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Endostatin

January 01, 1970

Endostatin is a naturally occurring, 20-kDa C-terminal fragment derived from type XVIII collagen. It is reported to serve as an anti-angiogenic agent, similar to angiostatin and thrombospondin.

Endostatin monomer, basic amino acid residues shown in red (source: pdb.org, 1KOE).

Endostatin is a broad-spectrum angiogenesis inhibitor and may interfere with the pro-angiogenic action of growth factors such as basic fibroblast growth factor (bFGF/FGF-2) and vascular endothelial growth factor (VEGF).[1]

Background edit

Endostatin is an endogenous inhibitor of angiogenesis. It was first found secreted in the media of non-metastasizing mouse cells from a hemangioendothelioma cell line in 1997 and was subsequently found in humans, e.g. in platelets.[2][3][4] It is produced by proteolytic cleavage of collagen XVIII, a member of the multiplexin family that is characterized by interruptions in the triple helix creating multiple domains, by proteases such as cathepsins.[5] Collagen is a component of epithelial and endothelial basement membranes. Endostatin, as a fragment of collagen 18, demonstrates a role of the ECM in suppression of neoangiogenesis.[3] Pro-angiogenic and anti-angiogenic factors can also be created by proteolysis during coagulation cascades.[6][7][8] Endogenous inhibitors of angiogenesis are present in both normal tissue and cancerous tissue.[9] Overall, endostatin down regulates many signaling cascades like ephrin, TNF-α, and NFκB signaling as well as coagulation and adhesion cascades.[10] Other collagen derived antiangiogenic factors include arresten, canstatin, tumstatin, α 6 collagen type IV antiangiogenic fragment, and restin.[11]

Structure edit

Human monomeric endostatin is a globular protein containing two disulfide bonds: Cys162−302 and Cys264−294.[12] It folds tightly, has a zinc binding domain at the N-terminus of the protein, and has a high affinity for heparin through an 11 arginine basic patch.[13][14][15] Endostatin also binds all heparan sulfate proteoglycans with low affinity.[16][17] Oligomeric endostatin (trimer or dimer) binds mainly with laminin of the basal lamina.[18]

Biological activity edit

In-vitro studies have shown endostatin blocks the proliferation and organization of endothelial cells into new blood vessels.[19] In animal studies endostatin inhibited angiogenesis and growth of both primary tumors and secondary metastasis.[3]

Mechanism edit

Endostatin suppresses angiogenesis through many pathways affecting both cell viability and movement. Endostatin represses cell cycle control and anti-apoptosis genes in proliferating endothelial cells, resulting in cell death.[20] Endostatin blocks pro-angiogenic gene expression controlled by c-Jun N terminal kinase (JNK) by interfering with TNFα activation of JNK.[21] It reduces the growth of new cells by inhibiting cyclin D1. As a result, cells arrest during G1 phase and enter apoptosis.[22][23] Alteration of FGF signal transduction by endostatin inhibits the migration of endothelial cells through disruption of cell-matrix adhesions, cell-cell adhesions, and cytoskeletal reorganization.[24] By binding integrin α5β1 on endothelia cells it inhibits the signaling pathways of Ras and Raf kinases and decreases ERK-1 and p38 activity.[25] Endostatin binding and clustering of integrins causes co-localization with caveolin-1 and activates non-receptor tyrosine kinases of the Src family involved in the regulation of cell proliferation, differentiation, and mobility.[26][27][28][29] Other receptor interactions include the VEGF-R2/KDR/Flk-1 receptor on human umbilical vein endothelial cells.[30]

Endostatin may prevent activity from certain metalloproteinase.[31] Several studies have focused on the downstream effects of endostatin reception. These studies have estimated that endostatin may significantly affect 12% of genes used by human endothelial cells. Although endostatin signaling may affect this vast number of genes, the downstream affects appear surprisingly limited. Endostatin reception seems to only affect angiogenesis that arrives from pathogenic sources, such as tumors. Processes associated with angiogenesis, such as wound healing and reproduction, are seemingly not affected by endostatin. The result is possible because pathogenic-derived angiogenesis usually involves signaling through integrins, which are directly affected by endostatin.[1]

Cancer edit

Although this process by which endostatin works is not fully understood, it involves metalloproteases and endopeptidases that digest components of the extracellular matrix. Several similar endogeneous angiogenic factors are produced from matrix components in this fashion. For example, perlecan degradation can yield endorepellin which functions as an anti-angiogenic factor. Collectively, these products are thought to balance regulation between pro-angiogenic and anti-angiogenic factors outside epithelial and endothelial layers.[32]

