Your search keyword '"Lyp-1"' showing total 20 results

1. Enhancing the Stability of Tumor Homing LyP-1 Peptide Using Cyclization and Retro Grafting Strategies.

Author

Kara, Şeyda, Ayazoglu Demir, Elif, Celik Uzuner, Selcen, and Akcan, Muharrem

Abstract

Anticancer peptide therapeutics are promising candidates for cancer treatment as they are highly specific to their targets and can have tumor-homing abilities. Several studies have been shown that a nine-residue tumor-homing LyP-1 peptide can be used in anticancer agent development and in tumor imaging studies. However, because it is a small linear peptide, it is very unstable in serum as most of the peptide therapeutics face before they enter to clinical studies. The main aim of this study is to enhance the serum stability of LyP-1 using cyclization and grafting (and/or retro grafting) strategies. Four grafted versions onto sunflower trypsin inhibitor peptide SFTI-1 and a cyclic homodimerized version of LyP-1 were synthesized and tested on MDA-MB-435S cancer (melanoma) cells and HFF-1 normal fibroblast cells in comparison with cisplatin chemotherapeutics. The cyclic homodimer LyP-1 peptide exhibited extraordinary stability in serum. Additionally, the retro grafted peptides have also improved stability that indicates the retro sequence concept provides peptides with higher stability. [ABSTRACT FROM AUTHOR]

Published

2023

2. Recent progress in LyP-1-based strategies for targeted imaging and therapy

Author

Ningning Song, Lingzhou Zhao, Meilin Zhu, and Jinhua Zhao

Subjects

lyp-1, tumor, metastatic lesions, atherosclerotic plaque, diagnosis and therapeutics, Therapeutics. Pharmacology, RM1-950

Abstract

The identification of markers expressed by pathological cells or their microenvironment would help to distinguish such cells from the normal tissues. The strategies derived from this theory can be a promising modality for imaging and treating diseases. LyP-1, a tumor homing peptide, can selectively bind to its receptor p32 protein overexpressed in various tumor-associated cells and atherosclerotic plaque macrophages. During recent decades, multiple types of LyP-1-based imaging probes and drug delivery systems have been designed and developed for diagnostic and therapeutic applications. This review first introduces LyP-1 and its receptor p32, as well as its homing, internalization and proapoptotic properties. Next, we highlight recent studies focusing on the applications of LyP-1-based strategies in the diagnosis and treatment of tumors, metastatic lesions, and atherosclerotic plaques. Finally, several limitations in the clinical translation of LyP-1-based bioconjugates are summarized.

Published

2019

3. LyP-1-Modified Oncolytic Adenoviruses Targeting Transforming Growth Factor β Inhibit Tumor Growth and Metastases and Augment Immune Checkpoint Inhibitor Therapy in Breast Cancer Mouse Models.

Author

Xu, Weidong, Yang, Yuefeng, Hu, Zebin, Head, Maria, Mangold, Kathy A., Sullivan, Megan, Wang, Edward, Saha, Poornima, Gulukota, Kamalakar, Helseth, Donald L., Guise, Theresa, Prabhkar, Bellur S., Kaul, Karen, Schreiber, Hans, and Seth, Prem

Subjects

*IMMUNE checkpoint inhibitors, *TRANSFORMING growth factors, *BREAST cancer, *METASTASIS, *TUMOR growth, *PROGRAMMED cell death 1 receptors, *ADENOVIRUS diseases

Abstract

We report here the development of oncolytic adenoviruses (Ads) that have reduced toxicity, enhanced tumor tropism, produce strong antitumor response, and can overcome resistance to immune checkpoint inhibitor therapy in breast cancer. We have shown that LyP-1 receptor (p32) is highly expressed on the surface of breast cancer cells and tumors from cancer patients, and that increased stromal expression of transforming growth factor β-1 (TGFβ-1) is associated with triple-negative breast cancer. Therefore, we constructed oncolytic Ads, AdLyp.sT and mHAdLyp.sT, in which the p32-binding LyP-1 peptide was genetically inserted into the adenoviral fiber protein. Both AdLyp.sT and mHAdLyp.sT express sTGFβRIIFc, a TGFβ decoy that can inhibit TGFβ pathways. mHAdLyp.sT is an Ad5/48 chimeric hexon virus in which hypervariable regions (HVRs 1–7) of Ad5 are replaced with the corresponding Ad48 HVRs. AdLyp.sT and mHAdLyp.sT exhibited better binding, replication, and produced higher sTGFβRIIFc protein levels in breast cancer cell lines compared with Ad.sT or mHAd.sT control viruses without LyP-1 peptide modification. Systemic delivery of mHAdLyp.sT in mice resulted in reduced hepatic/systemic toxicity compared with Ad.sT and AdLyp.sT. Intravenous delivery of AdLyp.sT and mHAdLyp.sT elicited a strong antitumor response in a human MDA-MB-231 bone metastasis model in mice, as indicated by bioluminescence imaging, radiographic tumor burden, serum TRACP 5b and calcium, and body weight analyses. Furthermore, intratumoral delivery of AdLyp.sT in 4T1 model in immunocompetent mice inhibited tumor growth and metastases, and augmented anti-PD-1 and anti-CTLA-4 therapy. Based on these studies, we believe that AdLyp.sT and mHAdLyp.sT can be developed as potential targeted immunotherapy agents for the treatment of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2020

4. Recent progress in LyP-1-based strategies for targeted imaging and therapy.

Author

Song, Ningning, Zhao, Lingzhou, Zhu, Meilin, and Zhao, Jinhua

Subjects

*DRUG delivery systems, *ATHEROSCLEROTIC plaque, *MOLECULAR probes, *BIOCONJUGATES, *PROTEIN receptors, *TUMOR treatment

Abstract

The identification of markers expressed by pathological cells or their microenvironment would help to distinguish such cells from the normal tissues. The strategies derived from this theory can be a promising modality for imaging and treating diseases. LyP-1, a tumor homing peptide, can selectively bind to its receptor p32 protein overexpressed in various tumor-associated cells and atherosclerotic plaque macrophages. During recent decades, multiple types of LyP-1-based imaging probes and drug delivery systems have been designed and developed for diagnostic and therapeutic applications. This review first introduces LyP-1 and its receptor p32, as well as its homing, internalization and proapoptotic properties. Next, we highlight recent studies focusing on the applications of LyP-1-based strategies in the diagnosis and treatment of tumors, metastatic lesions, and atherosclerotic plaques. Finally, several limitations in the clinical translation of LyP-1-based bioconjugates are summarized. [ABSTRACT FROM AUTHOR]

Published

2019

5. Foam Cell Targeted Liposomes Co-Encapsulating Superoxide Dismutase and Catalase to Attenuate Atherosclerosis by Inhibiting Oxidative Stress.

