Homologous recombination deficiency gene panel analysis results in synchronous endometrial and ovarian cancers

Kazanci, Ferah; Çelik, Zerrin Yılmaz; Polat, Mert; Karademir, Ferhat; Erdem, Ozlem; Şahin, Feride İffet; Onan, Mehmet Anil

doi:10.1590/1806-9282.20240534

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ORIGINAL ARTICLE • Rev. Assoc. Med. Bras. 70 (10) • 2024 • https://doi.org/10.1590/1806-9282.20240534 copy

Homologous recombination deficiency gene panel analysis results in synchronous endometrial and ovarian cancers

Authorship SCIMAGO INSTITUTIONS RANKINGS

SUMMARY

OBJECTIVE:

The objective of this study was to analyze the genetic alterations of tumors within the scope of the homologous recombination deficiency gene panel in patients diagnosed with synchronous endometrial ovarian cancer who have been followed for over 5 years using next-generation sequencing.

METHODS:

DNA was isolated from the patient’s formalin-fixed, paraffin-embedded tissue blocks. Next-generation sequencing was performed using the Illumina capture-based sequencing method. Samples were sequenced using the Sophia HR Solution DNA Kit.

RESULTS:

Seven patients were included in this study. The ratios of likely pathogenic (LP)/pathogenic (P) somatic mutations in ATM (serine/threonine kinase or Ataxia-telangiectasia mutated gene), BRCA2 (breast cancer type 2 susceptibility gene), BARD1 (BRCA1 associated RING domain 1), TP53 (tumor protein p53), BIRP1 (BRCA1-interacting helicase 1 gene), PALB2 (partner and localizer of BRCA2), and CHECK2 were 21 (48.8%), 8 (18.6%), 5 (11.6%), 3 (6.9%), 2 (4.6%), 2 (4.6%), and 2 (4.6%), respectively, in endometrium, and the ratios of somatic mutations in ATM, BRCA2, TP53, BARD1, RAD54L (DNA repair/recombination protein like), BIRP1, and RAD51D (RAD51 recombinase paralog D) were 24 (60%), 6 (15%), 5 (12.5%), 2 (5%), 2 (5%), 1 (2.5%), and 1 (2.5%), respectively, in ovary. In endometrioid-synchronous endometrial ovarian cancer cases, P/LP mutations were observed in ATM and CHECK2 genes in endometrium and ATM, BRCA2, and TP53 genes in ovary. In two non-endometrioid-synchronous endometrial ovarian cancer cases, CHEK2 (checkpoint kinase 2) mutations were observed in endometrium and ATM and TP53 mutations in ovary, whereas in one case, P/LP mutations in ATM and TP53 genes were common in both tissues.

CONCLUSION:

Pathogenic variations confirming the diagnosis of synchronous endometrial ovarian cancer with genetic alterations were identified in all but one case. ATM gene mutation emerged as the most common alteration and has a potential association with a favorable prognosis.

KEYWORDS:
Synchronous neoplasm; Homologous recombination; Deficiency; ATM; Genes

	n (%)	Grade (n, %)	Evre (n, %)
Age (med/min–max)	49 (38–64)
Nullipar/mıltipar	3 (42.9)/4 (57.2)
BMI (med/min–max)	30 (27–32)
Symptoms at the time of presentation
Abnormal uterine bleeding	2 (28.6)
Pelvic pain/abdominal distention	3 (42.9)/2 (28.6)
History of other disease (-)	4 (57.1)
DM/HT/DM+HT	2 (14.3)/1 (14.3)
Ca-125 levels (med/min–max)	16 (11–776)
Preop.Biopsy (+)/(-)	2/5 (28.6/71.4)
TAH+BSO+PPLND+Omentektomi	0/7 (100)
Malign cytology (+)/(-)	1/6 (14.3/85.7)
Histology of endometrium
Endometriod	6 (85.7)	G1-2 (28.6)	Ia-6 (85.7)
Nonendometriod	1 (14.3)	G2-4 (57.1)	IIIc1-1 (14.3)
Serous	1 (14.3)	G3-1 (14.3)
Malign invasion (Invasion depth/<1/2)	2 (28.6)/5 (71.4)
Cervical invasion (+)/(-)	1/6 (14.3/85.7)
Endometrial LVSI (+)/(-)	1/6 (14.3/85.7)
Ovarian cytology
Endometrioid	4 (57.1)	G1-1 (14.3)	Ia-4 (57.1)
Nonendometrioid	3 (42.9)	G2-3 (42.9)	Ib-1 (14.3)
Serous	3 (42.9)	G3-3 (42.9)	IIIc-2 (28.6)
Ovarian LVSI (+)/(-)	2/5 (28.6/71.4)
Endometriosis (+)/(-)	4/3 (57.1/42.9)
RT+CT/CT	4 (57.1)/3 (42.9)
OS (med/min–max)	101 (61–128)/
RFS (med/min–max)	101 (13–128)
Total (patient, n)	7

