Functional characterization of 84 PALB2 variants of uncertain significance

Wiltshire, Timothy D.; Ducy, Mandy; Foo, Tzeh Keong; Hu, Chunling; Lee, Kun Y.; Nagaraj, Anil Belur; Rodrigue, Amélie; Gomes, Thiago T.; Simard, Jacques; Monteiro, Alvaro N.A.; Xia, Bing; Carvalho, Marcelo A.; Masson, Jean‐Yves; Couch, Fergus J.

doi:10.1038/s41436-019-0682-z

Cited by 37 publications

(67 citation statements)

References 29 publications

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“…In the PALB2 N-terminus, p.L35P (c.104T>C) disrupts BRCA1-PALB2 interaction and abolishes the HR activity of PALB2, resulting in sensitivity to the PARPi (106). Moreover, p.P8L (c.23C>T), p.K18R (c.53A>G), p.L24S (c.71T>C), p.Y28C (c.83A>G), and p.R37H (c.110G>A) compromise HR activity of PALB2 and are suggested to be pathogenic (106)(107)(108). In the PALB2 C-terminus, p.W912G, p.G937R, p.L939W, p.I944N (c.2831T>A), p.L947F (c.2841G>T), p.L947S (c.2840T>C), p.L961P, p.L972Q, p.A1025R, p.T1030I (c.3089C>T), p.I1037T, p.G1043D, p.L1070P (c.3209T>C), p.P1088S (c.3262C>T), p.W1140G (c.3418T>C), p.L1143P, and p.L1172P promoted a decrease in the HR activity of PALB2 (20,(107)(108)(109)112).…”

Section: The Challenges Of Palb2 Research In Clinical Applicationmentioning

confidence: 99%

“…Moreover, p.P8L (c.23C>T), p.K18R (c.53A>G), p.L24S (c.71T>C), p.Y28C (c.83A>G), and p.R37H (c.110G>A) compromise HR activity of PALB2 and are suggested to be pathogenic (106)(107)(108). In the PALB2 C-terminus, p.W912G, p.G937R, p.L939W, p.I944N (c.2831T>A), p.L947F (c.2841G>T), p.L947S (c.2840T>C), p.L961P, p.L972Q, p.A1025R, p.T1030I (c.3089C>T), p.I1037T, p.G1043D, p.L1070P (c.3209T>C), p.P1088S (c.3262C>T), p.W1140G (c.3418T>C), p.L1143P, and p.L1172P promoted a decrease in the HR activity of PALB2 (20,(107)(108)(109)112). Among these mutations, p.L939W, p.A1025R, p.T1030I, p.P1088S, and p.L1143P disrupt BRCA2-PALB2 interaction; p.W912G, p.G937R, p.I944N, p.L961P, p.L972Q, p.T1030I, p.I1037T, p.G1043D, and p.L1172P are associated with PALB2 protein instability; and p.I944N, p.L947F, p.L947S, p.T1030I, p.L1070P, and p.W1140G result in the mislocalization of PALB2 to the cytoplasm.…”

Section: The Challenges Of Palb2 Research In Clinical Applicationmentioning

confidence: 99%

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Molecular Mechanisms of PALB2 Function and Its Role in Breast Cancer Management

Zhou

Zhang

et al. 2020

Front. Oncol.

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Partner and localizer of BRCA2 (PALB2) is vital for homologous recombination (HR) repair in response to DNA double-strand breaks (DSBs). PALB2 functions as a tumor suppressor and participates in the maintenance of genome integrity. In this review, we summarize the current knowledge of the biological roles of the multifaceted PALB2 protein and of its regulation. Moreover, we describe the link between PALB2 pathogenic variants (PVs) and breast cancer predisposition, aggressive clinicopathological features, and adverse clinical prognosis. We also refer to both the opportunities and challenges that the identification of PALB2 PVs provides in breast cancer genetic counseling and precision medicine.

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Section: The Challenges Of Palb2 Research In Clinical Applicationmentioning

confidence: 99%

Section: The Challenges Of Palb2 Research In Clinical Applicationmentioning

confidence: 99%

Molecular Mechanisms of PALB2 Function and Its Role in Breast Cancer Management

Zhou

Zhang

et al. 2020

Front. Oncol.

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“…Assays using HR as a read-out have emerged as the standard for the functional characterisation of VUS in BRCA1 and BRCA2 (Bouwman et al, 2013;Woods et al, 2016;Shimelis et al, 2017;Starita et al, 2018;Mesman et al, 2019). More recently, VUS in PALB2 have also been characterized in a similar manner (Figures 1, 2) (Park et al, 2014;Foo et al, 2017;Boonen et al, 2019;Rodrigue et al, 2019;Wiltshire et al, 2019). To identify variants that impact HR, the well described DR-GFP reporter, as well as the more recently introduced CRISPR-LMNA HR assay were used (Kass et al, 2013;Ducy et al, 2019).…”

