Cancer chemotherapy based on targeting of cytotoxic peptide conjugates to their receptors on tumors

In view of non-specific toxicity of most chemotherapeutic agents against normal cells, the development of targeted chemotherapy is warranted. Efficient targeting of chemotherapeutic drugs to the cancerous area could be of great benefit for patients with advanced or metastatic tumors. Targeted cytotoxic peptide conjugates are hybrid molecules composed of a peptide carrier which binds to receptors on tumors and a cytotoxic moiety. New cytotoxic analogs of LHRH, AN-152 in which doxorubicin (DOX) is linked to [d-Lys(6)]LHRH, and AN-207 which consists of 2-pyrrolino-DOX (AN-201) coupled to the same carrier, show high-affinity binding and are much less toxic and more effective in vivo than their respective radicals in inhibiting tumor growth in LHRH receptor-positive models of human ovarian, mammary, or prostatic cancer. These results suggest that targeted cytotoxic LHRH analogs such as AN-207 could be considered for treatment of these cancers. The presence of receptors for bombesin-like peptides on a wide variety of tumors prompted us to use some of our bombesin/gastrin-releasing peptide antagonists as carrier molecules. Cytotoxic bombesin analogs, such as AN-215 containing AN-201, might find application in the treatment of small cell lung carcinoma (SCLC), and colorectal, gastric, pancreatic, mammary, and prostatic cancers. Since somatostatin receptors are found in various human neoplasms and the receptor subtypes to which octapeptide analogs bind with high affinity have been identified, we synthesized several cytotoxic somatostatin analogs including AN-162 and AN-238 containing DOX and 2-pyrrolino-DOX respectively, linked to octapeptide RC-121. Cytotoxic somatostatin analog AN-238 efficaciously inhibits growth of human breast or prostate cancers expressing somatostatin receptors-2 and -5 and can be used for receptor-targeted chemotherapy. Cytotoxic somatostatin analogs might also find applications for the therapy of human pancreatic, colorectal, and gastric cancer as well as brain tumors and non-SCLC. Cytotoxic compounds linked to analogs of hormonal peptides like LHRH, bombesin, and somatostatin that can be targeted to certain tumors possessing receptors for those peptides could be an important addition to oncological armamentarium.

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Novel insights in somatostatin receptor physiology

Acta Endocrinologica ◽

10.1530/eje.1.02354 ◽

2007 ◽

Vol 156 (suppl_1) ◽

pp. S3-S11 ◽

Cited By ~ 42

Author(s):

Giovanni Tulipano ◽

Stefan Schulz

Keyword(s):

Somatostatin Receptor ◽

Somatostatin Receptors ◽

Somatostatin Analogs ◽

Receptor Subtypes ◽

Ligand Complex ◽

Endosomal Sorting ◽

Intracellular Vesicle ◽

Molecular Events ◽

Somatostatin Receptor Subtypes

The experimental data reviewed in the present paper deal with the molecular events underlying the agonist-dependent regulation of the distinct somatostatin receptor subtypes and may suggest important clues about the clinical use of somatostatin analogs with different pattern of receptor specificity for the in vivo targeting of tumoral somatostatin receptors. Somatostatin receptor subtypes are characterized by differential β-arrestin trafficking and endosomal sorting upon agonist binding due, at least in part, to the differences in their C-terminal tails. Moreover, the subcellular expression pattern of somatostatin receptor subtypes and their activity in response to agonist treatment are affected by intracellular complements, such as proteins involved in intracellular vesicle trafficking. Different somatostatin analogs may induce distinct conformations of the receptor/ligand complex, preferentially coupled to either receptor signaling or receptor endocytosis.

