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Genetic and Telomere Characteristics of High of Grade Soft Tissue Sarcomas

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ClinicalTrials.gov Identifier: NCT02547376
Recruitment Status : Recruiting
First Posted : September 11, 2015
Last Update Posted : February 7, 2019
Sponsor:
Information provided by (Responsible Party):
University Hospitals, Leicester

Brief Summary:

Soft tissue sarcomas (STSs) are a rare group of cancers that can arise in any 'soft' tissue but commonly involve muscles, fat and nerves. Even following surgery and radiotherapy over 50% of tumours will recur or spread and at present, there is no reliable test that allows doctors to predict in which patients this will occur.

DNA that is not inside cells (cell-free or cfDNA) is present in very small quantities circulating in blood. In cancer patients some of this cfDNA comes from cancer cells. Analysis of cancer-derived cfDNA in patients with other cancers has shown that the quantity and characteristics of cfDNA changes with stage of disease and treatment. The researchers plan to investigate the abundance and persistence of cancer-derived cfDNA in STS patients at various stages of disease to investigate the potential role of these characteristics as biomarkers.

Selection of the genetic characters to be tracked in the patients' cfDNA is an important consideration. An established hallmark of a cancer cell is the ability to undergo an unlimited number of cell divisions. In normal human cells protective structures on the ends of chromosomes called telomeres provide a mechanism to limit the number of times a healthy cell can divide. This limitation has to be overcome in cancer cells for a tumour to form. This occurs by the activation of one of two telomere maintenance mechanisms (TMM) - either an enzyme called Telomerase or a mechanism known as Alternative Lengthening of Telomeres (ALT). In many sarcomas the activation of either TMM is associated with genetic changes (mutations) in a small number of genes. As these mutations are not present in normal cells but mark an essential feature of cancer cells (and their capacity for unlimited cell division) they are likely to be reliable markers of the presence of STS cells.

The investigators plan to develop sensitive, quantitative assays to detect TMM associated mutations in tumour derived cfDNA in the blood of patients with STSs, and track these mutations overtime. They will establish the amount of cancer-derived cfDNA in STS patients at the time of surgery, and persistence of this cfDNA during follow up visits following tumour resection and in the events of local tumour recurrence or spread (metastatic disease). Once these basic parameters are established analysis will be broadened to include other genes that are commonly mutated in STSs with a view of identifying other genetic characteristics that may also aid identification of patients at high risk of recurrence or spread. In summary all of the assays described above should facilitate better monitoring of patients with STS, and allow earlier treatment if STS recurs following surgery.


Condition or disease
Soft Tissue Sarcoma

Detailed Description:

Aims

The investigators plan a 2 year pilot observational study to:

  • Identify and quantify circulating cell-fee DNA (cfDNA) in cases of Soft Tissue Sarcoma (STS)
  • Investigate Telomere Maintenance Mechanisms (TMM) in STSs.
  • Use TMM associated genetic mutations to identify and quantify tumour-derived cfDNA in STSs at time of tumour resection and throughout follow up
  • Track the tumour derived cfDNA characteristics above over time and correlate with clinical outcome to identify potential STS biomarkers Hypotheses Based on findings in other cancers it is hypothesised that plasma cfDNA will be detectable in cases of STS. Given the key role telomere length maintenance plays in cancer cell development the investigators also hypothesise that TMM associated mutations will be present in tumour derived cfDNA, act as stable markers of STS tissue, and therefore increase in concentration as local recurrence or metastatic disease occurs.

Tumour derived cfDNA identification In months 0-3 sensitive assays to target known tumour-specific mutations will be developed. Using these on retrospectively collected tissues the investigators will verify that cfDNA can be detected (and quantified) in the plasma of patients with STSs.

Analysis of TMMs in STS tissue In months 3-12 tumour samples from every prospectively recruited sample will be analysed to establish which TMM is activated in STSs. Telomerase and ALT activity will each be assessed by published laboratory techniques.

Quantification and characterisation of TMM associated mutations / tumour derived cfDNA In months 10-12 quantitative Polymerase Chain Reaction based assays will be developed to identify the TMM associated mutations found to be most prevalent in STSs. In months 12-22 these assays will be used to identify and quantify these TMM associated mutations (and therefore also tumour-derived cfDNA) in the plasma samples taken from every prospectively recruited patient at time of surgery and throughout follow up.