Author

Zhang S, Liu D, Zhang J, Liu S, Sun R, Huo R, and Cui C

Subjects

Animals, Foam Cells, Liposomes pharmacology, Superoxide Dismutase pharmacology, Catalase pharmacology, Antioxidants therapeutic use, Antioxidants pharmacology, Reactive Oxygen Species, Oxidative Stress, Lipoproteins, LDL pharmacology, Atherosclerosis drug therapy, Plaque, Atherosclerotic

Abstract

Background: Oxidative stress, propelled by reactive oxygen species (ROS), serves as a significant catalyst for atherosclerosis (AS), a primary contributor to vascular diseases on a global scale. Antioxidant therapy via nanomedicine has emerged as a pivotal approach in AS treatment. Nonetheless, challenges such as inadequate targeting, subpar biocompatibility, and limited antioxidant effectiveness have restrained the widespread utilization of nanomedicines in AS treatment. This study aimed to synthesize a specialized peptide-modified liposome capable of encapsulating two antioxidant enzymes, intending to enhance targeted antioxidant therapy for AS., Methods: The film dispersion method was employed for liposome preparation. Fluorescence quantification was conducted to assess the drug encapsulation rate. Characterization of liposome particle size was performed using dynamic light scattering (DLS) and transmission electron microscopy (TEM). Laser confocal microscopy and flow cytometry were utilized to analyze liposome cell uptake and target foam cells. Antioxidant analysis was conducted using 2',7'-Dichlorodihydrofluorescein diacetate (DCFH-DA) staining, while pro-lipid efflux analysis utilized Oil Red O (ORO) staining. Safety evaluation was performed using Hematoxylin and Eosin (H&E) staining. The level of inflammatory factors was determined through enzyme-linked immunosorbent assay (ELISA). The degree of lipid oxidation at the cellular level was assessed using the malonaldehyde (MDA) assay. In vivo targeting analysis was conducted using small animal live imaging., Results: Our in vitro and in vivo findings substantiated that the modification of Lyp-1 led to increased delivery of antioxidant enzymes into foam cells ( p < 0.05), the primary pathological cells within AS plaques. Upon accumulation in foam cells, liposomes loaded with superoxide dismutase (SOD) and catalase (CAT) (LyP-lip@SOD/CAT) effectively mitigated excess ROS and shielded macrophages from ROS-induced damage ( p < 0.01). Furthermore, the reduction in ROS levels notably hindered the endocytosis of oxidized low-density lipoprotein (Ox-LDL) by activated macrophages, subsequently alleviating lipid accumulation at atherosclerotic lesion sites, evident from both in vitro and in vivo ORO staining results ( p < 0.01). LyP-lip@SOD/CAT significantly curbed the secretion of inflammatory factors at the plaque site ( p < 0.001). Additionally, LyP-lip@SOD/CAT demonstrated commendable biological safety., Conclusions: In this study, we effectively synthesized LyP-lip@SOD/CAT and established its efficacy as a straightforward and promising nano-agent for antioxidant therapy targeting atherosclerosis.

Published

2024

6. Efficacy of a novel LyP-1-containing self-microemulsifying drug delivery system (SMEDDS) for active targeting to breast cancer.

Author

Timur, Selin S., Yöyen-Ermiş, Diğdem, Esendağlı, Güldal, Yonat, Selcen, Horzum, Utku, Esendağlı, Güneş, and Gürsoy, R. Neslihan

Subjects

*BREAST cancer, *DRUG delivery systems, *METASTASIS, *LYMPHATICS

Abstract

Graphical abstract Abstract An ideal cancer therapy targets the tumor cells selectively without damaging healthy tissues. Even though the tumor-specific markers are limited, these molecules can be used for the delivery of anti-cancer drugs as an active targeting strategy. Since the lymphatic system plays a critical role in the dissemination of cancer cells, the drugs directed through lymphatics can feasibly reach to the sites of metastasis. LyP-1 is a peptide that binds to the p32 receptor which is highly expressed not only on the lymphatic endothelium but also on the malignant cells; thus, making this peptide ligand a preferable candidate to mediate active targeting of lymphatics and cancer cells. In this study, different formulations of LyP-1 containing lipid-based nanopharmaceutics so-called self-microemulsifying drug delivery systems (SMEDDS) were developed and tested for their efficacy in targeting breast cancer. Following the selection of non-toxic formulation, doxorubicin hydrochloride and LyP-1 were co-administered in the SMEDDS, which resulted in a significant increase in in vitro cytotoxicity in p32-expressing breast cancer cells, 4T1 and MDA-MB-231. Accordingly, the uptake of LyP-1 in the SMEDDS by the cancer cells was demonstrated. The expression of p32 was detected in the 4T1 tumor tissues which were efficiently targeted with LyP-1 in the SMEDDS. When doxorubicin was co-administrated with LyP-1 in SMEDDS via intraperitonial administration, tumor growth and metastasis were significantly reduced. In conclusion, a novel and efficacious SMEDDS formulation containing LyP-1 with a droplet size less than 100 nm was developed for the lymphatic targeting of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2019

7. A targeted nanoplatform co-delivering chemotherapeutic and antiangiogenic drugs as a tool to reverse multidrug resistance in breast cancer.

Author

Tian, Fengchun, Dahmani, Fatima Zohra, Qiao, Jianan, Ni, Jiang, Xiong, Hui, Liu, Tengfei, Zhou, Jianping, and Yao, Jing

Subjects

DRUG delivery systems, HEPARIN, MULTIDRUG resistance, QUERCETIN, CELL proliferation

