Randomized placebo-controlled double-blind phase II study of zaltoprofen for patients with diffuse-type and unresectable localized tenosynovial giant cell tumors: a study protocol

A tenosynovial giant cell tumor (TGCT) is a locally aggressive benign neoplasm arising from intra- or extra-articular tissue. A localized extra-articular TGCT, also known as a giant cell tumor of the tendon sheath, commonly emerges from the smaller joints including the hand and ankle/foot. It is slight more predominant in women than in men [1] and an annual incidence has been reported as approximately one in 50,000 [2]. Diffuse TGCT (D-TGCT), is a synonymous with pigmented villonodular synovitis, grows in the large joint such as the knee, hip, ankle, elbow, and shoulder. and the recurrence rete is high despite the surgical removal. An incidence of it has been reported as approximately two cases per million annually with mostly younger than 40 years and a slight female predominance [3]. Surgical removal (open or arthroscopic synovectomy) is the only effective treatment, but the local recurrence rate has been reported to be 16 to 47% [4, 5]. It has been reported that TGCT growth is driven by overexpression of colony-stimulating factor 1 (CSF1) as a result of fusion of the CSF1 gene to the collagen type VI α3 (COL6A3) promoter in the t(1;2) translocation [6]. Therefore, systemic therapies targeting the CSF1/CSF1R axis have been tested in patients with locally advanced or relapsed D-TGCT [7].

Recently, we reported the case of a giant cell tumor of bone arising in the right distal femur, which demonstrated adipocyte lineage, strong expression of peroxisome proliferator-activated receptor gamma (PPARγ), and complete necrosis after taking zaltoprofen, a nonsteroidal anti-inflammatory drug (NSAID) for four weeks before biopsy [8]. PPARγ is a key transcriptional factor stimulates the adipocyte differentiation [9]. It also has the ability of antitumor activity by inhibiting tumor proliferation and invasion and through the induction of differentiation and apoptosis. PPARγ ligands including synthetic ligands such as thiazolidinedione (TZD) [10] and 15-deoxy-delta-12,14-prostaglandin J2 (15d-PGJ2) [11] have been investigated. Certain of NSAIDs, including indomethacin, play the role as direct ligands for PPARγ [12]. Zaltoprofen has been reported to induce apoptosis in rheumatoid synovial cells via the activation of PPARγ [13]. In some types of cancer, including liposarcoma [14], as well as colon cancer [15], breast cancer [16], and prostate cancer [17], the targeted-therapy for PPARγ has been tried. The long-term safety of zaltoprofen in the patients with rheumatoid arthritis was reported [18]. Based on those approaches, we analyzed the antitumor effect of zaltoprofen on primary cultured cells from TGCT, and zaltoprofen was found to inhibit their cell proliferation via activation of PPARγ [19].

We conducted a pilot study of zaltoprofen treatment for diffuse-type TGCTs arising in knee and ankle joints. This study included ten patients (6 knees and 4 ankles). Oral zaltoprofen (240 mg) was given daily for 48 weeks or until the disease was deemed progressive. Eight patients maintained stable disease at 48 weeks and one patient showed progressive disease at 72 weeks. At their request, surgery was performed for 3 patients with ankle D-TGCT at 12, 24, and 48 weeks, although all of them maintained stable disease. Since the zaltoprofen was well-tolerated and maintained stable disease [20], it could be a treatment option in patients with TGCT.

Herein, we describe an investigator-initiated clinical trial protocol to evaluate the efficacy and safety of zaltoprofen for patients with D-TGCT or unresectable localized TGCT (L-TGCT).

To the best of our knowledge, this is the first evaluation of the efficacy of zaltoprofen for patients with diffuse-type and unresectable localized TGCT by a randomized placebo-controlled double-blind phase II investigator-initiated study.

TGCT progresses slowly [21]. However, it causes local destruction with invasion of the adjacent joint cartilage [22], and more severe symptoms such as joint pain, limited range of motion, swelling, erythema, and hemorrhagic effusion [23]. Excision by arthroscopic or open synovectomy is recommended, but complete removal is sometimes difficult to achieve due to the wide spread of the growth, resulting in high local recurrence [4, 5]. In addition, total joint replacement is necessary in the case of severe joint destruction due to tumor progression [24].

Based on our pilot study [20], we hypothesized that zaltoprofen treatment would produce a higher progression-free rate than that of placebo at 48 weeks. Moreover, we considered that the benefit of zaltoprofen is to avoid serious events, such as repetitive hemorrhage effusion, limitation of range of motion, adjacent joint cartilage destruction, and tumor enlargement, which require surgical interventions. Therefore, we defined the criteria of exacerbation in each serious event: 1) An increase in joint circumference by 2 cm or more with respect to the baseline measurement by hematoma is used to reflect repetitive hemorrhage in the joint, which risks joint cartilage destruction by inflammation [25]. 2) A reduced range of motion of the joint (i.e., active motion) by 20% or more with respect to the baseline value is used because the limited range of motion represents joint destruction and 20% reduction is the worst Ogilvie-Harris score [26]. 3) An invasion of 5 mm or more of bone / cartilage erosion or new lesions of bone /cartilage erosion of 5 mm or more compared with that of baseline by CT or MRI is used because bone invasion is responsible for joint destruction and MRI can detect 5 mm of invaded tumor [27]. 4) The disappearance of joint space detected by X-ray photography in the standing position is used because severe joint space narrowing is the worst grade of the Kellgren and Lawrence (KL) grading system [28]. and 5) An increase in the target lesion size by 20% or more by RECIST is used because a ≥ 20% increase in the sum of the diameters of the target lesions is defined as progressive disease (PD) by the RECIST criteria [29].

We believe that the results of this trial can conclusively identify zaltoprofen as a novel treatment strategy to stabilize disease progression for patients with D-TGCT or unresectable L-TGCT. The recruiting of eligible patients has been ongoing since April, 2017.