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Immunohistochemical Expression of Somatostatin Receptor Subtypes in a Panel of Neuroendocrine Neoplasias

Journal of Histochemistry & Cytochemistry ◽

10.1369/0022155419856900 ◽

2019 ◽

Vol 67 (10) ◽

pp. 735-743 ◽

Cited By ~ 2

Author(s):

Satu M. Remes ◽

Helena L. Leijon ◽

Tiina J. Vesterinen ◽

Johanna T. Arola ◽

Caj H. Haglund

Keyword(s):

Somatostatin Receptor ◽

Somatostatin Receptors ◽

Somatostatin Analogs ◽

Membrane Receptors ◽

Receptor Subtypes ◽

Receptor Imaging ◽

Primary Tumors ◽

Somatostatin Receptor Subtypes ◽

Negative Controls ◽

G Protein Coupled

Neuroendocrine neoplasias (NENs) are known to express somatostatin receptors (SSTRs) 1–5, which are G-protein-coupled cell membrane receptors. Somatostatin receptor imaging and therapy utilizes the SSTR expression. Synthetic somatostatin analogs with radioligands are used to detect primary tumors, metastases, and recurrent disease. Receptor analogs are also used for treating NENs. Furthermore, commercially available SSTR antibodies can be used for the immunohistochemical (IHC) detection of SSTRs. We investigated different SSTR antibody clones applying diverse IHC protocol settings to identify reliable clones and feasible protocols for NENs. A tissue microarray including NENs from 12 different primary sites were stained. Only UMB clones were able to localize SSTR on the cell membranes of NENs. SSTR2 (UMB1) emerged as the most common subtype followed by SSTR5 (UMB4) and SSTR1 (UMB7). SSTR3 (UMB5) expression was mainly cytoplasmic. Yet, SSTR4 expression was weak and located primarily in the cytoplasm. Thus, appropriate IHC protocols, including proper positive and negative controls, represent requirements for high-quality NEN diagnostics and for planning personalized therapy.

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Characterization and sub-cellular localization of somatostatin receptors in DU-145 and PC-3 human androgen-independent prostate cancer cells: effect of mono- and bi-specific somatostatin analogs on cell growth

Endocrine Abstracts ◽

10.1530/endoabs.32.p514 ◽

2013 ◽

Author(s):

Massimiliano Ruscica ◽

Marica Arvigo ◽

Liliana Steffani ◽

Federico Gatto ◽

Manuela Albertelli ◽

...

Keyword(s):

Prostate Cancer ◽

Cell Growth ◽

Cancer Cells ◽

Cellular Localization ◽

Somatostatin Receptors ◽

Somatostatin Analogs ◽

Prostate Cancer Cells ◽

Androgen Independent

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A High-Affinity Human Antibody That Targets Tumoral Blood Vessels

Blood ◽

10.1182/blood.v94.1.192.413k22_192_198 ◽

1999 ◽

Vol 94 (1) ◽

pp. 192-198 ◽

Cited By ~ 141

Author(s):

Lorenzo Tarli ◽

Enrica Balza ◽

Francesca Viti ◽

Laura Borsi ◽

Patrizia Castellani ◽

...

Keyword(s):

Blood Vessels ◽

Small Cell Lung Carcinoma ◽

Antibody Fragment ◽

Human Colon ◽

Experimental Models ◽

Human Antibody ◽

Cell Lung Carcinoma ◽

High Affinity ◽

Biodistribution Studies

Angiogenesis is a characteristic feature of many aggressive tumors and of other relevant disorders. Molecules capable of specifically binding to new-forming blood vessels, but not to mature vessels, could be used as selective vehicles and would, therefore, open diagnostic and therapeutic opportunities. We have studied the distribution of the ED-B oncofetal domain of fibronectin, a marker of angiogenesis, in four different tumor animal models: the F9 murine teratocarcinoma, SKMEL-28 human melanoma, N592 human small cell lung carcinoma, and C51 human colon carcinoma. In all of these experimental models we observed accumulation of the fibronectin isoform containing the ED-B domain around neovascular structures when the tumors were in the exponentially growing phase, but not in the slow-growing phase. Then we performed biodistribution studies in mice bearing a subcutaneously implanted F9 murine teratocarcinoma, using a high-affinity human antibody fragment (L19) directed against the ED-B domain of fibronectin. Radiolabeled L19, but not an irrelevant anti-lysozyme antibody fragment (D1.3), efficiently localizes in the tumoral vessels. The maximal dose of L19 accumulated in the tumor was observed 3 hours after injection (8.2% injected dose per gram). By virtue of the rapid clearance of the antibody fragment from the circulation, tumor-to-blood ratios of 1.9, 3.7, and 11.8 were obtained at 3, 5, and 24 hours, respectively. The tumor-targeting performance of L19 was not dose-dependent in the 0.7 to 10 μg range of injected antibody. The integral of the radioactivity localized in tumoral vessels over 24 hours was greater than 70-fold higher than the integral of the radioactivity in blood over the same time period, normalized per gram of tissue or fluid. These findings quantitatively show that new-forming blood vessels can selectively be targeted in vivo using specific antibodies, and suggest that L19 may be of clinical utility for the immunoscintigraphic detection of angiogenesis in patients.