Abstract

Several obstacles are currently impeding the successful treatment of breast cancer, namely impaired drug accumulation into the tumor site, toxicity to normal cells and narrow therapeutic index of chemotherapy, multidrug resistance (MDR) and the metastatic spread of cancer cells through the blood and lymphatic vessels. In this regard, we designed a novel multifunctional nano-sized drug delivery system based on LyP-1 peptide-modified low-molecular-weight heparin-quercetin conjugate (PLQ). This nanosystem was developed for targeted co-delivery of multiple anticancer drugs to p32-overexpressing tumor cells and peritumoral lymphatic vessels, using LyP-1 peptide as active targeting ligand, with the aim to achieve a targeted combinatorial chemo/angiostatic therapy and MDR reversal. The cellular uptake of PLQ nanoparticles by p32-overexpressing breast cancer cells was significantly higher than nonfunctionalized nanoparticles. Besides, the anti-angiogenic activity of PLQ nanoparticles was proven by the effective inhibition of the bFGF-induced neovascularization in subcutaneous Matrigel plugs. More importantly, PLQ/GA nanoparticles with better targeting ability toward p32-positive tumors, displayed a high antitumor outcome by inhibition of tumor cells proliferation and angiogenesis. Immunohistochemistry and western blot assay showed that PLQ/GA nanoparticles significantly disrupted the lymphatic formation of tumor, and inhibited the P-glycoprotein (P-gp) expression in MCF-7 tumor cells, respectively. In conclusion, PLQ/GA nanoparticles provide a synergistic strategy for effective targeted co-delivery of chemotherapeutic and antiangiogenic agents and reversing MDR and metastasis in breast cancer. Statement of Significance Herein, we successfully developed a novel amphiphilic nanomaterial, LyP-1-LMWH-Qu (PLQ) conjugate, consisting of a tumor-targeting moiety LyP-1, a hydrophobic quercetin (a multidrug resistance [MDR]–reversing drug) inner core, and a hydrophilic low-molecular-weight heparin (an antiangiogenic agent) outer shell for encapsulating and delivering a hydrophobic chemotherapeutic agent (gambogic acid). This versatile nanoplatform with multiple targeted features, i.e., dual chemo/angiostatic effects, destruction ability of the peritumoral lymphatic vessels, and reversal of MDR, resulted in a significantly stronger antitumor efficacy and lower toxic side effect than those of nontargeted nanoparticles and the free drug solution. Therefore, this versatile nanosystem might provide a novel insight for the treatment and palliation of breast cancer by targeted co-delivery of chemo/antiangiogenic agents and reversing MDR and metastasis. [ABSTRACT FROM AUTHOR]

Published

2018

8. LyP-1-conjugated Fe 3 O 4 nanoparticles suppress tumor growth by magnetic induction hyperthermia.

Author

Teo, Peishan, Wang, Xiaowen, Zhang, Jieying, Zhang, Han, Yang, Xin, Huang, Yun, and Tang, Jintian

Subjects

*MAGNETIC nanoparticle hyperthermia, *SUPERPARAMAGNETIC materials, *POLYETHYLENE glycol, *IRON oxide nanoparticles, *CANCER

Abstract

To find a promising drug carrier to suppress tumor using magnetic induction hyperthermia (MIH) and targeted therapy, two superparamagnetic iron oxide nanoparticles (SPIONs) coated with polyethylene glycol (PEG) and LyP-1, respectively, were prepared and compared. The particle size ranges of PEG-SPIONs and LyP-1-SPIONs were 10–15 nm, and 15–20 nm, respectively. In FTIR spectra, PEG-SPIONs and LyP-1-SPIONs had strong peaks between 575 and 1630 cm−1. Specifically, the PEG-SPIONs mainly has peaks in 581 and 1630 cm−1. The LyP-1-SPIONs mainly had peaks in 575, 1050 and 1625 cm−1. The contents of Fe3O4in the PEG-SPIONs and LyP-1-SPIONs were about 94.24 and 89.26%, respectively. The iron contents in the MCF-7 and CT-26 cells were 33.1 ± 1.8 and 27.9 ± 0.95 pg, respectively, after co-incubation with LyP-1-SPIONs for 8 h. The LyP-1-SPIONs accumulated in the nucleus of MCF-7 cells while PEG-SPIONs in cytoplasma.In vitro, after 30 days we can found the tumor almost stopped to grow in Group LyP-1-SPIONs. LyP-1-SPIONs are promising in treating cancer as they accumulated in the nucleus of MCF-7 cells which expressed p32 and almost stopped tumor growth by combined MIH and targeted therapy. [ABSTRACT FROM PUBLISHER]

Published

2018

9. Magnetic mesoporous nanospheres anchored with LyP-1 as an efficient pancreatic cancer probe.

Author

Jiang, Yongjian, Liu, Shaojun, Zhang, Yu, Li, Hengchao, He, Hang, Dai, Juntao, Jiang, Tao, Ji, Weihang, Geng, Daoying, Elzatahry, Ahmed A., Alghamdi, Abdulaziz, Fu, Deliang, Deng, Yonghui, and Zhao, Dongyuan

Subjects

*THERAPEUTIC immobilization, *MESOPOROUS silica, *SUPERPARAMAGNETIC materials, *PANCREATIC cancer diagnosis, *MAGNETIC resonance imaging of cancer, *LABORATORY mice

Abstract

Immobilization of a ligand that selectively interacts with cancer cells to nanomaterials can enhance their diagnostic and therapeutic efficiency. In this study, we firstly demonstrate the high expression of receptor for cyclic nine-amino acid peptide LyP-1 (Cys-Gly-Asn-Lys-Arg-Thr-Arg-Gly-Cys) in both mouse and human pancreatic cancer. Based on these findings, sub-50 nm multifunctional superparamagnetic mesoporous nanospheres with surface modified with LyP-1 are rationally designed. Theses nanospheres have a core of silica-protected magnetite nanoparticle and a shell of FITC-labeled mesoporous silica, and they are able to specifically recognize and conjugate with the pancreatic cancer cell in vitro, as verified by the combined techniques of fluorescent imaging and T2 weight magnetic resonance imaging. After systematic administration, these LyP-1 immobilized nanospheres are found to actively target to mouse orthotopic xenograft of pancreatic cancer, which opens up the door for applications in early probing and diagnosis of pancreatic cancer by the multimodal imaging. [ABSTRACT FROM AUTHOR]

Published

2017

10. Dyslipidemia at the crossroad of the skin barrier and the arterial wall

Author

Martins Cardoso, R., Bouwstra, J.A., Eck, M. van, Irth, H., Kuiper, J., Smeden, J. van, Rensen, P.C.N., Vermonden, T., Mulder, T., and Leiden University

Subjects

Mice, Hypercholesterolemia, Liposomes, Lyp-1, Liver X receptor, Free fatty acids, Atherosclerosis, Skin barrier, Skin lipids

Abstract

The research described in this thesis shows that hypercholesterolemia, a well-established risk factor for atherosclerosis, can impact skin lipid pool and barrier function already at young age. In the field of atherosclerosis, we showed that the small peptide Lyp-1 can be used as a targeting molecule in liposomal formulations to deliver liver X receptor agonist to plaque resident foam cells/lipid-rich macrophages. Elucidation of the mechanisms underlying the intercommunication between plasma lipids and skin lipids may also bring valuable opportunities to prevent and treat dermatological pathologies in dyslipidemic patients; perhaps in combination with anti-atherogenic therapies. Thus, by deepening our knowledge we may improve our advice to the patients and ultimately improve their quality of life.

