate showed preferential binding for bone tissues. The development of probes for nuclear imaging was also attempted, but with unsatisfactory results.…”

Section: Biomedical Applications Of Solid-binding Peptidesmentioning

confidence: 99%

A sticky tale : Biomaterial coatings from modular proteins

Alvisi¹

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Selection and identification of a novel bone-targeting peptide for biomedical imaging of bone

Cited by 9 publications

References 39 publications

Investigating the Role of Amino Acids in Short Peptides for Hydroxyapatite Binding and Osteogenic Differentiation of Mesenchymal Stem Cells to Aid Bone Regeneration

Investigating the Role of Amino Acids in Short Peptides for Hydroxyapatite Binding and Osteogenic Differentiation of Mesenchymal Stem Cells to Aid Bone Regeneration

AP-2δ Is the Most Relevant Target of AP-2 Family-Focused Cancer Therapy and Affects Genome Organization

A sticky tale : Biomaterial coatings from modular proteins

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