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Cholecystokinin receptors

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.1995.269.5.g628 ◽

1995 ◽

Vol 269 (5) ◽

pp. G628-G646 ◽

Cited By ~ 48

Author(s):

S. A. Wank

Keyword(s):

Function Analysis ◽

Receptor Gene ◽

Wide Distribution ◽

Receptor Expression ◽

Receptor Subtypes ◽

Cck Receptors ◽

High Affinity ◽

Recombinant Receptor ◽

Receptor Pharmacology ◽

Specific Variation

The cholecystokinin (CCK) and gastrin families of peptides act as hormones and neuropeptides on central and peripheral CCK receptors to mediate secretion and motility in the gastrointestinal (GI) tract in the physiological response to a normal meal. CCK and its receptors are also widely distributed in the central nervous system (CNS) and contribute to the regulation of satiety, anxiety, analgesia, and dopamine-mediated behavior. Although the wide distribution, myriad number of functions, and reported pharmacological heterogeneity of CCK receptors would suggest a large number of receptor subtypes, the application of modern molecular biological techniques has identified two CCK receptors, CCK-A receptor (CCK-AR) and CCK-B receptor (CCK-BR), that mediate the actions of CCK and gastrin; gastrin receptors have been found to be identical to CCK-BR. CCK-AR, found predominantly in the GI system and select areas of the CNS, have high affinity for CCK and the nonpeptide antagonist L-364,718, whereas CCK-BR, found predominantly in the CNS and select areas of the GI system, have high affinity for CCK and gastrin and the nonpeptide antagonist L-365,260. Both CCK-AR and CCK-BR are highly conserved between species, although there is some tissue-specific variation in expression. Recombinant receptor expression faithfully reproduces the native receptor pharmacology and signal transduction pathways, allowing direct comparisons of receptor function between species as well as serving as a convenient source of receptor. Our present knowledge of the chromosomal localization, receptor gene structure, and primary sequence will allow further studies in disease association, receptor regulation, and structure-function analysis.

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68Ga-DOTANOC: a first compound for PET imaging with high affinity for somatostatin receptor subtypes 2 and 5

European Journal of Nuclear Medicine and Molecular Imaging ◽

10.1007/s00259-004-1697-4 ◽

2004 ◽

Vol 32 (6) ◽

pp. 724-724 ◽

Cited By ~ 117

Author(s):

Damian Wild ◽

Helmut R. Mäcke ◽

Beatrice Waser ◽

Jean Claude Reubi ◽

Mihaela Ginj ◽

...

Keyword(s):

Pet Imaging ◽

Somatostatin Receptor ◽

Receptor Subtypes ◽

High Affinity ◽

Somatostatin Receptor Subtypes

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Transport of antimicrobial agents using peptide carrier systems: anticandidal activity of m-fluorophenylalanine-peptide conjugates

Journal of Medicinal Chemistry ◽

10.1021/jm00366a013 ◽

1983 ◽

Vol 26 (12) ◽

pp. 1725-1729 ◽

Cited By ~ 29

Author(s):

William D. Kingsbury ◽

Jeffrey C. Boehm ◽

Rajanikant J. Mehta ◽

Sarah F. Grappel

Keyword(s):

Antimicrobial Agents ◽

Peptide Conjugates ◽

Peptide Carrier ◽

Anticandidal Activity ◽

Carrier Systems

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Evaluation of a New 177Lu-Labeled Somatostatin Analog for the Treatment of Tumors Expressing Somatostatin Receptor Subtypes 2 and 5

Molecules ◽

10.3390/molecules25184155 ◽

2020 ◽

Vol 25 (18) ◽

pp. 4155

Author(s):

Rosalba Mansi ◽

Guillaume Pierre Nicolas ◽

Luigi Del Pozzo ◽

Karim Alexandre Abid ◽

Eric Grouzmann ◽

...