Published

2021

11. Recent progress in LyP-1-based strategies for targeted imaging and therapy

Author

Meilin Zhu, Jinhua Zhao, Ningning Song, and Lingzhou Zhao

Subjects

tumor, Metastatic lesions, media_common.quotation_subject, Normal tissue, Pharmaceutical Science, Apoptosis, Review Article, 02 engineering and technology, atherosclerotic plaque, Peptides, Cyclic, 030226 pharmacology & pharmacy, Mitochondrial Proteins, 03 medical and health sciences, Drug Delivery Systems, 0302 clinical medicine, Neoplasms, Animals, Humans, Medicine, Internalization, Receptor, media_common, business.industry, lcsh:RM1-950, metastatic lesions, General Medicine, LyP-1, 021001 nanoscience & nanotechnology, Plaque, Atherosclerotic, lcsh:Therapeutics. Pharmacology, Drug delivery, Cancer research, diagnosis and therapeutics, Tumor homing, Carrier Proteins, 0210 nano-technology, business, Biomarkers, Homing (hematopoietic)

Abstract

The identification of markers expressed by pathological cells or their microenvironment would help to distinguish such cells from the normal tissues. The strategies derived from this theory can be a promising modality for imaging and treating diseases. LyP-1, a tumor homing peptide, can selectively bind to its receptor p32 protein overexpressed in various tumor-associated cells and atherosclerotic plaque macrophages. During recent decades, multiple types of LyP-1-based imaging probes and drug delivery systems have been designed and developed for diagnostic and therapeutic applications. This review first introduces LyP-1 and its receptor p32, as well as its homing, internalization and proapoptotic properties. Next, we highlight recent studies focusing on the applications of LyP-1-based strategies in the diagnosis and treatment of tumors, metastatic lesions, and atherosclerotic plaques. Finally, several limitations in the clinical translation of LyP-1-based bioconjugates are summarized.

Published

2019

12. Complement Receptor Targeted Liposomes Encapsulating the Liver X Receptor Agonist GW3965 Accumulate in and Stabilize Atherosclerotic Plaques

Author

Benne, Naomi, Martins Cardoso, Renata, Boyle, Aimee L., Kros, Alexander, Jiskoot, Wim, Kuiper, Johan, Bouwstra, Joke, Van Eck, Miranda, Slütter, Bram, Benne, Naomi, Martins Cardoso, Renata, Boyle, Aimee L., Kros, Alexander, Jiskoot, Wim, Kuiper, Johan, Bouwstra, Joke, Van Eck, Miranda, and Slütter, Bram

Abstract

Atherosclerosis is characterized by the retention of lipids in foam cells in the arterial intima. The liver X receptor (LXR) agonist GW3965 is a promising therapeutic compound, since it induces reverse cholesterol transport in foam cells. However, hepatic LXR activation increases plasma and liver lipid levels, inhibiting its clinical development. Herein, a formulation that specifically enhances GW3965 deposition in the atherosclerotic lesion is aimed to be developed. GW3965 is encapsulated in liposomes functionalized with the cyclic peptide Lyp-1 (CGNKRTRGC), which binds the p32 receptor expressed on foam cells. These liposomes show preferential uptake by foam cells in vitro and higher accumulation in atherosclerotic plaques in mice compared to non-targeted liposomes as determined by in vivo imaging. Flow cytometry analysis of plaques reveals increased retention of Lyp-1 liposomes in atherosclerotic plaque macrophages compared to controls (p < 0.05). Long term treatment of established plaques in LDLR -/- mice with GW3965-containing Lyp-1 liposomes significantly reduces plaque macrophage content by 50% (p < 0.01). Importantly, GW3965-containing Lyp-1 liposomes do not increase plasma or hepatic lipid content. Thus, GW3965-containing Lyp-1 liposomes successfully target the atherosclerotic macrophages allowing plaque stabilization without commonly observed side effects of LXR agonists.

Published

2020

13. Vaccination and targeted therapy using liposomes : opportunities for treatment of atherosclerosis and cancer

Author

Benne, N., Jiskoot W., Kuiper J., Slütter, B.A., Irth, H., Bouwstra, J.A., Mastrobattista, E., Perrie, Y., Eden, W. van, and Leiden University

Subjects

Atomic force microscopy, Rigidity, Vaccination, Liposomes, Immunotherapy, Lyp-1, Liver X Receptor Agonist, Atherosclerosis, Foam cells, Tolerance

Abstract

This thesis focuses on using liposomes in two different treatment strategies; vaccination (or immunotherapy) and delivery of a small molecule, and in two different disease models; cancer and atherosclerosis. For each of these treatment strategies, the liposomal formulation was tailored to obtain the desired therapeutic effect. Chapter 2 reviews some of the most important physicochemical properties (size, shape, and rigidity) that determine the immunological effects of liposomes and other nanoparticles. In chapter 3 we present a detailed study on the effect of the rigidity of anionic liposomes, as measured by atomic force microscopy, on antigen-specific regulatory T-cell (Treg) responses. In chapter 4, we show that our optimized anionic liposomes can induce potent antigen-specific Treg responses, and can be used to delay atherosclerosis progression in a mouse model. Chapter 5 also focuses on liposomal treatment of atherosclerosis, but here targeted liposomes were prepared to successfully deliver a small molecule to foam cells in atherosclerotic plaques. In Chapter 6, we used cationic liposomes in combination with an adjuvant for cancer immunotherapy in mice. Finally, we summarize the overall findings in chapter 7 and discuss perspectives of using liposomes for vaccination and targeted drug delivery.