Section: A Comprehensive Functional Analysis Of Vus In Palb2mentioning

confidence: 99%

“…PALB2-interacting proteins are depicted underneath their respective PALB2 interacting domain/regions. All PALB2 genetic variants from five functional studies (Park et al, 2014;Foo et al, 2017;Boonen et al, 2019;Rodrigue et al, 2019;Wiltshire et al, 2019) are shown and categorized per (functional) domain as benign (green framed sections), truncating (red framed sections), or VUS and synthetic missense variants (MVs) (blue framed sections) based on ClinVar. All functionally damaging PALB2 VUS with an HR efficiency < 50% compared to wild type PALB2 in at least one functional assay are highlighted in red.…”

Section: A Comprehensive Functional Analysis Of Vus In Palb2mentioning

confidence: 99%

“…This phenotype was used as a readout for the functional characterization of several PALB2 variants, revealing that two variants, p.L939W and p.L1143P, impaired PALB2 function (Park et al, 2014). Lastly, since PALB2 interacts with BRCA1 and BRCA2 to load RAD51 at sites of DSBs, co-immunoprecipitation, recruitment to laser micro-irradiation induced DNA damage, and DNA-damage-induced RAD51 foci formation were among the additional functional readouts to study the impact of PALB2 variants on HR ( Figure 2) (Park et al, 2014;Foo et al, 2017;Boonen et al, 2019;Rodrigue et al, 2019;Wiltshire et al, 2019). A complete overview of all functional assays that were performed by three recent studies is provided in Table 1 (Boonen et al, 2019;Rodrigue et al, 2019;Wiltshire et al, 2019).…”

Section: A Comprehensive Functional Analysis Of Vus In Palb2mentioning

confidence: 99%

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Functional Characterization of PALB2 Variants of Uncertain Significance: Toward Cancer Risk and Therapy Response Prediction

Boonen

Vreeswijk

Attikum

2020

Front. Mol. Biosci.

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In recent years it has become clear that pathogenic variants in PALB2 are associated with a high risk for breast, ovarian and pancreatic cancer. However, the clinical relevance of variants of uncertain significance (VUS) in PALB2, which are increasingly identified through clinical genetic testing, is unclear. Here we review recent advances in the functional characterization of VUS in PALB2. A combination of assays has been used to assess the impact of PALB2 VUS on its function in DNA repair by homologous recombination, cell cycle regulation and the control of cellular levels of reactive oxygen species (ROS). We discuss the outcome of this comprehensive analysis of PALB2 VUS, which showed that VUS in PALB2's Coiled-Coil (CC) domain can impair the interaction with BRCA1, whereas VUS in its WD40 domain affect PALB2 protein stability. Accordingly, the CC and WD40 domains of PALB2 represent hotspots for variants that impair PALB2 protein function. We also provide a future perspective on the high-throughput analysis of VUS in PALB2, as well as the functional characterization of variants that affect PALB2 RNA splicing. Finally, we discuss how results from these functional assays can be valuable for predicting cancer risk and responsiveness to cancer therapy, such as treatment with PARP inhibitor-or platinumbased chemotherapy.

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The p.Ser64Leu and p.Pro104Leu missense variants of PALB2 identified in familial pancreatic cancer patients compromise the DNA damage response

et al. 2020

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PALB2 has been identified as a breast and pancreatic cancer susceptibility gene. Utilizing a targeted sequencing approach, we discovered two novel germline missense PALB2 variants c.191C>T and c.311C>T, encoding p.Ser64Leu and p.Pro104Leu, respectively, in individuals in a pancreatic cancer registry. No missense PALB2 variants from familial pancreatic cancer patients, and few PALB2 variants overall, have been functionally characterized. Given the known role of PALB2, we tested the impact of p.Ser64Leu and p.Pro104Leu variants on DNA damage responses. Neither p.Ser64Leu nor p.Pro104Leu have clear effects on interactions with BRCA1 and KEAP1, which are mediated by adjacent motifs in PALB2. However, both variants are associated with defective recruitment of PALB2, and the RAD51 recombinase downstream, to DNA damage foci. Furthermore, p.Ser64Leu and p.Pro104Leu both largely compromise DNA double‐strand break‐initiated homologous recombination, and confer increased cellular sensitivity to ionizing radiation (IR) and the poly (ADP‐ribose) polymerase (PARP) inhibitor Olaparib. Taken together, our results represent the first demonstration of functionally deleterious PALB2 missense variants associated with familial pancreatic cancer and of deleterious variants in the N‐terminus outside of the coiled‐coil domain. Furthermore, our results suggest the possibility of personalized treatments, using IR or PARP inhibitor, of pancreatic and other cancers that carry a deleterious PALB2 variant.

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Functional characterization of 84 PALB2 variants of uncertain significance

Cited by 37 publications

References 29 publications

Molecular Mechanisms of PALB2 Function and Its Role in Breast Cancer Management

Molecular Mechanisms of PALB2 Function and Its Role in Breast Cancer Management

Functional Characterization of PALB2 Variants of Uncertain Significance: Toward Cancer Risk and Therapy Response Prediction

The p.Ser64Leu and p.Pro104Leu missense variants of PALB2 identified in familial pancreatic cancer patients compromise the DNA damage response

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