Unique clonal relationship between T‐cell acute lymphoblastic leukemia and subsequent Langerhans cell histiocytosis with <scp><i>TCR</i></scp> rearrangement and <scp><i>NOTCH1</i></scp> mutation

Yokokawa, Yuichi; Taki, Tomohiko; Chinen, Yoshiaki; Kobayashi, Satoru; Nagoshi, Hisao; Akiyama, Masaharu; Morimoto, Akira; Ida, Hiroyuki

doi:10.1002/gcc.22252

Cited by 20 publications

(8 citation statements)

References 31 publications

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“…For example, in Case 1, the MAP2K1 and RAF1 mutations were (presumably) only present in the HS and not in the CMML, suggesting that these mutations may have contributed to the development of the HS from a common KRAS mutated HSPC or primary CMML clone. Similar situations of one or more shared genetic alterations and additional unique mutations in the histiocytic neoplasm and/or associated haematological malignancy have been reported in other cases [15,18,23,25–27,29,31,32,39,41,44,45,47,52–57,59,60,63–67,87–95]. The histiocytic neoplasms often harboured unique mutations in genes encoding proteins of the MAPK signalling pathway, including NRAS [52,55], KRAS [39,53,56], BRAF [15,23,44,45,54,92,94] and RAF1 [32], again demonstrating the importance of constitutive MAPK pathway activation in the pathogenesis of the histiocytic neoplasms [3,96].…”

Section: Discussionmentioning

confidence: 67%

Spectrum of histiocytic neoplasms associated with diverse haematological malignancies bearing the same oncogenic mutation

Kemps

Hebeda

Pals

et al. 2020

The Journal of Pathology CR

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Histiocytic disorders are a spectrum of rare diseases characterised by the accumulation of macrophage‐, dendritic cell‐, or monocyte‐differentiated cells in various tissues and organs. The discovery of recurrent genetic alterations in many of these histiocytoses has led to their recognition as clonal neoplastic diseases. Moreover, the identification of the same somatic mutation in histiocytic lesions and peripheral blood and/or bone marrow cells from histiocytosis patients has provided evidence for systemic histiocytic neoplasms to originate from haematopoietic stem/progenitor cells (HSPCs). Here, we investigated associations between histiocytic disorders and additional haematological malignancies bearing the same genetic alteration(s) using the nationwide Dutch Pathology Registry. By searching on pathologist‐assigned diagnostic terms for the various histiocytic disorders, we identified 4602 patients with a putative histopathological diagnosis of a histiocytic disorder between 1971 and 2019. Histiocytosis‐affected tissue samples of 187 patients had been analysed for genetic alterations as part of routine molecular diagnostics, including from nine patients with an additional haematological malignancy. Among these patients, we discovered three cases with different histiocytic neoplasms and additional haematological malignancies bearing identical oncogenic mutations, including one patient with concomitant KRAS p.A59E mutated histiocytic sarcoma and chronic myelomonocytic leukaemia (CMML), one patient with synchronous NRAS p.G12V mutated indeterminate cell histiocytosis and CMML, and one patient with subsequent NRAS p.Q61R mutated Erdheim–Chester disease and acute myeloid leukaemia. These cases support the existence of a common haematopoietic cell‐of‐origin in at least a proportion of patients with a histiocytic neoplasm and additional haematological malignancy. In addition, they suggest that driver mutations in particular genes (e.g. N/KRAS) may specifically predispose to the development of an additional clonally related haematological malignancy or secondary histiocytic neoplasm. Finally, the putative existence of derailed multipotent HSPCs in these patients emphasises the importance of adequate (bone marrow) staging, molecular analysis and long‐term follow‐up of all histiocytosis patients.