Published

2020

14. LyP-1-conjugated PEGylated liposomes: A carrier system for targeted therapy of lymphatic metastatic tumor

Author

Yan, Zhiqiang, Wang, Fei, Wen, Ziyi, Zhan, Changyou, Feng, Linglin, Liu, Yu, Wei, Xiaoli, Xie, Cao, and Lu, Weiyue

Subjects

*LIPOSOMES, *LYMPH nodes, *MACROPHAGES, *DOXORUBICIN, *FLUORESCEIN, *IMMUNOFLUORESCENCE, *DRUG delivery systems, *ANTINEOPLASTIC agents, *LYMPHATIC metastasis

Abstract

Abstract: The application of liposomes in targeted therapy of lymphatic metastatic tumors has been hampered by the low uptake rate of liposome by metastatic lymph nodes. In this report, LyP-1, a peptide that can specifically bind tumor cells, tumor lymphatics and tumor-associated macrophages, was conjugated to liposomes for targeting and treating lymphatic metastatic tumors. Firstly, LyP-1-conjugated PEGylated liposomes loaded with fluorescein or doxorubicin (DOX) were prepared and showed satisfactory vesicle size and size distribution. The in vitro cellular uptake and in vivo near-infrared fluorescence imaging results showed that LyP-1 modification increased liposome uptake by tumor cells and metastatic lymph nodes, but did not increase uptake by normal lymph nodes. The immunofluorescence analysis evidenced that LyP-1-conjugated liposomes were distributed adjacent to tumor lymphatics and tumor-associated macrophages in metastatic lymph nodes. The pharmacodynamic study suggested that compared with unmodified liposomes, LyP-1-conjugated DOX-loaded liposomes exhibited enhanced inhibition effect on tumor cells in vitro and lymphatic metastatic tumors in vivo. Pathological examination showed that liposomal DOX caused reduced tissue damage to injection site compared with DOX solution. In summary, LyP-1-conjugated PEGylated liposomes could be targeted to metastatic lymph nodes based on their specific binding to tumor cells, tumor lymphatics and tumor-associated macrophages. They are a safe and effective drug delivery system of antineoplastic agents for targeted therapy of lymphatic metastatic tumors. [Copyright &y& Elsevier]

Published

2012

15. Meme Kanseri Tedavisinde Aktif Hedeflendirme Amacıyla Kullanılmak Üzere Nano Boyutlu İlaç Taşıyıcı Sistemlerin (Nanofarmasötikler) Tasarımı, İn Vitro/İn Vivo Değerlendirilmesi

Author

Timur, Selin Seda, Gürsoy, R. Neslihan, and Farmasötik Teknoloji

Subjects

Lipid bazlı nanofarmasötikler, Lenfatik hedeflendirme, Meme kanseri tedavisi, LyP-1