Among anti-angiogenesis inhibitors, endostatin has a wide range of anti-cancer spectrum targets, increasing its significance since synthetic inhibitors usually have single targets and struggle with toxicity.[33] Endostatin has several characteristics that may be advantageous to cancer therapy. First of all, endogenous endostatin has been described as "the least toxic anti-cancer drug in mice". Furthermore, neither resistance nor toxicity to endostatin occur in humans.[citation needed] Also, endostatin has been estimated to affect 12% of the human genome. This reveals a broad spectrum of activity focused on preventing angiogenesis. This is very different from single-molecule therapies, and may change how cancer therapies are designed: drugs may be designed to target a wide range of genes instead of one particular protein. However, endostatin does not affect all tumors. For example, cancers that may have extreme pro-angiogenic activity through VEGF may overcome the anti-angiogenic effects of endostatin.[1]

Possible cancer treatment edit

Endostatin is currently being studied as part of cancer research. Prior results indicated that endostatin can be beneficial in combinations with other medicines, but endostatin alone gave no significant improvements in tumor/disease progression.

Phase I edit

In a Phase I clinical trial of Endostatin, of the 19 patients treated, 12 were switched out of the trial by their physicians due to continued progression of their disease.[34] Two patients continued to be treated, and the remaining patients withdrew on their own. The trial, designed primarily to demonstrate safety, indeed showed that the drug was safe and well tolerated (at the dosages used).

Phase II edit

In a Phase II clinical trial of Endostatin, 42 patients with pancreatic endocrine tumors or carcinoid tumors were treated.[35] Of the 40 patients which could be evaluated for a radiologic response, none experienced partial response to therapy, as defined by World Health Organization criteria.

The conclusion from the trial was that, "Treatment with Endostatin did not result in significant tumor regression in patients with advanced neuroendocrine tumors."

Phase III edit

A phase III clinical trial was carried out on 493 histology or cytology-confirmed stage IIIB and IV NSCLC patients with a life expectancy >3 months. Patients were treated with Endostar (rh-endostatin, YH-16), a recombinant endostatin product, in combination with vinorelbine and cisplatin (a standard chemotherapeutic regimen). The addition of Endostar to the standard chemotherapeutic regimen in these advanced NSCLC patients resulted in significant and clinically meaningful improvement in response rate, median time to progression, and clinical benefit rate compared with the chemotherapeutic regimen alone.[36]

Clinical significance edit

Endostatin may also be useful as a therapeutic for inflammatory diseases like rheumatoid arthritis as well as Crohn disease, diabetic retinopathy, psoriasis, and endometriosis by reducing the infiltration of inflammatory cells through invading angiogenesis.[37] Down syndrome patients seem to be protected from diabetic retinopathy due to an additional copy of chromosome 21, and elevated expression of endostatin.[38]

