Tumor-penetrating peptide for systemic targeting of Tenascin-C

Lingasamy, Prakash; Tobi, Allan; Kurm, Kaarel; Kopanchuk, Sergei; Sudakov, Aleksander; Salumäe, Markko; Rätsep, Tõnu; Asser, Toomas; Bjerkvig, Rolf; Teesalu, Tambet

doi:10.1038/s41598-020-62760-y

Cited by 44 publications

(34 citation statements)

References 53 publications

(79 reference statements)

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“…Several ECM components such as fibronectin ( FN1 ) [ 65 ], tenascin C ( TNC ) [ 66 ], thrombospondin 1 ( THBS1) [ 67 ] and osteopontin ( SPP1 ) [ 68 ], which were highly overexpressed in our dataset, are associated with an adverse prognosis and represent potential therapeutic targets [ 2 , 65 , 66 , 67 , 68 ]. Unfortunately, many ECM-related proteins are not exclusively expressed in cancer tissues, making direct targeting difficult.…”

Section: Discussionmentioning

confidence: 99%

“…In summary, we revealed an overexpression of ECM components, which are associated with enhanced migratory capacities of tumour cells ( TNC [ 76 , 77 ], FN1 [ 78 ]), resistance to chemotherapy ( COL11A1 [ 43 , 75 ], SPP1 [ 79 ]) and adverse outcome ( COL11A1 [ 42 ], TNC [ 80 ], FN1 [ 78 ]) in other primaries. The functional role of these molecules and their potential as therapeutic targets are currently under intense investigation [ 65 , 66 , 75 , 79 , 81 , 82 ]. Hence, as new therapeutic approaches for SGC are needed, our findings are of high translational relevance.…”

Section: Discussionmentioning

confidence: 99%

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Expression Profiling of Extracellular Matrix Genes Reveals Global and Entity-Specific Characteristics in Adenoid Cystic, Mucoepidermoid and Salivary Duct Carcinomas

Arolt

Meyer

Hoffmann

et al. 2020

Cancers

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The composition of the extracellular matrix (ECM) plays a pivotal role in tumour initiation, metastasis and therapy resistance. Until now, the ECM composition of salivary gland carcinomas (SGC) has not been studied. We quantitatively analysed the mRNA of 28 ECM-related genes of 34 adenoid cystic (AdCy; n = 11), mucoepidermoid (MuEp; n = 14) and salivary duct carcinomas (SaDu; n = 9). An incremental overexpression of six collagens (including COL11A1) and four glycoproteins from MuEp and SaDu suggested a common ECM alteration. Conversely, AdCy and MuEp displayed a distinct overexpression of COL27A1 and LAMB3, respectively. Nonhierarchical clustering and principal component analysis revealed a more specific pattern for AdCy with low expression of the common gene signature. In situ studies at the RNA and protein level confirmed these results and indicated that, in contrast to MuEp and SaDu, ECM production in AdCy results from tumour cells and not from cancer-associated fibroblasts (CAFs). Our findings reveal different modes of ECM production leading to common and distinct RNA signatures in SGC. Of note, an overexpression of COL27A1, as in AdCy, has not been linked to any other neoplasm so far. Here, we contribute to the dissection of the ECM composition in SGC and identified a panel of deferentially expressed genes, which could be putative targets for SGC therapy and overcoming therapeutic resistance.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Expression Profiling of Extracellular Matrix Genes Reveals Global and Entity-Specific Characteristics in Adenoid Cystic, Mucoepidermoid and Salivary Duct Carcinomas

Arolt

Meyer

Hoffmann

et al. 2020

Cancers

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“…iRGD peptide is clinically developed by CEND Therapeutics Inc. (La Jolla, CA, USA) in phase I clinical trial on pancreatic cancer patients as an add-on treatment in combination with Abraxane and gemcitabine (clinical trial identifier: NCT03517176). Other vascular-homing peptides cilengitide (sequence: RGDfV) ( 9 ), SFITGv6 (sequence: GRCTFRGDLMQLCYPD) ( 10 ), CNGRC (sequence: CNGRC) ( 11 ), tumor extracellular matrix (ECM) homing peptides DAG (sequence: CDAGRKQKC) ( 12 ), ZD2 (sequence: CTVRTSADC) ( 13 ), PL1 (sequence: PPRRGLIKLKTS) ( 14 ) and PL3 (sequence: AGRGRLVR) ( 15 ), IP3 (sequence: CKRDLSRRC) ( 16 ), CAR (sequence: CARSKNKDC) ( 17 ) and M2 tumor-associated macrophage targeting UNO peptide ( 18 ) have been selected for possible therapeutic use and reviewed recently ( 19 ). Moreover, healthy organs can be specifically targeted with homing peptides.…”

