Archives of Gynecology and Obstetrics (2019) 300:15–23

https://doi.org/10.1007/s00404-019-05167-z

REVIEW

Treatments and overall survival in patients with Krukenberg tumor

Ruggero Lionetti1 · Marcello De Luca1 · Antonio Travaglino2   · Antonio Raffone3 · Luigi Insabato2 ·
Gabriele Saccone3 · Massimo Mascolo2 · Maria D’armiento4 · Fulvio Zullo3 · Francesco Corcione1

Received: 22 February 2019 / Accepted: 16 April 2019 / Published online: 1 May 2019
© Springer-Verlag GmbH Germany, part of Springer Nature 2019

Abstract
Background  Krukenberg tumor (KT) is a rare secondary ovarian tumor, primarily localized at the gastrointestinal tract in
most cases. KT is related to severe prognosis due to its aggressiveness, diagnostic difficulties and poor treatment efficacy.
Several treatments have been used, such as cytoreductive surgery (CRS), adjuvant chemotherapy (CT) and/or hyperthermic
intraperitoneal chemotherapy (HIPEC). To date, it is still unclear which treatment or combination of treatments is related
to better survival.
Objective  To assess the most effective therapeutic protocol in terms of overall survival (OS).
Methods  A systematic review of the literature was performed by searching MEDLINE, Scopus, EMBASE, ClinicalTrial.
gov, OVID, Web of Sciences, Cochrane Library, and Google Scholar for all studies assessing the association of treatments
with OS in KTs. The effectiveness of each treatment protocol was evaluated by comparing the OS between patients treated
with different treatment protocols.
Results  Twenty retrospective studies, with a total sample size of 1533 KTs, were included in the systematic review. Thera-
peutic protocols used were CRS in 18 studies, CT in 13 studies, HIPEC in 7 studies, neoadjuvant CT in 2 studies, and some
combinations of these in 6 studies. Seven studies showed that CRS significantly improved OS compared to other treatments
or association of treatments without it. 11 studies showed that CRS without residual (R0 CRS) had a significantly better OS
than CRS with residual (R + CRS). Five studies showed that CT significantly improved OS, but other five showed it did not.
Two studies showed that HIPEC in association with CRS improved OS, while another study showed that efficacy of HIPEC
was comparable to CT. Two studies evaluated neoadjuvant CT, but results were conflicting.
Conclusion  CRS and in particular R0 CRS are the treatments showing the clearest results in improving OS in KT patients.
Results about CT are conflicting. HIPEC appears effective both alone and in combination with CRS, and also related to fewer
adverse effect than CT. The usefulness of neoadjuvant CT is still unclear. The association of R0 CRS with HIPEC seems to
be the most effective and safe therapeutic protocol for KT patients.

Keywords  Cancer · Metastasis · Prognosis · Management · oncology · hazard ratio · Therapy

Introduction
* Antonio Travaglino
[email protected]
Krukenberg tumor (KT) is a rare secondary ovarian tumor
1
General Surgery Unit, Department of Public Health, School that represents 1–2% of all ovarian tumors.
of Medicine, University of Naples Federico II, Naples, Italy The most frequent primary localization is the gastrointes-
2
Anatomic Pathology Unit, Department of Advanced tinal tract, while breast and appendix are involved in a minor
Biomedical Sciences, School of Medicine, University percentage of cases [1, 2].
of Naples Federico II, Via Sergio Pansini, 5, 80131 Naples,
Italy
Not all secondary tumors of the ovary are KT: signet ring
3
cells that produce mucin and the sarcomatoid proliferation
Gynecology and Obstetrics Unit, Department
of Neurosciences, Reproductive Sciences and Dentistry,
of the stroma are the distinguishing features [3].
School of Medicine, University of Naples Federico II, KT has a poor prognosis due to its aggressiveness,
Naples, Italy advanced stage, diagnostic difficulties and poor treatment
4
Pathology Unit, Department of Public Health, School efficacy [2, 4].
of Medicine, University of Naples Federico II, Naples, Italy