References edit

  1. ^ a b c Folkman, J. (2006). "Antiangiogenesis in cancer therapy--endostatin and its mechanisms of action". Exp. Cell Res. 312 (5, part 2): 594–607. doi:10.1016/j.yexcr.2005.11.015. PMID 16376330.
  2. ^ Custo, S; Baron, B; Felice, A; Seria, E (5 July 2022). "A comparative profile of total protein and six angiogenically-active growth factors in three platelet products". GMS Interdisciplinary Plastic and Reconstructive Surgery DGPW. 11 (Doc06): Doc06. doi:10.3205/iprs000167. PMC 9284722. PMID 35909816.
  3. ^ a b c OReilly, M.S.; Boehm, T.; Shing, Y.; Fukai, N.; Vasios, G.; Lane, W.W.; Flynn, E.; Birkhead, J.R.; Olsen, B.R.; Folkman, J. (1997). "Endostatin: an endogenous inhibitor of angiogenesis and tumor growth". Cell. 88 (2): 277–85. doi:10.1016/S0092-8674(00)81848-6. PMID 9008168.
  4. ^ Standker, L; Schrader, M.; Kanse, S.M.; Jurgens, M.; Forssmann, W.G.; Prissner, K.T. (1997). "Isolation and characterization of the circulating form of human endostatin". FEBS Lett. 420 (2–3): 129–33. doi:10.1016/S0014-5793(97)01503-2. PMID 9459295. S2CID 9852143.
  5. ^ Felbor, U; et al. (2000). "Secreted cathepsin L generates endostatin from collagen XVIII". EMBO J. 19 (6): 1187–94. doi:10.1093/emboj/19.6.1187. PMC 305660. PMID 10716919.
  6. ^ Browder, T.; Folkman, J.; Pirie-Shepherd, S. (2000). "The hemostatic system as a regulator of angiogenesis". J. Biol. Chem. 275 (3): 1521–4. doi:10.1074/jbc.275.3.1521. PMID 10636838.
  7. ^ Ma, L; Hollenberg, M.D.; Wallace, J.L. (2001). "Thrombin-induced platelet endostatin release is blocked by a proteinase activated receptor-4 (PAR4) antagonist". Br. J. Pharmacol. 134 (4): 701–4. doi:10.1038/sj.bjp.0704312. PMC 1573005. PMID 11606309.
  8. ^ Rhim, T.Y.; Park, C.S.; Kim, E.; Kim, S.S. (1998). "Human prothrombin fragment 1 and 2 inhibit bFGF-induced BCE cell growth". Biochem. Biophys. Res. Commun. 252 (2): 513–6. doi:10.1006/bbrc.1998.9682. PMID 9826562.
  9. ^ Nyberg, P.; Xie, L.; Kalluri, R. (2005). "Endogenous inhibitors of angiogenesis". Cancer Res. 65 (10): 3967–79. doi:10.1158/0008-5472.CAN-04-2427. PMID 15899784.
  10. ^ Abdollahi, A.; Hahnfeldt, P.; Maercker, C.; Grone, H.; Debus, J.; Ansorge, W.; Folman, J.; Hlatky, L.; Huber, P.E. (2004). "Endostatin's antiangiogenic signaling network". Mol. Cell. 13 (5): 649–63. doi:10.1016/S1097-2765(04)00102-9. PMID 15023336.
  11. ^ Assadian, S.; Teodoro, J.G. (2008). "Regulation of collagen-derived antiangiogenic factors by p53". Expert Opin. Biol. Ther. 8 (7): 941–50. doi:10.1517/14712598.8.7.941. PMID 18549324. S2CID 72058014.
  12. ^ John, H.; Forssmann, W.G. (2001). "Determination of the disulfide bond pattern of the endogenous and recombinant angiogenesis inhibitor endostatin by mass spectrometry". Rapid Commun. Mass Spectrom. 15 (14): 1222–8. Bibcode:2001RCMS...15.1222J. doi:10.1002/rcm.367. PMID 11445906.
  13. ^ Hohenester, E.; Sasaki, T.; Olsen, B.R.; Timpl, R. (1998). "Crystal structure of the angiogenesis inhibitor endostatin at 1.5 A resolution". EMBO J. 17 (6): 1656–64. doi:10.1093/emboj/17.6.1656. PMC 1170513. PMID 9501087.
  14. ^ Ding, Y.H.; Javaherian, K.; Lo, K.M.; Chopra, R.; Boehm, T.; Lanciotti, J.; Harris, B.A.; Li, Y.; Shapiro, R.; Hohenester, E.; et al. (1998). "Zinc-dependent dimers observed in crystals of human endostatin". Proc. Natl. Acad. Sci. U.S.A. 95 (18): 10443–8. Bibcode:1998PNAS...9510443D. doi:10.1073/pnas.95.18.10443. PMC 27913. PMID 9724722.
  15. ^ Dixelius, J.; Cross, M.; Matsumoto, T.; Sasaki, T.; Timpl, R.; Claesson-Welsh, L. (2002). "Endostatin regulates endothelial cell adhesion and cytoskeletal organization". Cancer Res. 62 (7): 1944–7. PMID 11929807.
  16. ^ Karumanchi, S.A.; Jha, V.; Ramchandran, R.; Karihaloo, A.; Tsiokas, L.; Chan, B.; Dhanabal, M.; Hanai, J.I.; Venkataraman, G.; Shriver, Z.; et al. (2001). "Cell surface glypicans are low-affinity endostatin receptors" (PDF). Mol. Cell. 7 (4): 811–22. doi:10.1016/S1097-2765(01)00225-8. PMID 11336704. S2CID 43358048.
  17. ^ Sasaki, T; Larsson, H.; Kreuger, J.; Salmivirta, M.; Claesson-Welsh, L.; Lindahl, U.; Hohenester, E.; Timpl, R. (1999). "Structural basis and potential role of heparin/heparan sulfate binding to the angiogenesis inhibitor endostatin". EMBO J. 18 (22): 6240–8. doi:10.1093/emboj/18.22.6240. PMC 1171687. PMID 10562536.
  18. ^ Javaherian, K.; Park, S.Y.; Pickl, W.F.; LaMontagne, K.R.; Sjin, R.T.T.; Gillies, S.; Lo, K. (2002). "Laminin modulates morphogenic properties of the collagen XVIII endostatin domain". J. Biol. Chem. 277 (47): 45211–8. doi:10.1074/jbc.M206358200. PMID 12237301.