Abstract

The aim of an ideal therapy using anticancer molecules is to target tumors selectively without damaging healthy tissues. Tumor specific markers formed by the physiological and morphological changes during the growth of cancer cells are identified by the help of specific ligands. The aim of active targeting, which is developed in this direction, is to protect the normal tissues from the therapy. The lymphatic system plays a critical role in the metastasis of cancer cells, thus lymphatic targeting approach has gained importance for the prevention of cancer metastasis. Laakkonen et al. have identified a cyclic 9-amino-acid (CGNKRTRGC) peptide called LyP-1, which specifically binds to tumor lymphatic vessels using phage-displayed peptide libraries in 2002. Within the scope of this thesis, LyP-1 containing lipid-based nanopharmaceutics (self emulsifying drug delivery systems, SEDDS) were targeted to p32, which is found in high amounts on the surface of breast cancer cells and to which LyP-1 binds and is internalized. Furthermore, the conjugates of the peptide were prepared with doxorubicin hydrochloride, anti-DTPA antibody and fluorescein. The characterization studies were carried out for all prepared formulations. Caco-2, MDA-MB-231 and 4T1 cell lines were used for in vitro evaluation of SEDDS formulations (liquid and solid), as well as in vivo efficacy studies were performed in 4T1 mouse breast cancer model in accordance with the results obtained from in vitro studies. At the end of this thesis, SEDDS formulations of LyP-1 for parenteral and oral use were developed and their potential for the treatment of breast cancer by lymphatic targeting were shown. Bu tez, TÜBİTAK SBAG 1002(Proje Numarası: 113S569), TÜBİTAK 2214/A, HÜBAB Hızlı Destek (Proje Numarası: THD-2017-11642) ve HÜBAB Lisansüstü Tez Desteği Projesi (Proje Numarası: TDK-2017-15964) kapsamında desteklenmiştir. ONAY SAYFASI iii YAYIMLAMA VE FİKRİ MÜLKİYET HAKLARI BEYANI iv ETİK BEYAN SAYFASI v TEŞEKKÜR vi ÖZET vii ABSTRACT viii İÇİNDEKİLER ix SİMGELER ve KISALTMALAR xiv ŞEKİLLER xvi TABLOLAR xxi 1. GİRİŞ 1 2. GENEL BİLGİLER 3 2.1. Kanser ve Kanser Tedavisinde Güncel Yaklaşımlar 3 2.2. Kanser Tedavisinde Tümöre Hedeflendirme 4 2.2.1. Tümöre Hedeflendirilmiş Peptitler 8 2.2.2. LyP-1 ve Aktif Hedeflendirme 10 2.3. Lenfatik Sistem ve Kanserdeki Rolü 17 2.3.1. Kanser Tedavisinde Lenfatik Hedeflendirme Yaklaşımları 18 2.4. Nano Boyutlu İlaç Taşıyıcı Sistemler ve Kanser Tedavisindeki Yeri 20 2.5. Peptit Konjugatları 22 2.5.1. Peptit – İlaç Konjugatları 23 2.6. Antikor Konjugatları 25 2.6.1. Bispesifik Hedeflendirme 27 2.7. Yağ Bazlı İlaç Taşıyıcı Sistemler 28 2.7.1. Kendiliğinden Emülsifiye Olabilen İlaç Taşıyıcı Sistemler 31 (SEDDS) 2.7.2. SEDDS Oluşum Mekanizmaları 33 2.7.3. SEDDS Türleri 34 2.8. SEDDS Formülasyonlarının Hazırlanması ve Hazırlamada Kullanılan 36 Yardımcı Maddeler ix 2.8.1. Yağlar 36 2.8.2. Yüzey Etkin Maddeler / Yardımcı Yüzey Etkin Maddeler 38 2.8.3. Yardımcı Çözücüler 40 2.9. SEDDS Formülasyonlarında Güncel Yaklaşımlar 41 3. GEREÇ VE YÖNTEM 47 3.1. Kullanılan Kimyasal Madde, Malzeme ve Aletler 47 3.1.1. Kullanılan Kimyasal Madde ve Malzemeler 47 3.1.2. Kullanılan Aletler 48 3.2. Önformülasyon Çalışmaları 50 3.2.1. Yardımcı Maddelerin Seçimi 50 3.2.2. Üçgen Faz Diyagramları 50 3.2.3. Sıvı Formülasyonların Hazırlanması 55 3.2.4. Katı Formülasyonların Hazırlanması 56 3.3. Formülasyon Optimizasyonu ve Karakterizasyonu 59 3.3.1. Makroskobik Özellikler 59 3.3.2. Mikroskobik Özellikler 59 3.3.3. Damlacık Büyüklüğü ve Zeta Potansiyel Tayini 59 3.3.4. Diferansiyel Taramalı Kalorimetre (DSC) Analizi 60 3.4. Konjugasyon Çalışmaları 60 3.4.1. Peptit – İlaç Konjugatlarının Hazırlanması 60 3.4.2. Polimer – İlaç Konjugatlarının Hazırlanması 61 3.4.3. Bispesifik Konjugatların Hazırlanması 63 3.5. Konjugatların Karakterizasyonu 66 3.5.1. D-PGA Konjugatlarının Tayini için ELISA Testi 66 3.5.2. Modifiye Edilmiş anti-DTPA’nın İmmunoreaktivite Tayini 66 3.5.3. Sodyum Dodesil Sülfat-Poliakrilamid Jel Elektroforezi (SDS- 67 PAGE) 3.5.4. Floresan Aktive Hücre Ayırma (Fluorescence Activated Cell 67 Sorting, FACS) Analizi 3.5.5. In – Cell ELISA 68 3.5.6. İmmünositokimya Çalışmaları 68 3.6. Etkin Madde Miktar Tayin Yöntemi Geliştirilmesi ve Validasyonu 69 x 3.6.1. HPLC Yönteminin Geliştirilmesi ve Validasyonu 69 3.6.2. LC-MS/MS Yönteminin Geliştirilmesi 73 3.7. Stabilite Çalışmaları 74 3.7.1. Etkin Maddenin Stabilitesi 74 3.7.2. Formülasyonların Stabilitesi 77 3.8. Dissolüsyon Çalışması 77 3.9. Hücre Kültürü Çalışmaları 78 3.9.1. 3.9.2. 3.9.3. 3.9.4. 3.10. İn Vivo 3.10.1. 3.11. İn Vivo Formülasyonlara Ait Çalışmalar 79 Konjugatlara Ait Çalışmalar 83 Western Blot Analizi 84 Polimeraz Zincir Reaksiyonu (PCR) 86 Etkililik Çalışmaları 89 Tümör Modeline Karar Verilmesi 90 Biyodağılım Çalışması 91 3.12. Bulguların İstatistiksel Olarak Değerlendirilmesi 92 4. BULGULAR 93 4.1. Önformülasyon Çalışmaları 93 4.1.1. Makroskobik Özellikler 93 4.1.2. Mikroskobik Özellikler 94 4.1.3. Damlacık Büyüklüğü ve Zeta Potansiyel Tayini 94 4.2. Formülasyon Çalışmaları 97 4.2.1. Üçgen Faz Diyagramları 97 4.3. Formülasyonların Karakterizasyonu 99 4.3.1. Makroskobik Özellikler 99 4.3.2. Mikroskobik Özellikler 99 4.3.3. Damlacık Büyüklüğü ve Zeta Potansiyel Tayini 99 4.3.4. Katı Formülasyonların Karakterizasyonu 100 4.3.5. Diferansiyel Taramalı Kalorimetre (DSC) Analizi 104 4.4. Konjugasyon Çalışmaları 105 4.4.1. Peptit – İlaç Konjugatlarının Hazırlanması 105 4.4.2. Polimer – İlaç Konjugatlarının Hazırlanması 106 4.5. Konjugatların Karakterizasyonu 108 xi 4.5.1. D-PGA Konjugatlarının Tayini için ELISA Testi 108 4.5.2. Modifiye Edilmiş anti-DTPA’nın İmmunoreaktivite Tayini 109 4.5.3. Sodyum Dodesil Sülfat-Poliakrilamid Jel Elektroforezi (SDS- 110 PAGE) 4.5.4. Floresan Aktive Hücre Ayırma (Fluorescence Activated Cell 112 Sorting, FACS) Analizi 4.5.5. In – Cell ELISA 112 4.5.6. İmmünositokimya Çalışmaları 114 4.6. Etkin Madde Miktar Tayin Yöntemi Geliştirilmesi ve Validasyonu 119 4.6.1. HPLC Yönteminin Geliştirilmesi ve Validasyonu 119 4.6.2. LC-MS/MS Yönteminin Geliştirilmesi 123 4.7. Stabilite Çalışmaları 125 4.7.1. Etkin Maddenin Stabilitesi 125 4.7.2. Formülasyonların Stabilitesi 131 4.8. Dissolüsyon Çalışması 132 4.9. Hücre Kültürü Çalışmaları 134 4.9.1. 4.9.2. 4.9.3. 4.9.4. 5.1.1. Makroskobik Özellikler 171 5.1.2. Mikroskobik Özellikler 172 5.1.3. Damlacık Büyüklüğü ve Zeta Potansiyel Tayini 172 5.2. Formülasyon Çalışmaları 173 5.2.1. Üçgen Faz Diyagramları 173 5.3. Formülasyonların Karakterizasyonu 174 5.3.1. Katı Formülasyonların Karakterizasyonu 175 5.3.2. Diferansiyel Taramalı Kalorimetre (DSC) Analizi 176 Formülasyonlara Ait Çalışmalar 134 Konjugatlara Ait Çalışmalar 155 Western Blot Analizi 156 Polimeraz Zincir Reaksiyonu (PCR) 157 Etkililik Çalışmaları 158 Biyodağılım Çalışması 163 4.10. İn Vivo 4.11. İn Vivo 5. TARTIŞMA 5.1. Önformülasyon Çalışmaları 171 171 xii 5.4. Konjugasyon Çalışmaları 177 5.4.1. Peptit – İlaç Konjugatlarının Hazırlanması 177 5.4.2. Polimer – İlaç Konjugatlarının Hazırlanması 179 5.5. Konjugatların Karakterizasyonu 180 5.5.1. D-PGA Konjugatlarının Tayini için ELISA Testi 180 5.5.2. Sodyum Dodesil Sülfat-Poliakrilamid Jel Elektroforezi (SDS- 179 PAGE) 5.5.3. Floresan Aktive Hücre Ayırma (Fluorescence Activated Cell 181 Sorting, FACS) 5.5.4. In – Cell ELISA 181 5.5.5. İmmünositokimya Çalışmaları 182 5.6. Etkin Madde Miktar Tayin Yöntemi Geliştirilmesi ve Validasyonu 184 5.6.1. HPLC Yönteminin Geliştirilmesi ve Validasyonu 184 5.6.2. LC-MS/MS Yönteminin Geliştirilmesi 185 5.7. Stabilite Çalışmaları 185 5.8. Dissolüsyon Çalışması 187 5.9. Hücre Kültürü Çalışmaları 188 5.9.1. Formülasyonlara Ait Çalışmalar 188 5.9.2. Konjugatlara Ait Çalışmalar 193 5.9.3. Western Blot Analizi 194 5.9.4. Polimeraz Zincir Reaksiyonu (PCR) 195 5.10. İn Vivo Etkinlilik Çalışmaları 196 5.11. İn Vivo Biyodağılım Çalışması 198 6. SONUÇ ve ÖNERİLER 200 7. KAYNAKLAR 202 8. EKLER 222 EK-1: Tez Çalışması ile İlgili Etik Kurul İzni EK-2: Tez Çalışması ile İlgili Bildiriler ve Yayınlar 9. ÖZGEÇMİŞ 228 Antikanser özellikte etkin maddeler kullanılarak ulaşılması istenen ideal kanser tedavisinde, normal dokular zarar görmeden tümörlü dokunun seçici olarak tanınması amaçlanmaktadır. Kanser hücrelerinin gelişimleri sırasında uğradığı fizyolojik ve morfolojik değişimler sonucunda ortaya çıkan tümöre özgü belirleyici moleküller, bu yapılara özgü ligandlar kullanılarak tanınmaktadır. Bu yönde geliştirilen yaklaşımlardan aktif hedeflendirmede amaç, vücutta bulunan sağlıklı dokuların tedaviden etkilenmesini önlemektir. Lenfatik sistem kanser hücrelerinin metastazında kilit rol oynadığından, kanserde metastazın önlenmesi amacıyla lenfatik hedeflendirme yaklaşımı önem kazanmıştır. Siklik yapıda, 9 aminoasitten oluşan LyP-1 (CGNKRTRGC), Laakkonen ve ark. tarafından 2002 yılında faj sunum tekniğiyle tanımlanan, tümör lenf damarlarına özgü bir peptittir. Bu tez kapsamında; meme kanseri hücreleri yüzeyinde yüksek miktarda bulunan ve LyP-1’e bağlanarak hücre içerisine alınmasını sağlayan p32 reseptörüne, LyP-1 içeren yağ bazlı nanofarmasötikler (kendiliğinden emülsifiye olabilen ilaç taşıyıcı sistemler, SEDDS) ile hedeflendirme yapılmıştır. Ayrıca, peptidin doksorubisin, anti-DTPA antikoru ve floresin ile konjugatları hazırlanmıştır. Hazırlanan tüm formülasyonların karakterizasyon çalışmaları gerçekleştirilmiştir. SEDDS formülasyonlarının (sıvı ve katı) in vitro değerlendirmesi için Caco-2, MDA-MB-231 ve 4T1 hücre hatları kullanılmış; elde edilen sonuçlar doğrultusunda 4T1 fare meme kanseri modelinde in vivo etkililik çalışmaları yürütülmüştür. Bu tezin sonunda, peptit yapılı LyP-1’in parenteral ve oral yoldan uygulanabilecek SEDDS formülasyonları geliştirilerek, lenfatik hedeflendirme ile meme kanseri tedavisindeki potansiyeli gösterilmiştir.

