Diagnosis and management of tropomyosin receptor kinase (TRK) fusion sarcomas: expert recommendations from the World Sarcoma Network

Demetri, George D.; Antonescu, Cristina R.; Bjerkehagen, Bodil; Bovée, Judith V.M.G.; Boye, Kjetil; Chacón, Matías; Tos, Angelo Paolo Dei; Desai, Jayesh; Fletcher, Jonathan A.; Gelderblom, Hans; George, Suzanne; Gronchi, Alessandro; Haas, Rick L.; Hindi, Nadia; Hohenberger, Peter; Joensuu, Heikki; Jones, Robin L.; Judson, Ian; Kang, Yoon Koo; Kawai, Akira; Lazar, Alexander J.; Cesne, Axel Le; Maestro, Roberta; Maki, Robert G.; Martín, Juan Díaz; Patel, Shreyaskumar; Penault‐Llorca, Frédérique; Raut, Chandrajit P.; Rutkowski, Piotr; Safwat, Akmal; Sbaraglia, Marta; Schaefer, Inga‐Marie; Shen, Lin; Serrano, César; Schöffski, Patrick; Stacchiotti, Silvia; Hall, Kirsten Sundby; Tap, William D.; Thomas, David M.; Trent, Jonathan C.; Valverde, Claudia; Graaf, Winette T.A. van der; Mehren, Margaret von; Wagner, Andrew J.; Wardelmann, E.; Naito, Yoichi; Zalcberg, John; Blay, Jean‐Yves

doi:10.1016/j.annonc.2020.08.2232

Cited by 107 publications

(101 citation statements)

References 77 publications

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“…This requires a coordinated effort, worldwide, to achieve this goal given the rarity of certain histotypes. This is currently being conducted by intergroup studies, and international networks such as WSN or more recently EURACAN [26][27][28]. This work also confirms the importance of national registries to investigate these rare subtypes.…”

Section: Plos Onesupporting

confidence: 60%

“…Overall, this calls for a revision of the criteria to define standard treatment for such rare tumors where phase III are hardly or not feasible [26][27][28][29]. Health authorities and reimbursement bodies should adapt their decisions on approval and reimbursement on the feasible level of evidence which could be reached for tumors with and incidence <1/10 6 per year in order not to discriminate against patients with rare cancers.…”

Section: Plos Onementioning

confidence: 99%

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Nationwide incidence of sarcomas and connective tissue tumors of intermediate malignancy over four years using an expert pathology review network

Pinieux¹,

Karanian²,

Loarer³

et al. 2021

PLoS ONE

144

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Background Since 2010, nationwide networks of reference centers for sarcomas (RREPS/NETSARC/RESOS) collected and prospectively reviewed all cases of sarcomas and connective tumors of intermediate malignancy (TIM) in France. Methods The nationwide incidence of sarcoma or TIM (2013–2016) was measured using the 2013 WHO classification and confirmed by a second independent review by expert pathologists. Simple clinical characteristics, yearly variations and correlation of incidence with published clinical trials are presented and analyzed. Results Over 150 different histological subtypes are reported from the 25172 patients with sarcomas (n = 18712, 74,3%) or TIM (n = 6460, 25.7%), with n = 5838, n = 6153, n = 6654, and n = 6527 yearly cases from 2013 to 2016. Over these 4 years, the yearly incidence of sarcomas and TIM was therefore 70.7 and 24.4 respectively, with a combined incidence of 95.1/106/year, higher than previously reported. GIST, liposarcoma, leiomyosarcomas, undifferentiated sarcomas represented 13%, 13%, 11% and 11% of tumors. Only GIST, as a single entity had a yearly incidence above 10/106/year. There were respectively 30, 64 and 66 different histological subtypes of sarcomas or TIM with an incidence ranging from 10 to 1/106, 1–0.1/106, or < 0.1/106/year respectively. The 2 latter incidence groups represented 21% of the patients with 130 histotypes. Published phase III and phase II clinical trials (p<10−6) are significantly higher with sarcomas subtypes with an incidence above 1/106 per. Conclusions This nationwide registry of sarcoma patients, with exhaustive histology review by sarcoma experts, shows that the incidence of sarcoma and TIM is higher than reported, and that tumors with a very low incidence (1<106/year) are less likely to be included in clinical trials.