  19. ^ Folkman, J.; Kalluri, R. (2004). "Cancer without disease". Nature. 427 (6977): 787. Bibcode:2004Natur.427..787F. doi:10.1038/427787a. PMID 14985739.
  20. ^ Shichiri, M.; Hirata (2001). "Y". FASEB J. 15 (6): 1044–53. doi:10.1096/fj.99-1083com. PMID 11292666.
  21. ^ Yin, G; Liu, W.; An, P.; Li, P.; Ding, I.; Planelles, V.; Schwarz, E.M.; Min, W. (2002). "Endostatin gene transfer inhibits joint angiogenesis and pannus formation in inflammatory arthritis". Mol. Ther. 5 (5 Pt 1): 547–54. doi:10.1006/mthe.2002.0590. PMID 11991745.
  22. ^ Dhanabal, M.; Volk, R.; Ramchandran, R.; Simons, M.; Sukhatme, V.P. (1999). "Cloning, expression, and in vitro activity of human endostatin". Biochem. Biophys. Res. Commun. 258 (2): 345–52. doi:10.1006/bbrc.1999.0595. PMID 10329390.
  23. ^ Hanai, J.; Dhanabal, M.; Karumanchi, S.A.; Albanese, C.; Waterman, M.; Chan, B.; Ramchandran, R.; Pestell, R.; Sukhatme, V.P. (2002). "Endostatin causes G1 arrest of endothelial cells through inhibition of cyclin D1". J. Biol. Chem. 277 (19): 16464–9. doi:10.1074/jbc.M112274200. PMID 11815623.
  24. ^ Dixelius, J; Larsson, H.; Sasaki, T.; Holmqvist, K.; Lu, L.; Engstrom, A.; Timpl, R.; Welsh, M.; Claesson-Welsh, L. (2000). "Endostatin-induced tyrosin kinase signaling through the Shb adaptor protein regulates endothelial cell apoptosis". Blood. 95 (11): 3403–11. doi:10.1182/blood.V95.11.3403. PMID 10828022.
  25. ^ Sudhakar, A.; Sugimoto, H.; Yang, C.; Lively, J.; Zeisberg, M.; Kalluri, R. (2003). "Human tumstatin and human endostatin exhibit distinct antiangiogenic activities mediated by alpha v beta 3 and alpha 5 beta 1 integrins". Proc. Natl. Acad. Sci. U.S.A. 100 (8): 4766–71. Bibcode:2003PNAS..100.4766S. doi:10.1073/pnas.0730882100. PMC 153630. PMID 12682293.
  26. ^ Tatosyan, A.G; Mizenina, O.A. (2000). "Kinases of the Src family: structure and functions". Biochemistry. 65 (1): 49–58. PMID 10702640.
  27. ^ Thomas, S.M.; Brugge, J.S. (1997). "Cellular functions regulated by Src family kinases". Annu. Rev. Cell Dev. Biol. 13: 513–609. doi:10.1146/annurev.cellbio.13.1.513. PMID 9442882.
  28. ^ Wary, K.K.; Mariotti, A.; Zurzolo, C.; Giancotti, F.G. (1998). "A requirement for caveolin-1 and associated kinase Fyn in integrin signaling and anchorage-dependent cell growth". Cell. 94 (5): 625–34. doi:10.1016/S0092-8674(00)81604-9. PMID 9741627.
  29. ^ Wickstrom, S.A.; Alitalo, K.; Keski-Oja, J. (2002). "Endostatin associates with integrin alpha5beta1 and caveolin-1, and activates Src via a tyrosyl phosphatase-dependent pathway in human endothelial cells". Cancer Res. 62 (19): 5580–9. PMID 12359771.
  30. ^ Kim, Y.; Hwang, S.; Kim, Y.; Pyun, B.; Kim, T.; Lee, S.; Gho, Y.S.; Kwon, Y. (2002). "Endostatin blocks vascular endothelial growth factor-mediated signaling via direct interaction with KDR/Flk-1". J. Biol. Chem. 277 (31): 27872–9. doi:10.1074/jbc.M202771200. PMID 12029087.
  31. ^ Felbor, U.; et al. (2000). "Secreted cathepsin L generates endostatin from collagen XVIII". EMBO J. 19 (6): 1187–94. doi:10.1093/emboj/19.6.1187. PMC 305660. PMID 10716919.
  32. ^ Marneros, A.G.; Olsen, B.R. (2005). "Physiological role of collagen XVIII and endostatin". The FASEB Journal. 19 (7): 716–28. doi:10.1096/fj.04-2134rev. PMID 15857886. S2CID 24259395.
  33. ^ Karamouzis, M.V.; Moschos, S.J. (2009). "The use of endostatin in the treatment of solid tumors". Expert Opin. Biol. Ther. 9 (5): 641–8. doi:10.1517/14712590902882118. PMID 19368526. S2CID 73212482.
  34. ^ "Boston hospitals report early results of Endostatin clinical trial" (Press release). ScienceDaily.com: Dana-Farber Cancer Institute. November 13, 2000. Retrieved 2006-07-12.
  35. ^ Kulke M H; et al. (2006). "Phase II study of recombinant human endostatin in patients with advanced neuroendocrine tumors". J. Clin. Oncol. 24 (22): 3555–3561. doi:10.1200/JCO.2006.05.6762. PMID 16877721.
  36. ^ Results of phase III trial of rh-endostatin (YH-16) in advanced non-small cell lung cancer (NSCLC) patients (Y. Sun, J. Wang, Y. Liu, X. Song, Y. Zhang, K. Li, Y. Zhu, Q. Zhou, L. You and C. Yao) [1]
  37. ^ Yin, G.; Liu, W.; An, P.; Li, P.; ding, I.; Planelles, V.; Schwarz, E.M.; Min, W. (2002). "Endostatin gene transfer inhibits joint angiogenesis and pannus formation in inflammatory arthritis". Mol. Ther. 5 (5 Pt 1): 547–54. doi:10.1006/mthe.2002.0590. PMID 11991745.
  38. ^ Ryeom S, Folkman J (March 2009). "Role of endogenous angiogenesis inhibitors in Down syndrome". J. Craniofac. Surg. 20 (Suppl 1): 595–6. doi:10.1097/SCS.0b013e3181927f47. PMID 19795527. S2CID 21576950.