Published

2017

16. Complement Receptor Targeted Liposomes Encapsulating the Liver X Receptor Agonist GW3965 Accumulate in and Stabilize Atherosclerotic Plaques.

Author

Benne N, Martins Cardoso R, Boyle AL, Kros A, Jiskoot W, Kuiper J, Bouwstra J, Van Eck M, and Slütter B

Subjects

Animals, Benzoates, Benzylamines, Liposomes, Liver X Receptors, Mice, Receptors, Complement, Plaque, Atherosclerotic drug therapy

Abstract

Atherosclerosis is characterized by the retention of lipids in foam cells in the arterial intima. The liver X receptor (LXR) agonist GW3965 is a promising therapeutic compound, since it induces reverse cholesterol transport in foam cells. However, hepatic LXR activation increases plasma and liver lipid levels, inhibiting its clinical development. Herein, a formulation that specifically enhances GW3965 deposition in the atherosclerotic lesion is aimed to be developed. GW3965 is encapsulated in liposomes functionalized with the cyclic peptide Lyp-1 (CGNKRTRGC), which binds the p32 receptor expressed on foam cells. These liposomes show preferential uptake by foam cells in vitro and higher accumulation in atherosclerotic plaques in mice compared to non-targeted liposomes as determined by in vivo imaging. Flow cytometry analysis of plaques reveals increased retention of Lyp-1 liposomes in atherosclerotic plaque macrophages compared to controls (p < 0.05). Long term treatment of established plaques in LDLR -/- mice with GW3965-containing Lyp-1 liposomes significantly reduces plaque macrophage content by 50% (p < 0.01). Importantly, GW3965-containing Lyp-1 liposomes do not increase plasma or hepatic lipid content. Thus, GW3965-containing Lyp-1 liposomes successfully target the atherosclerotic macrophages allowing plaque stabilization without commonly observed side effects of LXR agonists., (© 2020 The Authors. Published by WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

17. LyP-1-Modified Multifunctional Dendrimers for Targeted Antitumor and Antimetastasis Therapy.

Author

Song N, Zhao L, Xu X, Zhu M, Liu C, Sun N, Yang J, Shi X, and Zhao J

Subjects

Animals, Cell Line, Tumor, Cell Survival drug effects, Female, Humans, Iodine Radioisotopes chemistry, Mice, Mice, Inbred BALB C, Mice, Nude, Neoplasm Invasiveness, Neoplasms, Experimental diagnostic imaging, Neoplasms, Experimental radiotherapy, Radioisotopes chemistry, Tomography, Emission-Computed, Single-Photon methods, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Dendrimers chemistry, Neoplasm Metastasis, Peptides, Cyclic chemistry, Tumor Microenvironment drug effects

Abstract

We designed and synthesized 131 I-labeled dendrimers modified with the LyP-1 peptide as a multifunctional platform for single-photon emission computed tomography (SPECT) imaging, radionuclide therapy, and antimetastasis therapy of cancer. The multifunctional platform was constructed by modifying amine-terminated generation 5 poly(amidoamine) dendrimers with 33.1 LyP-1 peptide and 9.2 3-(4'-hydroxyphenyl)propionic acid-OSu (HPAO), followed by acetylation of the remaining dendrimer terminal amines and radiolabeling with 131 I via the HPAO moieties. The LyP-1-modified dendrimers showed favorable cytocompatibility in the studied concentration range of 0.1-10 μM for 24 h and could be labeled by 131 I with satisfactory radiochemical purity (>99%) and stability (>90% even at 16 h). The 131 I-labeled LyP-1-modified dendrimers were capable of being utilized as a diagnostic probe for SPECT imaging and as a therapeutic agent for radionuclide therapy and antimetastasis of cancer cells in vitro and in a subcutaneous tumor model in vivo. Based on analyses of the tumor microenvironment, the antitumor and antimetastasis effects could be because of the reduced levels of the molecular markers associated with proliferation and metastasis, improved local hypoxia, and increased apoptosis rate. The developed 131 I-labeled dendrimeric nanodevice may hold great promise to be used as a nanotheranostic platform for cancer diagnosis and therapy.