Correlation of cfDNA characteristics with clinical outcome In months 22-24 cfDNA concentration, tumour-derived cfDNA concentration and the genetic characteristics of both will be correlated with clinical outcome measure including local recurrence, metastatic recurrence and death to determine these characteristics' potential as future biomarkers.

Patient recruitment / sample collection Patients will be recruited through the East Midlands Sarcoma Service. Samples already available will be collected from 2 sources to verify that cfDNA can be detected in STSs: Firstly 20 patients with metastatic disease will be asked to give consent for retrospective analysis of their tumour tissue already archived following histological analysis. One blood sample will also be collected from these patients for analysis. Secondly every STS sample already stored in the Nottingham Health Science Biobank, (Nottingham City Hospital) with an accompanying plasma sample also stored (15 at time of writing) will be analysed.

For the investigators remaining analysis between months 0-22 patients with non-metastatic high-grade STSs undergoing a planned resection locally will be approached to participate. 2013 figures suggest over 100 patients will be eligible for inclusion. Tumour tissue, blood, and unaffected muscle and saliva (2 sources of control DNA) will be collected at time of resection. Repeat blood samples will be collected 3 monthly until the end of recruitment.


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Study Type : Observational
Estimated Enrollment : 100 participants
Observational Model: Case-Only
Time Perspective: Prospective
Official Title: Genetic and Telomere Characteristics of High of Grade Soft Tissue Sarcomas
Study Start Date : February 2015
Estimated Primary Completion Date : February 2021
Estimated Study Completion Date : February 2021

Resource links provided by the National Library of Medicine


Group/Cohort
Eligible patients with Soft Tissue Sarcoma
Primary Soft Tissue Sarcoma group



Primary Outcome Measures :
  1. Disease recurrence (local and distant) post surgery [ Time Frame: 18 months ]

Secondary Outcome Measures :
  1. Overall survival [ Time Frame: 18 months ]

Biospecimen Retention:   Samples With DNA
Soft tissue sarcoma tissue Blood (Plasma and Buffy coat) Saliva


Information from the National Library of Medicine

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Ages Eligible for Study:   18 Years and older   (Adult, Older Adult)
Sexes Eligible for Study:   All
Accepts Healthy Volunteers:   No
Sampling Method:   Non-Probability Sample
Study Population
Patient managed by East Midland Sarcoma Service with Soft Tissue Sarcoma undergoing attempted curative resection
Criteria

Inclusion Criteria:

  1. Cases of nonmetastatic biopsy proven highgrade soft tissue sarcoma (STS) presenting to the East Midlands Sarcoma Service
  2. Cases to be treated with curative intent with surgical resection (+/adjuvant therapy)

Exclusion Criteria:

  1. Cases presenting with local or distant recurrence
  2. Retroperitoneal soft tissue sarcomas
  3. Patients unable to provide informed consent
  4. Patients aged under 18

Information from the National Library of Medicine

To learn more about this study, you or your doctor may contact the study research staff using the contact information provided by the sponsor.

Please refer to this study by its ClinicalTrials.gov identifier (NCT number): NCT02547376


Contacts
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Contact: Nicholas C Eastley, MBChB +441162231727 nce8@le.ac.uk
Contact: Robert U Ashford, MBBS, FRCS +44116 265 3042 robert.ashford@uhl-tr.nhs.uk

Locations
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United Kingdom
University Hospitals of Leicester NHS Trust Recruiting
Leicester, Leicestershire, United Kingdom, LE5 4PW
Contact: Carolyn Maloney    0116 258 4109    carolyn.maloney@uhl-tr.nhs.uk   
Contact: Tara Sadler    0116 258 8246    tara.sadler@uhl-tr.nhs.uk   
Sponsors and Collaborators
University Hospitals, Leicester

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Responsible Party: University Hospitals, Leicester
ClinicalTrials.gov Identifier: NCT02547376     History of Changes
Other Study ID Numbers: UHL 11353
First Posted: September 11, 2015    Key Record Dates
Last Update Posted: February 7, 2019
Last Verified: February 2019

Keywords provided by University Hospitals, Leicester:
Telomeres
Telomerase
Alternative lengthening of Telomeres Mechanism

Additional relevant MeSH terms:
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Sarcoma
Neoplasms, Connective and Soft Tissue
Neoplasms by Histologic Type
Neoplasms