External links edit

  • Endostatin at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
  • PBS' Nova program explores Endostatin in 2001

January 01, 1970
endostatin, naturally, occurring, terminal, fragment, derived, from, type, xviii, collagen, reported, serve, anti, angiogenic, agent, similar, angiostatin, thrombospondin, monomer, basic, amino, acid, residues, shown, source, 1koe, broad, spectrum, angiogenesi. Endostatin is a naturally occurring 20 kDa C terminal fragment derived from type XVIII collagen It is reported to serve as an anti angiogenic agent similar to angiostatin and thrombospondin Endostatin monomer basic amino acid residues shown in red source pdb org 1KOE Endostatin is a broad spectrum angiogenesis inhibitor and may interfere with the pro angiogenic action of growth factors such as basic fibroblast growth factor bFGF FGF 2 and vascular endothelial growth factor VEGF 1 Contents 1 Background 2 Structure 3 Biological activity 4 Mechanism 5 Cancer 6 Possible cancer treatment 6 1 Phase I 6 2 Phase II 6 3 Phase III 7 Clinical significance 8 References 9 External linksBackground editEndostatin is an endogenous inhibitor of angiogenesis It was first found secreted in the media of non metastasizing mouse cells from a hemangioendothelioma cell line in 1997 and was subsequently found in humans e g in platelets 2 3 4 It is produced by proteolytic cleavage of collagen XVIII a member of the multiplexin family that is characterized by interruptions in the triple helix creating multiple domains by proteases such as cathepsins 5 Collagen is a component of epithelial and endothelial basement membranes Endostatin as a fragment of collagen 18 demonstrates a role of the ECM in suppression of neoangiogenesis 3 Pro angiogenic and anti angiogenic factors can also be created by proteolysis during coagulation cascades 6 7 8 Endogenous inhibitors of angiogenesis are present in both normal tissue and cancerous tissue 9 Overall endostatin down regulates many signaling cascades like ephrin TNF a and NFkB signaling as well as coagulation and adhesion cascades 10 Other collagen derived antiangiogenic factors include arresten canstatin tumstatin a 6 collagen type IV antiangiogenic fragment and restin 11 Structure editHuman monomeric endostatin is a globular protein containing two disulfide bonds Cys162 302 and Cys264 294 12 It folds tightly has a zinc binding domain at the N terminus of the protein and has a high affinity for heparin through an 11 arginine basic patch 13 14 15 Endostatin also binds all heparan sulfate proteoglycans with low affinity 16 17 Oligomeric endostatin trimer or dimer binds mainly with laminin of the basal lamina 18 Biological activity editIn vitro studies have shown endostatin blocks the proliferation and organization of endothelial cells into new blood vessels 19 In animal studies endostatin inhibited angiogenesis and growth of both primary tumors and secondary metastasis 3 Mechanism editEndostatin suppresses angiogenesis through many pathways affecting both cell viability and movement Endostatin represses cell cycle control and anti apoptosis genes in proliferating endothelial cells resulting in cell death 20 Endostatin blocks pro angiogenic gene expression controlled by c Jun N terminal kinase JNK by interfering with TNFa activation of JNK 21 It reduces the growth of new cells by inhibiting cyclin D1 As a result cells arrest during G1 phase and enter apoptosis 22 23 Alteration of FGF signal transduction by endostatin inhibits the migration of endothelial cells through disruption of cell matrix adhesions cell cell adhesions and cytoskeletal reorganization 24 By binding integrin a5b1 on endothelia cells it inhibits the signaling pathways of Ras and Raf kinases and decreases ERK 1 and p38 activity 25 Endostatin binding and clustering of integrins causes co localization with caveolin 1 and activates non receptor tyrosine kinases of the Src family involved in the regulation of cell proliferation differentiation and mobility 26 27 28 29 Other receptor interactions include the VEGF R2 KDR Flk 1 receptor on human umbilical vein endothelial cells 30 Endostatin may prevent activity from certain