| Literature DB >> 24135848 |
Sonia Tejada1, Guillermo Aldave, Miguel Marigil, Jaime Gállego Pérez-Larraya, Jaime de Gallego, Pablo Daniel Domínguez, Ricardo Díez-Valle.
Abstract
Our purpose was to analyze the pattern of failure in glioblastoma (GBM) patients at first recurrence after radiotherapy and temozolomide and its relationship with different factors. From 77 consecutive GBM patients treated at our institution with fluorescence guided surgery and standard radiochemotherapy, 58 first recurrences were identified and included in a retrospective review. Clinical data including age, Karnofsky performance score, preoperative tumor volume and location, extend of resection, MGMT promoter methylation status, time to progression (PFS), overall survival (OS) and adjuvant therapies were reviewed for every patient. Recurrent tumor location respect the original lesion was the end point of the study. The recurrence pattern was local only in 65.5% of patients and non-local in 34.5%. The univariate and multivariate analysis showed that greater preoperative tumor volume in T1 gadolinium enhanced sequences, was the only variable with statistical signification (p < 0.001) for increased rate of non-local recurrences, although patients with MGMT methylation and complete resection of enhancing tumor presented non-local recurrences more frequently. PFS was longer in patients with non-local recurrences (13.8 vs. 6.4 months; p = 0.019, log-rank). However, OS was not significantly different in both groups (24.0 non-local vs. 19.3 local; p = 0.9). Rate of non-local recurrences in our series of patients treated with fluorescence guided surgery and standard radiochemotherapy was higher than previously published in GBM, especially in patients with longer PFS. Greater preoperative enhancing tumor volume was associated with increased rate of non-local recurrences.Entities:
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Year: 2013 PMID: 24135848 PMCID: PMC3889292 DOI: 10.1007/s11060-013-1279-z
Source DB: PubMed Journal: J Neurooncol ISSN: 0167-594X Impact factor: 4.130
Clinical data of patients progressed
| Local recurrence | Non- local recurrence |
| |
|---|---|---|---|
| Mean age | 59 | 58 | 0.312 |
| T1-Gd preoperative volume | 36.7 cc | 49.9 cc | <0.001* |
| T2-FLAIR preoperative volume | 92.73 cc | 81.75 cc | 0.933 |
| Karnofsky | |||
| 70–100 | 72 % | 28 % | 0.175 |
| <70 | 54 % | 46 % | |
| MGMT | |||
| Methylated | 59 % | 41 % | 0.107 |
| Non-methylated | 68 % | 32 % | |
| Extend of resection | |||
| CRET | 59 % | 41 % | 0.412 |
| No CRET | 79 % | 21 % | |
| Included in vaccine trial | 46 % | 52 % | 0.307 |
| Median PFS | 6.4 | 13.8 | 0.019* |
| Median OS | 19.3 | 24 | 0.9 |
CRET complete resection of enhanced tumor, PFS progression free survival, OS overall survival
Fig. 163 years-old female with GBM. MRI at diagnosis (upper row) and first recurrence (lower row). At diagnosis a left parieto-occipital mass was found, hyperintense in T2 FLAIR (arrow in a) and with irregular peripheral enhancement with central necrosis in T1Gd (arrow in b), with normal left temporal lobe (c and d). 13 months after surgery there was no evidence of recurrence at the surgical cavity borders with only treatment-related changes, with gliosis in T2 FLAIR (arrow in e) and a small stable area on enhancement in T1 Gad (arrow in f). Yet a new remote nodule appeared in the left temporal lobe, outside the radiation field (arrows in g and h), confirmed to be a GBM recurrence after surgery
Multivariate analysis including complete resection of enhanced tumor (CRET), fluorescence tissue resection (Fl. Tissue resection), preoperative volume, MEGMT methylation status, age and Karnovsky Performance Score (KPS)
| B | E.T. | Wald | gl | Sig. | Exp (B) | |
|---|---|---|---|---|---|---|
| CRET | 2.242 | 1.283 | 2.743 | 3.055 | 1 | 0.08 |
| Fl. tissue resection | 1.366 | 0.837 | 2.663 | 1 | 0.103 | 3.92 |
| Preoperative volume | 0.032 | 0.016 | 3.968 | 1 |
| 1.033 |
| MGMT-met | 1.367 | 0.797 | 2.946 | 1 | 0.086 | 3.925 |
| Age | −0.014 | 0.034 | 0.158 | 1 | 0.691 | 0.986 |
| KPS | 0.033 | 0.031 | 1.139 | 1 | 0.286 | 1.034 |
Bold value indicates statistically significant
Fig. 2Kaplan–Meier curves for progression free survival (PFS) and overall survival (OS)
Series giving data about pattern of first recurrence in GBM after radiotherapy plus temozolomide
| Patient number | Local-only recurrences (%) | Non-local recurrences (%) | |
|---|---|---|---|
| Series with CRETa | |||
| Petrecca K14 | 20 | 85 | 15 |
| De Bonis P18 | 75 | ||
| Extended resection | 27 | 66.67 | 33.33 |
| Border resection | 48 | 87.5 | 12.50 |
| Series with MGMT analysisb: | |||
| Brandes AA16 | 79 | ||
| Methylated | 19 | 57.87 | 28.13 |
| Non-methylated | 60 | 85 | 15 |
| Niyazi M17 | 52 | ||
| Methylated | 11 | 64.71 | 35.29 |
| Non-methylated | 16 | 88.89 | 11.11 |
| Other series: | |||
| Dobelbower MC12 | 20 | 80 | 20 |
| McDonald MW15 | 41 | 98 | 2 |
| Milano MT 28 | 47 | 89 | 11 |
| Paulsson, AK13 | |||
| Chamberlain MC11 | 80 | 80 | 20 |
The numbers of patients included in this table are only cases with first recurrence, and the percentage is of the number of first recurrences. Only the data of the patients with known MGMT status has been included
aSeries that analyze complete resection of enhance tumor (CRET)
bSeries that give separate information of cases with methylated MGMT promoter versus non-methylated