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Review
. 2018 Dec;3(12):874-883.
doi: 10.1016/S2468-1253(18)30237-1.

Resolving gastric cancer aetiology: an update in genetic predisposition

Affiliations
Review

Resolving gastric cancer aetiology: an update in genetic predisposition

Paul C Lott et al. Lancet Gastroenterol Hepatol. 2018 Dec.

Abstract

Every year gastric cancer accounts for nearly 1 million new cases and more than 720 000 deaths worldwide. Prognosis is dismal because most patients are diagnosed with advanced disease; as such, gastric cancer outcomes will benefit from better methods for identification of at-risk individuals that can be targeted for early detection. One approach to targeting high-risk populations is to identify individuals who are genetically predisposed to gastric cancer, as up to 15% of all patients report family history of the disease. On the basis of clinical manifestations, three gastric cancer syndromes have been described, but the diagnosis of some of these syndromes is suboptimal and could benefit from genetic information. Over the past decade, genome-wide association and next-generation sequencing studies have identified several low penetrance variants and high-risk genes, considerably increasing our understanding of inherited gastric cancer predisposition. From these studies, PALB2 has emerged as a new familial gastric cancer gene. Furthermore, genetic analyses in patients with sporadic gastric cancer suggest that more than 10% of all cases have pathogenic mutations, a finding of great importance for cancer aetiology. In this Review, we summarise the role of genetics in gastric cancer aetiology and the implications of genetics findings for the prevention of this malignancy.

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Conflict of interest statement

Conflicts of Interest

The authors declared no conflicts of interest.

Figures

Figure 1:
Figure 1:
Gastric cancer anatomical classification into cardia and non-cardia cancer and the role of environmental and lifestyle risk factors. Risk factors for both cardia and non-cardia are shown in the middle of figure. They are shown in italics if they have stronger effects for cardia tumours and in bold if they have stronger effects for non-cardia tumours

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