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Section: Plos Onesupporting

confidence: 60%

Section: Plos Onementioning

confidence: 99%

Nationwide incidence of sarcomas and connective tissue tumors of intermediate malignancy over four years using an expert pathology review network

Pinieux¹,

Karanian²,

Loarer³

et al. 2021

PLoS ONE

144

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“…Given the relatively low incidence of NTRK gene rearrangements across a range of tumour types, it remains extremely challenging to identify these rearrangements in routine clinical practice. A range of different techniques, including IHC, FISH, reverse transcription PCR, and massive parallel sequencing, have been used 7,34,35,36 . As no single approach is perfectly sensitive or specific, there is an emerging consensus that combinations of different techniques are most appropriate in different settings, depending on the pre‐test probability of gene rearrangement 7,13,34 .…”

Section: Discussionmentioning

confidence: 99%

“…For example, in sarcomas with a very high pre‐test probability of NTRK rearrangement (e.g. infantile fibrosarcoma), upfront testing with two methods may be appropriate 35 . For sarcomas with a low incidence of NTRK rearrangement, either screening IHC with follow‐up testing only in cases with positive staining, 13 or molecular testing only of sarcomas known to lack canonical oncogene alterations, may be more appropriate 35 …”

Section: Discussionmentioning

confidence: 99%

Chromosomal imbalances detected in NTRK‐rearranged sarcomas by the use of comparative genomic hybridisation

et al. 2021

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Aims NTRK‐rearranged sarcomas are emerging as a distinct class of sarcomas of particular importance in the era of targeted therapy. The aim of this study was to use array comparative genomic hybridisation (aCGH) to explore the cytogenetic profile of six adult soft tissue sarcomas harbouring NTRK gene fusions. Methods and results aCGH was performed on six adult soft tissue sarcomas with proven NTRK rearrangements [NTRK1, n = 1 (TPM3–NTRK1); NTRK2, n = 1 (MTMR2–NTRK2); NTRK3, n = 4 (two ETV6–NTRK3; two with unknown partners). The morphological patterns of these cases included inflammatory myofibroblastic tumour‐like, fibrosarcoma/malignant peripheral nerve sheath tumour‐like, and Ewing sarcoma‐like. On the basis of the number of chromosomal copy number variations (CNVs), ranging from two to 15 per sample, NTRK‐associated sarcomas could be subdivided into two groups: one with a relatively simple karyotype (n = 2; median of three genomic alterations), and those with a more complex karyotype (n = 4; median of 11 genomic imbalances). Recurrent chromosomal CNVs included gains at chromosomes 6p, 1q, 7 (whole chromosome), and 12p, and losses at chromosomes 10q, 13q, 19q, and 9p. Conclusions NTRK‐rearranged sarcomas constitute a heterogeneous group of tumours that can show a relatively simple or a complex karyotype. Although there were some, but inconsistent, associations between karyotype complexity and morphology, our study showed that a more complex karyotype in this group of tumours appeared to correlate with more aggressive clinical behaviour. Gains at chromosome 6p and 1q were the most common recurrent genomic alterations, being present in 67% of the samples (4/6), followed by gains at chromosome 7, which were present in 50% of the samples (3/6).

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“…The excellent clinical response and outcome in patients harboring NTRK -rearranged tumors treated with these agents have been demonstrated in several studies [ 114 , 115 , 116 ]. Even though pan-TRK IHC is wildly used as a reliable and affordable screening method for the detection of NTRK -fusions in most of the pathology departments [ 117 , 118 ], it has its limitations. The positive expression has been reported in a subset of neoplasms with neuronal and smooth muscle differentiation, as well as GIST, where diffuse, moderate to strong cytoplasmic pan-TRK expression has been described ( Figure 7 ) with lack of an NTRK1-3 -fusions by RNA sequencing [ 119 ].…”

Section: Molecular Classificationmentioning

confidence: 99%

Update on Molecular Genetics of Gastrointestinal Stromal Tumors

2021

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Gastrointestinal stromal tumors (GISTs) are the most common mesenchymal tumors of the gastrointestinal tract. The majority are sporadic, solitary tumors that harbor mutually exclusive KIT or PDGFRA gain-of-function mutations. The type of mutation in addition to risk stratification corresponds to the biological behavior of GIST and response to treatment. Up to 85% of pediatric GISTs and 10–15% of adult GISTs are devoid of these (KIT/PDGFRA) mutations and are referred to as wild-type GISTs (wt-GIST). It has been shown that these wt-GISTs are a heterogeneous tumor group with regard to their clinical behavior and molecular profile. Recent advances in molecular pathology helped to further sub-classify the so-called “wt-GISTs”. Based on their significant clinical and molecular heterogeneity, wt-GISTs are divided into a syndromic and a non-syndromic (sporadic) subgroup. Recently, the use of succinate dehydrogenase B (SDHB) by immunohistochemistry has been used to stratify GIST into an SDHB-retained and an SDHB-deficient group. In this review, we focus on GIST sub-classification based on clinicopathologic, and molecular findings and discuss the known and yet emerging prognostic and predictive genetic alterations. We also give insights into the limitations of targeted therapy and highlight the mechanisms of secondary resistance.

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Diagnosis and management of tropomyosin receptor kinase (TRK) fusion sarcomas: expert recommendations from the World Sarcoma Network

Cited by 107 publications

References 77 publications

Nationwide incidence of sarcomas and connective tissue tumors of intermediate malignancy over four years using an expert pathology review network

Nationwide incidence of sarcomas and connective tissue tumors of intermediate malignancy over four years using an expert pathology review network

Chromosomal imbalances detected in NTRK‐rearranged sarcomas by the use of comparative genomic hybridisation

Update on Molecular Genetics of Gastrointestinal Stromal Tumors

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