metalloproteinase 31 Several studies have focused on the downstream effects of endostatin reception These studies have estimated that endostatin may significantly affect 12 of genes used by human endothelial cells Although endostatin signaling may affect this vast number of genes the downstream affects appear surprisingly limited Endostatin reception seems to only affect angiogenesis that arrives from pathogenic sources such as tumors Processes associated with angiogenesis such as wound healing and reproduction are seemingly not affected by endostatin The result is possible because pathogenic derived angiogenesis usually involves signaling through integrins which are directly affected by endostatin 1 Cancer editAlthough this process by which endostatin works is not fully understood it involves metalloproteases and endopeptidases that digest components of the extracellular matrix Several similar endogeneous angiogenic factors are produced from matrix components in this fashion For example perlecan degradation can yield endorepellin which functions as an anti angiogenic factor Collectively these products are thought to balance regulation between pro angiogenic and anti angiogenic factors outside epithelial and endothelial layers 32 Among anti angiogenesis inhibitors endostatin has a wide range of anti cancer spectrum targets increasing its significance since synthetic inhibitors usually have single targets and struggle with toxicity 33 Endostatin has several characteristics that may be advantageous to cancer therapy First of all endogenous endostatin has been described as the least toxic anti cancer drug in mice Furthermore neither resistance nor toxicity to endostatin occur in humans citation needed Also endostatin has been estimated to affect 12 of the human genome This reveals a broad spectrum of activity focused on preventing angiogenesis This is very different from single molecule therapies and may change how cancer therapies are designed drugs may be designed to target a wide range of genes instead of one particular protein However endostatin does not affect all tumors For example cancers that may have extreme pro angiogenic activity through VEGF may overcome the anti angiogenic effects of endostatin 1 Possible cancer treatment editEndostatin is currently being studied as part of cancer research Prior results indicated that endostatin can be beneficial in combinations with other medicines but endostatin alone gave no significant improvements in tumor disease progression Phase I edit In a Phase I clinical trial of Endostatin of the 19 patients treated 12 were switched out of the trial by their physicians due to continued progression of their disease 34 Two patients continued to be treated and the remaining patients withdrew on their own The trial designed primarily to demonstrate safety indeed showed that the drug was safe and well tolerated at the dosages used Phase II edit In a Phase II clinical trial of Endostatin 42 patients with pancreatic endocrine tumors or carcinoid tumors were treated 35 Of the 40 patients which could be evaluated for a radiologic response none experienced partial response to therapy as defined by World Health Organization criteria The conclusion from the trial was that Treatment with Endostatin did not result in significant tumor regression in patients with advanced neuroendocrine tumors Phase III edit A phase III clinical trial was carried out on 493 histology or cytology confirmed stage IIIB and IV NSCLC patients with a life expectancy gt 3 months Patients were treated with Endostar rh endostatin YH 16 a recombinant endostatin product in combination with vinorelbine and cisplatin a standard chemotherapeutic regimen The addition of Endostar to the standard chemotherapeutic regimen in these advanced NSCLC patients resulted in significant and clinically meaningful improvement in response rate median time to progression and clinical benefit rate compared with the chemotherapeutic regimen alone 36 Clinical significance editEndostatin may also be useful as a therapeutic for inflammatory diseases like rheumatoid arthritis as well as Crohn disease diabetic retinopathy psoriasis and endometriosis by