Section: Introductionmentioning

confidence: 99%

In vivo phage display: identification of organ-specific peptides using deep sequencing and differential profiling across tissues

Pleiko

Põšnograjeva

Haugas

et al. 2021

Nucleic Acids Research

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In vivo phage display is widely used for identification of organ- or disease-specific homing peptides. However, the current in vivo phage biopanning approaches fail to assess biodistribution of specific peptide phages across tissues during the screen, thus necessitating laborious and time-consuming post-screening validation studies on individual peptide phages. Here, we adopted bioinformatics tools used for RNA sequencing for analysis of high-throughput sequencing (HTS) data to estimate the representation of individual peptides during biopanning in vivo. The data from in vivo phage screen were analyzed using differential binding—relative representation of each peptide in the target organ versus in a panel of control organs. Application of this approach in a model study using low-diversity peptide T7 phage library with spiked-in brain homing phage demonstrated brain-specific differential binding of brain homing phage and resulted in identification of novel lung- and brain-specific homing peptides. Our study provides a broadly applicable approach to streamline in vivo peptide phage biopanning and to increase its reproducibility and success rate.

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“…Endoglin (ENG) is another CAF marker associated with adverse outcomes, and it has been shown to promote castration-resistant prostate cancer [49][50][51]. Tenascin C (TNC), 5'-nucleotidase ecto (NT5E), and platelet-derived growth factor receptor beta (PDGFRβ) are other CAF markers that are currently candidate targets for imaging or therapeutics [52][53][54][55].…”

mentioning

confidence: 99%

“…While the overall expression of NT5E, TNC, and PDGFRβ did not change in the tumor microenvironment, ASPN expression was altered in these cells. Studies are currently assessing NT5E, TNC, and PDGFRβ as candidates for therapeutic targeting [52][53][54][55]. To date, strategies targeting ASPN directly have not been reported, and therefore, therapies directed to these other markers may be an ideal way to target ASPN + fibroblasts.…”

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confidence: 99%

A distinct repertoire of cancer‐associated fibroblasts is enriched in cribriform prostate cancer

Hesterberg

Rios

Wolf

et al. 2021

The Journal of Pathology CR

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Outcomes for men with localized prostate cancer vary widely, with some men effectively managed without treatment on active surveillance, while other men rapidly progress to metastatic disease despite curative-intent therapies. One of the strongest prognostic indicators of outcome is grade groups based on the Gleason grading system. Gleason grade 4 prostate cancer with cribriform morphology is associated with adverse outcomes and can be utilized clinically to improve risk stratification. The underpinnings of disease aggressiveness associated with cribriform architecture are not fully understood. Most studies have focused on genetic and molecular alterations in cribriform tumor cells; however, less is known about the tumor microenvironment in cribriform prostate cancer. Cancer-associated fibroblasts (CAFs) are a heterogeneous population of fibroblasts in the tumor microenvironment that impact cancer aggressiveness. The overall goal of this study was to determine if cribriform prostate cancers are associated with a unique repertoire of CAFs. Radical prostatectomy whole-tissue sections were analyzed for the expression of fibroblast markers (ASPN in combination with FAP, THY1, ENG, NT5E, TNC, and PDGFRβ) in stroma adjacent to benign glands and in Gleason grade 3, Gleason grade 4 cribriform, and Gleason grade 4 noncribriform prostate cancer by RNAscope ® . Halo ® Software was used to quantify percent positive stromal cells and expression per positive cell. The fibroblast subtypes enriched in prostate cancer were highly heterogeneous. Both overlapping and distinct populations of low abundant fibroblast subtypes in benign prostate stroma were enriched in Gleason grade 4 prostate cancer with cribriform morphology compared to Gleason grade 4 prostate cancer with noncribriform morphology and Gleason grade 3 prostate cancer. In addition, gene expression was distinctly altered in CAF subtypes adjacent to cribriform prostate cancer. Overall, these studies suggest that cribriform prostate cancer has a unique tumor microenvironment that may distinguish it from other Gleason grade 4 morphologies and lower Gleason grades.

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Tumor-penetrating peptide for systemic targeting of Tenascin-C

Cited by 44 publications

References 53 publications

Expression Profiling of Extracellular Matrix Genes Reveals Global and Entity-Specific Characteristics in Adenoid Cystic, Mucoepidermoid and Salivary Duct Carcinomas

Expression Profiling of Extracellular Matrix Genes Reveals Global and Entity-Specific Characteristics in Adenoid Cystic, Mucoepidermoid and Salivary Duct Carcinomas

In vivo phage display: identification of organ-specific peptides using deep sequencing and differential profiling across tissues

A distinct repertoire of cancer‐associated fibroblasts is enriched in cribriform prostate cancer

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