| Literature DB >> 25174682 |
Armelle Dufresne1, Laurent Alberti, Mehdi Brahmi, Sarah Kabani, Héloïse Philippon, David Pérol, Jean Yves Blay.
Abstract
BACKGROUND: Aggressive fibromatosis (AF) is a rare fibroblastic proliferative disease with a locally aggressive behavior and no distant metastasis, characterized by driver mutations in CTNNB1 or the APC gene. When progressive and/or symptomatic AF is not amenable to local management, a variety of medical treatments may be efficient, including imatinib mesylate. The phase II "Desminib trial" included 40 patients with AF to evaluate the toxicity and efficacy of imatinib resulting in a 65% tumor control rate at 1 year. We investigated a potential predictive value of KIT exon 10 M541L variant (KITL541) on this prospective series.Entities:
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Year: 2014 PMID: 25174682 PMCID: PMC4161827 DOI: 10.1186/1471-2407-14-632
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Figure 1In Competitive Allele-Specific Taqman® PCR technology, each mutant allele assay detects specific mutant alleles and a blocker suppresses the wild type allele.
Characteristics of the 33 patients and their FFPE samples analyzed (%)
| Total | KIT L541 | KIT WT | ||
|---|---|---|---|---|
| n = 33 | n = 5 | n = 22 | ||
|
| ||||
| Gender | Male | 11 (33) | ||
| Female | 22 (67) | |||
| Median age at diagnosis | ||||
| [range], years | 40 [20–72] | 48 [39–57] | 39 [20–72] | |
| Chi-2: p = 0,22 | ||||
| Tumor location | Intra abdo | 6 (18) | - | 2 (9) |
| Abdo wall | 3 (9) | 2 (40) | 4 (18) | |
| Extra abdo | 24 (73) | 3 (60) | 15 (68) | |
| Chi-2: p = 0,51 | ||||
| Median tumor size [range], mm | 100 [25–220] | 70 [60–189] | 92 [33–220] | |
| Chi-2: p = 0,44 | ||||
| Familial Adenomatous Polyposis | Yes | 5 (15) | ||
| No | 28 (85) | |||
| Performans status | 0 | 22 (67) | ||
| 1 | 8 (24) | |||
| 2 | 1 (3) | |||
| Unknown | 2 (6) | |||
| Median TTP [range], months | 24.6 [2.8-42.3] | |||
|
| ||||
| Blocks age | 1997-1999 | 11 (33%) | ||
| 2000-2005 | 22 (66%) | |||
| Mean DNA quantity [range], ng/μl | 782,14 [106,42-1748,86] | |||
| Mean A260/280 ratio [range] | 1,98 [1,76-2,05] | |||
Figure 2For each evaluable patient, the cross represents Ct and the point represents Ct . Bars correspond to ΔCt. Surrounded bars correspond to cases KIT L541. Others bars correspond to cases KIT WT.
Figure 3Determination of status by the 2 methods (sequencing and CAST PCR) for 1 case harbouring and 1 case harbouring . (A) Representative multicomponent and amplification plots and sequencing of KIT L541 (B) Representative multicomponent and amplification plots and sequencing of KIT WT
Distribution of objective response observed at 6 months and 1 year according to status
|
|
| Chi 2 | |
|---|---|---|---|
| Response at 6 months | |||
| CR/PR | 3 | 1 | |
| SD | 15 | 4 | |
| PD | 4 | 0 | |
|
| |||
| Response at 1 year | |||
| CR/PR | 2 | 1 | |
| SD | 13 | 4 | |
| PD | 7 | 0 |
|
Figure 4Log-rank analysis of progression-free survival (PFS) and overall survival (OS) for patients with (M) and without (WT) variant in phase II Desminib trial.