reducing the infiltration of inflammatory cells through invading angiogenesis 37 Down syndrome patients seem to be protected from diabetic retinopathy due to an additional copy of chromosome 21 and elevated expression of endostatin 38 References edit a b c Folkman J 2006 Antiangiogenesis in cancer therapy endostatin and its mechanisms of action Exp Cell Res 312 5 part 2 594 607 doi 10 1016 j yexcr 2005 11 015 PMID 16376330 Custo S Baron B Felice A Seria E 5 July 2022 A comparative profile of total protein and six angiogenically active growth factors in three platelet products GMS Interdisciplinary Plastic and Reconstructive Surgery DGPW 11 Doc06 Doc06 doi 10 3205 iprs000167 PMC 9284722 PMID 35909816 a b c OReilly M S Boehm T Shing Y Fukai N Vasios G Lane W W Flynn E Birkhead J R Olsen B R Folkman J 1997 Endostatin an endogenous inhibitor of angiogenesis and tumor growth Cell 88 2 277 85 doi 10 1016 S0092 8674 00 81848 6 PMID 9008168 Standker L Schrader M Kanse S M Jurgens M Forssmann W G Prissner K T 1997 Isolation and characterization of the circulating form of human endostatin FEBS Lett 420 2 3 129 33 doi 10 1016 S0014 5793 97 01503 2 PMID 9459295 S2CID 9852143 Felbor U et al 2000 Secreted cathepsin L generates endostatin from collagen XVIII EMBO J 19 6 1187 94 doi 10 1093 emboj 19 6 1187 PMC 305660 PMID 10716919 Browder T Folkman J Pirie Shepherd S 2000 The hemostatic system as a regulator of angiogenesis J Biol Chem 275 3 1521 4 doi 10 1074 jbc 275 3 1521 PMID 10636838 Ma L Hollenberg M D Wallace J L 2001 Thrombin induced platelet endostatin release is blocked by a proteinase activated receptor 4 PAR4 antagonist Br J Pharmacol 134 4 701 4 doi 10 1038 sj bjp 0704312 PMC 1573005 PMID 11606309 Rhim T Y Park C S Kim E Kim S S 1998 Human prothrombin fragment 1 and 2 inhibit bFGF induced BCE cell growth Biochem Biophys Res Commun 252 2 513 6 doi 10 1006 bbrc 1998 9682 PMID 9826562 Nyberg P Xie L Kalluri R 2005 Endogenous inhibitors of angiogenesis Cancer Res 65 10 3967 79 doi 10 1158 0008 5472 CAN 04 2427 PMID 15899784 Abdollahi A Hahnfeldt P Maercker C Grone H Debus J Ansorge W Folman J Hlatky L Huber P E 2004 Endostatin s antiangiogenic signaling network Mol Cell 13 5 649 63 doi 10 1016 S1097 2765 04 00102 9 PMID 15023336 Assadian S Teodoro J G 2008 Regulation of collagen derived antiangiogenic factors by p53 Expert Opin Biol Ther 8 7 941 50 doi 10 1517 14712598 8 7 941 PMID 18549324 S2CID 72058014 John H Forssmann W G 2001 Determination of the disulfide bond pattern of the endogenous and recombinant angiogenesis inhibitor endostatin by mass spectrometry Rapid Commun Mass Spectrom 15 14 1222 8 Bibcode 2001RCMS 15 1222J doi 10 1002 rcm 367 PMID 11445906 Hohenester E Sasaki T Olsen B R Timpl R 1998 Crystal structure of the angiogenesis inhibitor endostatin at 1 5 A resolution EMBO J 17 6 1656 64 doi 10 1093 emboj 17 6 1656 PMC 1170513 PMID 9501087 Ding Y H Javaherian K Lo K M Chopra R Boehm T Lanciotti J Harris B A Li Y Shapiro R Hohenester E et al 1998 Zinc dependent dimers observed in crystals of human endostatin Proc Natl Acad Sci U S A 95 18 10443 8 Bibcode 1998PNAS 9510443D doi 10 1073 pnas 95 18 10443 PMC 27913 PMID 9724722 Dixelius J Cross M Matsumoto T Sasaki T Timpl R Claesson Welsh L 2002 Endostatin regulates endothelial cell adhesion and cytoskeletal organization Cancer Res 62 7 1944 7 PMID 11929807 Karumanchi S A Jha V Ramchandran R Karihaloo A Tsiokas L Chan B Dhanabal M Hanai J I Venkataraman G Shriver Z et al 2001 Cell surface glypicans are low affinity endostatin receptors PDF Mol Cell 7 4 811 22 doi 10 1016 S1097 2765 01 00225 8 PMID 11336704 S2CID 43358048 Sasaki T Larsson H Kreuger J Salmivirta M Claesson Welsh L Lindahl U Hohenester E Timpl R 1999 Structural basis and potential role of heparin heparan sulfate binding to the angiogenesis inhibitor endostatin EMBO J 18 22 6240 8 doi 10 1093 emboj 18 22 6240 PMC 1171687 PMID 10562536 Javaherian K Park S Y Pickl W F LaMontagne K R Sjin R T T Gillies S Lo K 2002 Laminin modulates morphogenic properties of the collagen XVIII endostatin domain J Biol Chem 277 47 45211 8 doi 10 1074 jbc M206358200 PMID 12237301 Folkman J Kalluri R 2004 Cancer without