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Section: Discussionmentioning

confidence: 67%

Spectrum of histiocytic neoplasms associated with diverse haematological malignancies bearing the same oncogenic mutation

Kemps

Hebeda

Pals

et al. 2020

The Journal of Pathology CR

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“…One T‐ALL case (TALL023) developed Langerhans cell histiocytosis (LCH) after achieving complete remission. In this case, the LCH cells are not only a derivative of the same ancestral clone but should be a branched clone from the one that already gave rise to T‐ALL, because the LCH cells have the same TCR rearrangements (Figure D,E) . WXS was performed at an average coverage of 107.8× (range: 66.2‐201.9) (Figure ).…”

Section: Resultsmentioning

confidence: 99%

NOTCH1 pathway activating mutations and clonal evolution in pediatric T‐cell acute lymphoblastic leukemia

et al. 2019

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Molecular mechanisms involved in the relapse of T‐cell acute lymphoblastic leukemia (T‐ALL) are not fully understood, although activating NOTCH1 signaling due to NOTCH1/FBXW7 alterations is a major oncogenic driver. To unravel the relevance of NOTCH1/FBXW7 mutations associated with relapse, we performed whole–exome sequencing in 30 pediatric T‐ALL cases, among which 11 diagnosis‐relapse paired cases were further investigated to track the clonal evolution of relapse using amplicon–based deep sequencing. NOTCH1/FBXW7 alterations were detected in 73.3% (diagnosis) and 72.7% (relapse) of cases. Single nucleotide variations in the heterodimerization domain were the most frequent (40.0%) at diagnosis, whereas proline, glutamic acid, serine, threonine–rich (PEST) domain alterations were the most frequent at relapse (54.5%). Comparison between non–relapsed and relapsed cases at diagnosis showed a predominance of PEST alterations in relapsed cases (P = .045), although we failed to validate this in the TARGET cohort. Based on the clonal analysis of diagnosis‐relapse samples, we identified NOTCH1 “switching” characterized by different NOTCH1 mutations in a major clone between diagnosis and relapse samples in 2 out of 11 diagnosis‐relapse paired cases analyzed. We found another NOTCH1 “switching” case in a previously reported Berlin‐Frankfurt‐Münster cohort (n = 13), indicating NOTCH1 importance in both the development and progression of T‐ALL. Despite the limitations of having a small sample size and a non–minimal residual disease–based protocol, our results suggest that the presence of NOTCH1 mutations might contribute to the disease relapse of T‐ALL.

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“…The authors identified two mutations in the NOTCH1 gene as well as a rearrangement in the T‐cell receptor in the T‐ALL and LCH cells. The identification of these mutations and rearrangements suggests a common clonal origin between acute leukemia and LCH 9 . An additional case of LCH following T‐ALL was also reported with an activating mutation in the NOTCH1 gene 7 …”

Section: Discussionmentioning

confidence: 97%

“…In the case of a 7-year-old male child from Japan, between acute leukemia and LCH. 9 An additional case of LCH following T-ALL was also reported with an activating mutation in the NOTCH1 gene. 7 The role of NOTCH1 in our patient and LCH has not been clearly identified but is being investigated.…”

Section: Discussionmentioning

confidence: 99%

Aggressive Langerhans cell histiocytosis following T‐cell acute lymphoblastic leukemia

Jansen

Dykstra

Callaway

et al. 2020

Pediatric Blood & Cancer

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A 4-year-old female child developed cutaneous Langerhans cell histiocytosis 6 months following a diagnosis of T-cell acute lymphoblastic leukemia. Imaging revealed no evidence of systemic disease. Seven months later, the first systemic lesion was discovered on laryngoscopy. Restaging Positron Emission Tomography-Computed Tomography at that time revealed new 18-fluorodeoxyglucose-positive lesions in the left apical pleural margin, right lower peri-esophageal region, left ventricular myocardium, pancreas, upper pole of the left kidney, and inguinal and gluteal regions consistent with progressive systemic disease. Genomic testing revealed a low tumor mutational burden as well as mutations in KRAS G12A, ARID1A Q524, CDKN2A/B loss, and an alteration in NOTCH1.

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Unique clonal relationship between T‐cell acute lymphoblastic leukemia and subsequent Langerhans cell histiocytosis with TCR rearrangement and NOTCH1 mutation

Cited by 20 publications

References 31 publications

Spectrum of histiocytic neoplasms associated with diverse haematological malignancies bearing the same oncogenic mutation

Spectrum of histiocytic neoplasms associated with diverse haematological malignancies bearing the same oncogenic mutation

NOTCH1 pathway activating mutations and clonal evolution in pediatric T‐cell acute lymphoblastic leukemia

Aggressive Langerhans cell histiocytosis following T‐cell acute lymphoblastic leukemia

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