Published

2020

18. Molecular dynamics, thermodynamic, and mutational binding studies for tumor-specific LyP-1 in complex with p32.

Author

Timur SS, Yalçın G, Çevik Ö, Andaç C, and Gürsoy RN

Subjects

Binding Sites, Carrier Proteins metabolism, Humans, Mitochondrial Proteins metabolism, Molecular Docking Simulation, Peptides, Cyclic metabolism, Protein Binding, Protein Conformation, Structure-Activity Relationship, Carrier Proteins chemistry, Carrier Proteins genetics, Mitochondrial Proteins chemistry, Mitochondrial Proteins genetics, Molecular Dynamics Simulation, Mutation, Peptides, Cyclic chemistry, Peptides, Cyclic genetics, Thermodynamics

Abstract

Recent studies in tumor homing peptides have shown the specificity of LyP-1 (CGNKRTRGC) to tumor lymphatics. In this present work, we evaluated the possible interactions between cyclic LyP-1 and its receptor, p32, with molecular dynamics and docking studies in order to lead the design of novel LyP-1 derivatives, which could bind to p32 more effectively and perform enhanced antitumor effect. The total binding enthalpy energies have been obtained by MM-PBSA thermodynamic computations and the favorability of p32.LyP-1 complex in water has been shown by explicit water MD computations. The last 30 ns of molecular dynamics trajectory have shown the strong interaction of LyP-1 with the inner surface chains of p32, especially with chains B and C. ALA-SCAN mutagenesis studies have indicated the considerable influence of Asn3, Lys4, Arg5, and Arg7 amino acid residues on the specific binding of LyP-1. Within the knowledge of the critical role of p32 receptor in cancer cell metabolism, this study can lead to further developments in anticancer therapy by targeting p32 with LyP-1 derivatives as active targeting moiety. This data can also be applied for the development of new drug delivery systems in which LyP-1 can be used for its targeting and anticancer properties.

Published

2018

19. Multistage Continuous Targeting with Quantitatively Controlled Peptides on Chitosan-Lipid Nanoparticles with Multicore-Shell Nanoarchitecture for Enhanced Orally Administrated Anticancer In Vitro and In Vivo.

Author

Su CW, Yen CS, Chiang CS, Hsu CH, and Chen SY

Subjects

Administration, Oral, Animals, Caco-2 Cells, Cell Death drug effects, Cell Membrane Permeability drug effects, Doxorubicin pharmacology, Drug Carriers chemistry, Endocytosis drug effects, Enterocytes drug effects, Enterocytes metabolism, Female, Humans, Ligands, Mice, Inbred BALB C, Microscopy, Fluorescence, Nanoparticles ultrastructure, Peptides chemistry, Peptides pharmacokinetics, Static Electricity, Tissue Distribution drug effects, Antineoplastic Agents administration & dosage, Antineoplastic Agents pharmacology, Chitosan chemistry, Lipids chemistry, Nanoparticles chemistry, Peptides pharmacology

Abstract

A DOX-loaded polysaccharide-lecithin reverse micelles triglyceride-based oral delivery nanocarrier (D-PL/TG NPs) conjugated with (i) RGD peptide for targeting to β1 integrin of M cells and (ii) Lyp-1 peptide for targeting to the p32 receptor of MDA-MB-231 cells is used to investigate the multistage continuous targeting capabilities of these peptide-conjugated nanocarriers (GLD-PL/TG NPs) for tumor therapy. Variations in the targeting efficacy and pharmacokinetic properties are investigated by quantitatively controlling the surface density of different peptides on the nanoparticles. In vitro permeability in a human follicle-associated epithelium model and cytotoxicity against MDA-MB-231 cells indicate that the nanocarriers conjugated with high RGD peptide concentrations display a higher permeability due to the existence of M cells with higher transcytosis activity, but a higher concentration of conjugated Lyp-1 peptide exhibits the lowest cell viability. Being benefited from specific targeting of peptide conjugation, improved bioavailability and enhanced tumor accumulation are achieved by the GLD-PL/TG NPs, leading to better antitumor efficacy. The results of in vivo biodistribution and antitumor studies reveal that the effect of LyP-1 peptide is more predominant than that of RGD peptide. This proof of multistage continuous targeting may open the door to a new generation of oral drug delivery systems in targeted cancer therapy., (© 2016 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2017

20. Identification and Characterization of Receptor-Specific Peptides for siRNA Delivery

Author

Ren, Yin, Hauert, Sabine, Lo, Justin Han-Je, and Bhatia, Sangeeta

Subjects

siRNA delivery, tumor-penetrating peptides, cell-penetrating peptides, LyP-1, cancer therapy

Abstract

Tumor-targeted delivery of siRNA remains a major barrier in fully realizing the therapeutic potential of RNA interference. While cell-penetrating peptides (CPP) are promising siRNA carrier candidates, they are universal internalizers that lack cell-type specificity. Herein, we design and screen a library of tandem tumor-targeting and cell-penetrating peptides that condense siRNA into stable nanocomplexes for cell type-specific siRNA delivery. Through physiochemical and biological characterization, we identify a subset of the nanocomplex library of that are taken up by cells via endocytosis, trigger endosomal escape and unpacking of the carrier, and ultimately deliver siRNA to the cytosol in a receptor-specific fashion. To better understand the structure–activity relationships that govern receptor-specific siRNA delivery, we employ computational regression analysis and identify a set of key convergent structural properties, namely the valence of the targeting ligand and the charge of the peptide, that help transform ubiquitously internalizing cell-penetrating peptides into cell type-specific siRNA delivery systems.

Published

2012