disease Nature 427 6977 787 Bibcode 2004Natur 427 787F doi 10 1038 427787a PMID 14985739 Shichiri M Hirata 2001 Y FASEB J 15 6 1044 53 doi 10 1096 fj 99 1083com PMID 11292666 Yin G Liu W An P Li P Ding I Planelles V Schwarz E M Min W 2002 Endostatin gene transfer inhibits joint angiogenesis and pannus formation in inflammatory arthritis Mol Ther 5 5 Pt 1 547 54 doi 10 1006 mthe 2002 0590 PMID 11991745 Dhanabal M Volk R Ramchandran R Simons M Sukhatme V P 1999 Cloning expression and in vitro activity of human endostatin Biochem Biophys Res Commun 258 2 345 52 doi 10 1006 bbrc 1999 0595 PMID 10329390 Hanai J Dhanabal M Karumanchi S A Albanese C Waterman M Chan B Ramchandran R Pestell R Sukhatme V P 2002 Endostatin causes G1 arrest of endothelial cells through inhibition of cyclin D1 J Biol Chem 277 19 16464 9 doi 10 1074 jbc M112274200 PMID 11815623 Dixelius J Larsson H Sasaki T Holmqvist K Lu L Engstrom A Timpl R Welsh M Claesson Welsh L 2000 Endostatin induced tyrosin kinase signaling through the Shb adaptor protein regulates endothelial cell apoptosis Blood 95 11 3403 11 doi 10 1182 blood V95 11 3403 PMID 10828022 Sudhakar A Sugimoto H Yang C Lively J Zeisberg M Kalluri R 2003 Human tumstatin and human endostatin exhibit distinct antiangiogenic activities mediated by alpha v beta 3 and alpha 5 beta 1 integrins Proc Natl Acad Sci U S A 100 8 4766 71 Bibcode 2003PNAS 100 4766S doi 10 1073 pnas 0730882100 PMC 153630 PMID 12682293 Tatosyan A G Mizenina O A 2000 Kinases of the Src family structure and functions Biochemistry 65 1 49 58 PMID 10702640 Thomas S M Brugge J S 1997 Cellular functions regulated by Src family kinases Annu Rev Cell Dev Biol 13 513 609 doi 10 1146 annurev cellbio 13 1 513 PMID 9442882 Wary K K Mariotti A Zurzolo C Giancotti F G 1998 A requirement for caveolin 1 and associated kinase Fyn in integrin signaling and anchorage dependent cell growth Cell 94 5 625 34 doi 10 1016 S0092 8674 00 81604 9 PMID 9741627 Wickstrom S A Alitalo K Keski Oja J 2002 Endostatin associates with integrin alpha5beta1 and caveolin 1 and activates Src via a tyrosyl phosphatase dependent pathway in human endothelial cells Cancer Res 62 19 5580 9 PMID 12359771 Kim Y Hwang S Kim Y Pyun B Kim T Lee S Gho Y S Kwon Y 2002 Endostatin blocks vascular endothelial growth factor mediated signaling via direct interaction with KDR Flk 1 J Biol Chem 277 31 27872 9 doi 10 1074 jbc M202771200 PMID 12029087 Felbor U et al 2000 Secreted cathepsin L generates endostatin from collagen XVIII EMBO J 19 6 1187 94 doi 10 1093 emboj 19 6 1187 PMC 305660 PMID 10716919 Marneros A G Olsen B R 2005 Physiological role of collagen XVIII and endostatin The FASEB Journal 19 7 716 28 doi 10 1096 fj 04 2134rev PMID 15857886 S2CID 24259395 Karamouzis M V Moschos S J 2009 The use of endostatin in the treatment of solid tumors Expert Opin Biol Ther 9 5 641 8 doi 10 1517 14712590902882118 PMID 19368526 S2CID 73212482 Boston hospitals report early results of Endostatin clinical trial Press release ScienceDaily com Dana Farber Cancer Institute November 13 2000 Retrieved 2006 07 12 Kulke M H et al 2006 Phase II study of recombinant human endostatin in patients with advanced neuroendocrine tumors J Clin Oncol 24 22 3555 3561 doi 10 1200 JCO 2006 05 6762 PMID 16877721 Results of phase III trial of rh endostatin YH 16 in advanced non small cell lung cancer NSCLC patients Y Sun J Wang Y Liu X Song Y Zhang K Li Y Zhu Q Zhou L You and C Yao 1 Yin G Liu W An P Li P ding I Planelles V Schwarz E M Min W 2002 Endostatin gene transfer inhibits joint angiogenesis and pannus formation in inflammatory arthritis Mol Ther 5 5 Pt 1 547 54 doi 10 1006 mthe 2002 0590 PMID 11991745 Ryeom S Folkman J March 2009 Role of endogenous angiogenesis inhibitors in Down syndrome J Craniofac Surg 20 Suppl 1 595 6 doi 10 1097 SCS 0b013e3181927f47 PMID 19795527 S2CID 21576950 External links editEndostatin at the U S National Library of Medicine Medical Subject Headings MeSH PBS Nova program explores Endostatin in 2001 Retrieved from https en wikipedia org w index php title Endostatin amp oldid 1215538218, wikipedia, wiki, book, books, library,

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