	AN	AE	GK	SG	MA	DU	SÇ
	EN-SEOC				NE-SEOC
Age	47	49	49	38	64	57	64
Ca-125 (IU/mL)	16	12	11	90	776	14	361
Endometrium histology	End.	End.	End.	End.	End	Ser.	End.
Endometrium grade	2	2	2	2	1	3	1
Myometrial invasion	<1/2	<1/2	Superficial	<1/2	<1/2	<1/2	Superficial
Cervical stromal invasion	(-)	(-)	(-)	(-)	(-)	(+)	(-)
Endometrial hyperplasia/polyp	(-)/(-)	(-)/(-)	(-)/(+)	(-)/(-)	(-)/(-)	(-)/(-)	(-)/(+)
LVSI	(-)	(-)	(-)	(-)	(-)	(+)	(-)
Tumor diameter (cm)	4	7	2.5	6	0.4	4	1
Endometrial mutation	-	-	ATM ¹ 1Different mutations in the same gene in both endometrium and ovary;	CHEK2	CHEK2	ATM ² 2identical mutations in the same gene in both endometrium and ovary. EN-SEOC: endometrioid synchronous endometrial ovarian cancer; NE-SEOC: nonendometrioid synchronous endometrial ovarian cancer; End: endometrioid; Ser: serous; RT: radiotherapy; KT: chemotherapy; OS: overall survival; RFS: recurrence-free survival; LVSI: lymphovascular space invasion. TP53 ² 2identical mutations in the same gene in both endometrium and ovary. EN-SEOC: endometrioid synchronous endometrial ovarian cancer; NE-SEOC: nonendometrioid synchronous endometrial ovarian cancer; End: endometrioid; Ser: serous; RT: radiotherapy; KT: chemotherapy; OS: overall survival; RFS: recurrence-free survival; LVSI: lymphovascular space invasion. BRCA2	-
Ovarian histology	End.	End.	End.	End.	Ser.	Ser.	Ser.
Ovarian grade	2	1	2	2	3	3	3
Ovarian endometriosis	(+)	(+)	(+)	(+)	(-)	(-)	(-)
LVSI	(-)	(-)	(-)	(-)	(+)	(+)	(-)
Tumor diameter (cm)	4	30	5	8	9	4	3
Ovarian mutation	ATM	ATM BRCA2 TP53	ATM ¹ 1Different mutations in the same gene in both endometrium and ovary;	ATM	ATM TP53	ATM ² 2identical mutations in the same gene in both endometrium and ovary. EN-SEOC: endometrioid synchronous endometrial ovarian cancer; NE-SEOC: nonendometrioid synchronous endometrial ovarian cancer; End: endometrioid; Ser: serous; RT: radiotherapy; KT: chemotherapy; OS: overall survival; RFS: recurrence-free survival; LVSI: lymphovascular space invasion. TP53 ² 2identical mutations in the same gene in both endometrium and ovary. EN-SEOC: endometrioid synchronous endometrial ovarian cancer; NE-SEOC: nonendometrioid synchronous endometrial ovarian cancer; End: endometrioid; Ser: serous; RT: radiotherapy; KT: chemotherapy; OS: overall survival; RFS: recurrence-free survival; LVSI: lymphovascular space invasion.	TP53
Adjuvant therapy	RT+KT	RT+KT	KT	RT+KT	RT+KT	KT	KT
Recurrence	-	-	-	-	Liver	-	-
Mortality	-	-	-	-	-	-	-
OS	65	128	114	121	65	101	70
RFS	65	128	114	121	13	101	70

	Gene	cDNA	Protein	Reference sequence	Variant detection rate	ACMG criteria	E	O
AE	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	5.8	PVS1, PM2	(-)	(+)
	BRCA2	c.2141_2143delinsCAT	p.(Glu714_Gly715delinsAla*)	NM_000059	7.2	PVS1, PM2	(-)	(+)
	TP53	c.707A>G	p.(Tyr236Cys)	NM_000546	10.8	PM2,PM1,PP3,PM5 PP2, PP5	(-)	(+)
GK	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	7	PVS1, PM2	(+)	(-)
GK	ATM	c.1236-2A>T	p.(?)	NM_000051		PVS1, PP5, PM2	(-)	(+)
AN	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	5.3	PVS1, PM2	(-)	(+)
AN	ATM	c.832del	p.(Val278Serfs*42)	NM_000051	5	PVS1, PM2	(-)	(+)
SG	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	6.2	PVS1, PM2	(-)	(+)
	ATM	c.832del	p.(Val278Serfs*42)	NM_000051	5.6	PVS1, PM2	(-)	(+)
	CHEK2	c.1549C>T	p.(Arg517Cys)	NM_001005735	6.5	PM2,PM5,PM1, PP3	(+)	(-)
SÇ	TP53	c.859G>T	p.(Glu287*)	NM_000546	10.1	PVS1, PM2	(-)	(+)
SÇ	TP53	c.532del	p.(His178Thrfs*69)	NM_000546	7.6	PVS1, PM2, PP5	(-)	(+)
MA	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	5.2	PVS1, PM2	(-)	(+)
	CHEK2	c.721+1G>A	p.(?)	NM_001005735	5.4	PVS1, PM2, PP5	(+)	(-)
	TP53	c.641A>G	p.(His214Arg)	NM_000546	59.8	PS3,PM2,PM1, PP3, PM5, PP2, PP5, PS4	(-)	(+)
DU	ATM	c.818_819insC	p.(Ser274Phefs*8)	NM_000051	6.4/8.3	PVS1, PM2	(+)	(+)
	ATM	c.832del	p.(Val278Serfs*42)	NM_000051	5.2/7	PVS1, PM2	(+)	(+)
		c.2141_2143delinsCAT	p.(Glu714_Gly715delinsAla*)	NM_000059	5.3	PVS1, PM2	(+)	(-)
		c.859G>T	p.(Glu287*)	NM_000546	69.6/22.4	PVS1, PM2	(+)	(+)

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[1] *Corresponding author: ferahkazanci@hotmail.com