Analysis of genomic and immune intratumor heterogeneity in linitis plastica via multiregional exome and T‐cell receptor sequencing

Huang, Jin; Zhao, Guofeng; Qiu, Ping; Yi, Xin; Ji, Liyan; Li, Jing; Li, Pansong; Guan, Yanfang; Ge, Jie; Chen, Ling; Chen, Runzhe; Hu, Xin; Lee, Won‐Chul; Reuben, Alexandre; Futreal, P. Andrew; Xia, Xuefeng; Ma, Jian; Zhang, Jianjun; Chen, Zihua

doi:10.1002/1878-0261.13381

Cited by 2 publications

(6 citation statements)

References 63 publications

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“…The etiology of LP is not solely rooted in mutations within cancerous cells, it also hinges on the interactions between stromal and cancerous cells. Huang et al assert that these mutations result from spontaneous deaminations or defects in DNA mismatch repair mechanisms, mostly occurring after failures in repairing DNA double-strand breaks [9]. LP stands out as one of the most heterogeneous cancers in terms of mutated genes, but in each distinct case, it exhibits the same mutations across all its regions, with a prevalence ranging from 68-95% [9].…”

Section: Discussionmentioning

confidence: 99%

“…Huang et al assert that these mutations result from spontaneous deaminations or defects in DNA mismatch repair mechanisms, mostly occurring after failures in repairing DNA double-strand breaks [9]. LP stands out as one of the most heterogeneous cancers in terms of mutated genes, but in each distinct case, it exhibits the same mutations across all its regions, with a prevalence ranging from 68-95% [9]. The invasive nature of LP is attributed to mutations in genes and proteins associated with tight junctions.…”

Section: Discussionmentioning

confidence: 99%

“…The PI3KT-AKT pathway is up-regulated in LP, while the AMPK pathway is down-regulated, both contributing to cell growth due to their "oncogene-like functioning" [3]. Huang et al, in their cohort, report that the most frequently traced mutations among LP patients were RELN, CDH1 and ARID1A, with occurrence rates of 76%, 65% and 40%, respectively [9]. On the other hand, Liu et al demonstrate that the most common mutations affect the TTN gene, followed by TP53, MUC16, CDH1, LRP1B, CYNE1 and ARID1A.…”

Section: Molecular Background (Oncogenes Drivers Pathways)mentioning

confidence: 99%

“…LP originates from the fundic gland cells and infiltrates the entire stomach with a desmoplastic growth pattern, unlike the development of a solid tumor. Tumor cells are dispersed within the thickened fibrous tissue, extending into the submucosal and serous layer [5,7,[9][10][11]. In 91.1% of cases, LP presents as a poorly differentiated adenocarcinoma, and in 77.7% of cases, it is often histologically linked with signet ring cells [8].…”

Section: Introductionmentioning

confidence: 99%

“…LP predominantly affects women and younger individuals, distinguishing it from other types of GC [8,11]. Its aggressive behavior, stemming from its unique features, places the 5-year overall survival (OS) at 5%, while non-LP GC patients have a median 5-year OS of 36%, respectively [8,9,12,13]. Only a small percentage of LP patients are diagnosed at an early stage and are consequently candidates for R0 resection.…”

Section: Introductionmentioning

confidence: 99%

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The Genomic Signatures of Linitis Plastica Signal the Entrance into a New Era: Novel Approaches for Diagnosis and Treatment

Christodoulidis,

Koumarelas,

Kouliou

et al. 2023

IJMS

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Linitis Plastica (LP) is a rare and aggressive tumor with a distinctive development pattern, leading to the infiltration of the gastric wall, the thickening of the gastric folds and a “leather bottle appearance”. LP is an extremely heterogeneous tumor caused by mutations in oncogenic and tumor suppressive genes, as well as molecular pathways, along with mutations in stromal cells and proteins related to tight junctions. Elucidating the molecular background of tumorigenesis and clarifying the correlation between cancerous cells and stromal cells are crucial steps toward discovering novel diagnostic methods, biomarkers and therapeutic targets/agents. Surgery plays a pivotal role in LP management, serving both as a palliative and curative procedure. In this comprehensive review, we aim to present all recent data on the molecular background of LP and the novel approaches to its management.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Molecular Background (Oncogenes Drivers Pathways)mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

The Genomic Signatures of Linitis Plastica Signal the Entrance into a New Era: Novel Approaches for Diagnosis and Treatment

Christodoulidis,

Koumarelas,

Kouliou

et al. 2023

IJMS

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The characteristics of T‐cell receptor repertoire in relation to systemic immune response of patients with ischemic stroke

Zong,

Liu,

Wang

et al. 2024

Journal of Neurochemistry

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T lymphocytes play a vital role in the immune‐inflammatory response following a stroke. However, the specific mechanisms behind the contrasting functions of T cells in the brain and peripheral tissues after a stroke remain unclear and require further investigation. T‐cell receptors (TCRs) are essential in controlling how T lymphocytes develop and become active. This study aims to gain a deeper understanding of the biological function of T lymphocytes by analyzing the TCR repertoire in patients who have experienced an acute ischemic stroke (AIS). High‐throughput TCR sequencing was conducted on peripheral blood samples from 25 AIS patients and 10 healthy controls. We compared the percentage of T cells and the characteristics of the TCR repertoire, specifically focusing on the recombination of V(D)J gene fragments and the diversity of the complementarity determining region 3 (CDR3) of the Vβ gene. Additionally, this study analyzed the potential biological significance of the skewed TCR repertoire in AIS patients. In patients with AIS, the proportion of circulating lymphocytes (LY%) decreased while the systemic immune‐inflammatory index (SII) increased compared to healthy controls. The average number of TCR read pairs decreased, corresponding with the presence of lymphopenia. However, the recombination of V(D)J gene fragments, the number of CDR3 clonotypes, and the diversity of CDR3 was elevated in the peripheral blood of AIS patients. Furthermore, the increased number of CDR3 amino acid or nucleotide clonotypes was negatively correlated with neurologic deficits but positively correlated with AIS patients' systemic immune condition and functional outcomes. Our findings suggest that both immunosuppression and enhanced antigen‐specific T‐cell response may exist in the periphery of the AIS patients. Further investigation into the mechanisms underlying these opposing changes may lead to the discovery of novel targets to reverse immunosuppression or mitigate the detrimental effects of T cells in the lesioned brain of AIS patients.image

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Analysis of genomic and immune intratumor heterogeneity in linitis plastica via multiregional exome and T‐cell receptor sequencing

Cited by 2 publications

References 63 publications

The Genomic Signatures of Linitis Plastica Signal the Entrance into a New Era: Novel Approaches for Diagnosis and Treatment

The Genomic Signatures of Linitis Plastica Signal the Entrance into a New Era: Novel Approaches for Diagnosis and Treatment

The characteristics of T‐cell receptor repertoire in relation to systemic immune response of patients with ischemic stroke

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