Prognostic significance of interim PET/CT based on visual, SUV-based, and MTV-based assessment in the treatment of peripheral T-cell lymphoma

The clinical characteristics of the 63 enrolled patients are summarized in Table 1. Their median age was 60 years (range, 20–81 years) with 49.2% of patients aged more than 60 years. Thirty-nine patients (61.9%) presented with advanced-stage disease, and 18 (28.6%) had bone marrow involvement. The histological subtypes were PTCL unspecified (n = 17; 27%), angioimmunoblastic T-cell lymphoma (n = 10; 15.9%), NK/T cell (n = 27; 42.9%), and others. Thirty-one patients (49.2%) were classified as high risk based on IPI, and 29 (46%) were classified as high risk (more than 2 factors) based on PIT. Most patients (84.1%) were treated with the CHOP/CHOP-like regimen with a median number of six cycles, and 10 (15.9%) were treated with other induction chemotherapy including IMVP, EPOCH, and VIDL. Fifteen patients, primarily with NK/T cell lymphoma, received a short course of chemotherapy followed by IFRT. Fifty-nine patients underwent interim PET/CT based on the three parameters. Twenty-four patients (38.1%) were classified as having a positive metabolic uptake (grade 4 and 5) based on the visual assessment using 5-PS. According to the response after primary chemotherapy, 34 (54.0%) patients achieved a complete response (CR), 7 (11.1%) achieved a partial response (PR), and 18 (28.6%) showed stable disease (SD) or progression. Nine (14.3%) patients, including those with PR after primary chemotherapy or with high-risk factors, underwent autologous stem cell transplantation as a frontline consolidation. Relapse occurred in 36 patients (57.1%), and the treatment-related mortality was 7.9%. After a median follow up of 40.3 months (range, 12.8–83.2 months), the 3-year OS and PFS rates were 48.3 ± 6.4% and 40.1 ± 6.8%, respectively (Figure 1A). There were no differences in OS depending on histologic subtype, with the exception of anaplastic large cell lymphoma (P = 0.595, Figure 1B). PIT exhibited greater differentiation of survival than IPI (80.8 months in PIT 0–1, 15.0 in PIT 2, and 8.8 months in PIT 3–4, P = 0.011, Figure 1D). Multivariate analysis showed that performance status (≥2), visual (5-PS ≥ 4) and combined (poor responder by all three assessments) assessment in interim PET/CT scans were independent prognostic variables in PFS.

Interim PET/CT images were analyzed by a consensus of two nuclear medicine physicians who were unaware of the clinical information. The sensitivity, specificity, positive predictive value (PPV), and negative predictive value (NPV) of visual assessment (Grade ≥ 3) for the prediction of disease progression were 69.4%, 65.2%, 87.8%, and 96.1%, respectively. Seven patients showed false-positive uptake during primary chemotherapy. Five patients with nasal-type NK/T cell lymphoma continued to have significant metabolic uptakes compared with the mediastinal blood pools that were confirmed to be inflammatory lesions by loco-regional biopsy. In addition, two patients with hot uptake in the gastric and colonic regions were confirmed to show inflammatory changes by endoscopic biopsies. In contrast, three patients classified as grade 3 by visual assessment exhibited false interim PET/CT negativity; however, the original lesion was partially regressed.

Patients with interim PET/CT-positive (grade 4–5) on visual assessment showed a higher relapse rate than patients with interim PET/CT-negative (grade 1–3) (27.3% vs. 9.9%, P = 0.02). In addition, patients with the interim PET/CT-positive showed significantly shorter PFS times compared to patients with interim PET/CT-negative (5.0 vs. 27.0 months, P = 0.000, Figure 2A). However, among the 35 patients classified as interim PET/CT negative, 9 patients with grade 3 had a poor clinical outcome compared with 26 with grades 1–2 (8.8 vs. 64.0 months, P < 0.001; Figure 2B). A high relapse rate in patients with grade 3 or false-negative interpretation of interim PET/CT accounted for the difference in survival.

In ROC analysis, the optimal cutoff values for ΔSUVmax and ΔMTV2.5 were 67.6% with an AUC of 0.673 (P = 0.002, 95% confidence interval (CI); 0.626–0.874) and 98.7% with an AUC of 0.627 (P < 0.001, 95% CI; 0.590–0.852), respectively. Each interim PET/CT assessment based on the ΔSUVmax cutoff, and ΔMTV2.5 cutoff was predictive of disease progression with relatively high positive predictive values (PPV) (92.3% and 92.8%, respectively) and negative predictive values (NPV) (90.0% and 92.8% respectively) (Table 2).

The response assessment of interim PET/CT based on the ΔSUVmax, and ΔMTV2.5 showed significant prognostic potential for PFS. Similarly, based on SUV-based (optimal cutoff value of 67.6%) and MTV-based assessments (optimal cutoff value of 98.7%), the probability of 3-year PFS in the 33 patients who achieved ΔSUVmax > the optimal cutoff was 52.6% compared with 24.7% in the 26 patients who failed to achieve the optimal cutoff (P = 0.001). Moreover, the 3-year PFS rate for 31 patients who achieved ΔMTV2.5 > the optimal cutoff was 49.9%. Furthermore, the 3-year PFS rate for the 28 patients with lower than the optimal cutoff of ΔMTV2.5 was 25.9% (P < 0.005; Figure 2C and D).

Although an interim PET/CT response based on single-parameter assessment could increase the predictive power for clinical outcomes, it was unable to distinguish the outcomes in the good and poor response groups, particularly in patients with grade 3 or higher or those with less than the optimal cutoff of ΔSUVmax or ΔMTV2.5. To increase the predictive accuracy of interim PET/CT, we divided patients into three groups according to the sum of scores for the three adverse responses based on the visual, SUV-based, and MTV-based assessments. This combined assessment using the three parameters consisted of each adverse response, including grade 4 or 5 in 5-PS and little reduction in the optimal cutoffs of ΔSUVmax and ΔMTV2.5: i) favorable responders were satisfied with no adverse response assessed by the three parameters, ii) poor responders had three adverse responses, and iii) intermediate responders were satisfied with one or two adverse responses in three parameters. The clinical outcomes of patients in the favorable group were significantly superior to those of patients in the poor or intermediate responder group (P = 0.002, P = 0.004, respectively, Figure 3A, B). This classification based on the “poor” response category of visual, ΔSUVmax and ΔMTV2.5 assessments on interim PET/CT showed the subdividing ability for predicting the outcomes compared with single-parameter assessment.