Keyword(s):

Somatostatin Receptor ◽

Somatostatin Analogs ◽

Somatostatin Analog ◽

Receptor Subtypes ◽

In Vivo Evaluation ◽

Somatostatin Receptor Subtypes ◽

Lower Extent ◽

Lower Background

Targeted radionuclide therapy of somatostatin receptor (SST)-expressing tumors is only partially addressed by the established somatostatin analogs having an affinity for the SST subtype 2 (SST2). Aiming to target a broader spectrum of tumors, we evaluated the bis-iodo-substituted somatostatin analog ST8950 ((4-amino-3-iodo)-d-Phe-c[Cys-(3-iodo)-Tyr-d-Trp-Lys-Val-Cys]-Thr-NH2), having subnanomolar affinity for SST2 and SST5, labeled with [177Lu]Lu3+ via the chelator DOTA (1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid). Human Embryonic Kidney (HEK) cells stably transfected with the human SST2 (HEK-SST2) and SST5 (HEK-SST5) were used for in vitro and in vivo evaluation on a dual SST2- and SST5-expressing xenografted mouse model. natLu-DOTA-ST8950 showed nanomolar affinity for both subtypes (IC50 (95% confidence interval): 0.37 (0.22–0.65) nM for SST2 and 3.4 (2.3–5.2) for SST5). The biodistribution of [177Lu]Lu-DOTA-ST8950 was influenced by the injected mass, with 100 pmol demonstrating lower background activity than 10 pmol. [177Lu]Lu-DOTA-ST8950 reached its maximal uptake on SST2- and SST5-tumors at 1 h p.i. (14.17 ± 1.78 and 1.78 ± 0.35%IA/g, respectively), remaining unchanged 4 h p.i., with a mean residence time of 8.6 and 0.79 h, respectively. Overall, [177Lu]Lu-DOTA-ST8950 targets SST2-, SST5-expressing tumors in vivo to a lower extent, and has an effective dose similar to clinically used radiolabeled somatostatin analogs. Its main drawbacks are the low uptake in SST5-tumors and the persistent kidney uptake.

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trans-2-(2,5-Dimethoxy-4-iodophenyl)cyclopropylamine and trans-2-(2,5-dimethoxy-4-bromophenyl)cyclopropylamine as potent agonists for the 5-HT2 receptor family

Beilstein Journal of Organic Chemistry ◽

10.3762/bjoc.8.194 ◽

2012 ◽

Vol 8 ◽

pp. 1705-1709 ◽

Cited By ~ 9

Author(s):

Adam Pigott ◽

Stewart Frescas ◽

John D McCorvy ◽

Xi-Ping Huang ◽

Bryan L Roth ◽

...

Keyword(s):

Serotonin Receptor ◽

Side Chain ◽

Receptor Subtypes ◽

Receptor Function ◽

High Affinity ◽

Receptor Family

A strategy to replace the ethylamine side chain of 2,5-dimethoxy-4-iodoamphetamine (DOI, 1a), and 2,5-dimethoxy-4-bromoamphetamine (DOB, 1b) with a cyclopropylamine moiety was successful in leading to compounds with high affinity at the 5-HT2 family of receptors; and the more potent stereoisomer of the cyclopropane analogues had the expected (−)-(1R,2S)-configuration. Screening for affinity at various serotonin receptor subtypes, however, revealed that the cyclopropane congeners also had increased affinity at several sites in addition to the 5-HT2A and 5-HT2B receptors. Therefore, at appropriate doses – although (−)-4 and (−)-5 may be useful as tools to probe 5-HT2 receptor function – one would need to be mindful that their selectivity for 5-HT2A receptors is somewhat less than for DOI itself.

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