Uncovering novel lncRNAs linked to melanoma growth and migration with CRISPR-inhibition screening.

Publication date: Jun 24, 2025

Melanoma being one of the most common and deadliest skin cancers, has been rising since the past decade. Patients at advanced stages of the disease have very poor prognoses, as opposed to at the earlier stages. Nowadays the standard-of-care of advanced melanoma is resection followed by immune checkpoint inhibition based immunotherapy. However, a substantial proportion of patients either do not respond or develop resistances. This underscores a need for novel approaches and therapeutic targets as well as a better understanding of the mechanisms of melanoma pathogenesis. Long non-coding RNAs (lncRNAs) comprise a poorly characterized class of functional players and promising targets in promoting malignancy. Certain lncRNAs have been identified to play integral roles in melanoma progression and drug resistances, however systematic screens to uncover novel functional lncRNAs are scarce. Here, we profile differentially expressed lncRNAs in patient derived short-term metastatic cultures and BRAF- MEK-inhibition resistant cells. We conduct a focused growth-related CRISPR-inhibition screen of overexpressed lncRNAs, validate and functionally characterize lncRNA hits with respect to cellular growth, invasive capacities and apoptosis in vitro as well as the transcriptomic impact of our lead candidate the novel lncRNA XLOC_030781. In sum, we extend the current knowledge of ncRNAs and their potential relevance on melanoma.

Concepts Keywords
Cancers Advanced
Deadliest Crispr
Earlier Functional
Patient Growth
Xloc_030781 Inhibition
Linked
Lncrna
Lncrnas
Melanoma
Migration
Resistances
Screening
Stages
Targets
Uncovering

Semantics

Type Source Name
disease MESH melanoma
pathway KEGG Melanoma
disease MESH skin cancers
drug DRUGBANK Tropicamide
disease MESH pathogenesis
disease MESH malignancy
pathway REACTOME Apoptosis

Original Article

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