13
Vol.:(0123456789)

16
Available treatments consist of cytoreductive surgery
(CRS), adjuvant chemotherapy (CT) and/or hyperthermic
intraperitoneal chemotherapy (HIPEC), but there is no clar-
ity about which treatment or combination of treatments is
related to better survival [5–7].
The aim of this study was to assess which treatment or
combination of treatments may be the most effective in
terms of increased overall survival (OS) in patients with KT.
Materials and methods
Methods for electronic search, study selection, risk of bias
assessment and data extraction were defined before the
beginning of the study.
All stages of the review were conducted independently
by three reviewers (RL, MDL, AR). Disagreements were
resolved by consensus among the three reviewers, or among
all authors if necessary.
The study was reported according to the Preferred
Reporting Item for Systematic Reviews and Meta-analyses
(PRISMA) statement [8].
Search strategy
MEDLINE, Scopus, EMBASE, ClinicalTrial.gov, OVID,
Web of Sciences, Cochrane Library, and Google Scholar
were used as electronic databases to be searched. Relevant
articles were searched from the inception of each database
to August 2018. Several searches were performed using
combinations of the following text words: “krukenberg”;
“ovarian”; “ovary”; “ovaries”; “metastasis”; “metastases”;
“metastatic”; “tumor”; “cancer”; “neoplasm”; “survival”.
Reference from relevant studies were also assessed.
Study selection
All retrospective or prospective studies assessing the asso-
ciation of treatments with OS in KTs were included.
Exclusion criteria, defined a priori, were sample size < 10;
case reports; reviews. No language restrictions were applied.
Risk of bias within studies assessment
According to the Methodological Index for Non-Rand-
omized Studies (MINORS) [9], we evaluated the risk of
bias for each study, in relation to seven domains: (1) Aim
(i.e. clearly stated aim); (2) Patients (i.e. all patients satis-
fying the criteria for inclusion were included in the study
during the study period); (3) Data (i.e. data were collected
according to a protocol established before the beginning of
the study); (4) Endpoint (i.e. unambiguous explanation of
the criteria used to measure outcomes); (5) Bias (i.e. the
13
Archives of Gynecology and Obstetrics (2019) 300:15–23
study endpoint was assessed without bias); (6) Follow-up
(i.e. the follow-up was sufficiently long to allow the assess-
ment of the main endpoint), (7) Loss (i.e. no more than 5%
of patients were lost to follow-up).
The risk of bias was categorized as “low” (criterion met),
“high” (criterion not met) or “unclear” (data not reported).
Data extraction and analysis
Data from original studies were not modified
during extraction
Primary extracted data were therapeutic protocols used to
treat KTs with the related OS. Secondary extracted data were
country, period of recruitment, sample size, patients’ age,
primary site of the tumor, treatment side effects.
The effectiveness of each treatment protocol was evalu-
ated by comparing the OS between patients treated with dif-
ferent treatment protocols.
The data analysis was performed using Review Manager
5.3 (Copenhagen: The Nordic Cochrane Centre, Cochrane
Collaboration, 2014).
Results
Selection and characteristics of the included studies
Twenty retrospective studies, with a total sample size of
1533 KTs, were included in the systematic review. The
whole process of study selection is reported in detail in
Fig. 1.
Therapeutic protocols used were CRS in 18 studies, CT in
13 studies, HIPEC in 7 studies, neoadjuvant CT in 2 studies,
and combinations of these in 6 studies.
Characteristics of the included studies, patients and KTs
were shown in Table 1.
Risk of bias within studies assessment
About the “Aim”, “Data” and “Endpoints” domains, all stud-
ies were classified at low risk of bias.
About the “Patients” domain, three studies were catego-
rized at low risk of bias [10–12], while 15 at unclear risk
of bias because they did not clearly specify the inclusion
criteria [4–7, 13–23]. Last, two studies were classified at
high risk of bias: one for considering all metastatic ovarian
tumors as KTs irrespectively of histology [24], and another
one for lumping together KT and other metastatic ovarian
cancers [25].
Archives of Gynecology and Obstetrics (2019) 300:15–23 17
Fig. 1  Flow diagram of studies identified in the systematic review
[Prisma template (Preferred Reporting Item for Systematic Reviews
and Meta-analyses)]
About the “Bias” domain, nine studies were considered
at unclear risk of bias, as they did not carry out multivariate
analysis to confirm results [5, 7, 11, 13, 18, 21–24].
About the “Follow-up” domain, one study was considered
at high risk of bias due to a follow-up too short in reference
to the OS to be assessed [7]; while five studies were consid-
ered at unclear risk because they did not specify how long
the follow-up was [4, 5, 12, 19, 22].
About the “Loss” domain, three studies were categorized
at low risk of bias, while other three studies at high risk of
bias because they lost more than 5% of the patients dur-
ing follow-up [5, 11, 12]. The remaining 14 studies were
considered at unclear risk because they did not specify how
many patients completed follow-up [4, 7, 10, 13–15, 17–19,
21–25].
Results about risk of bias for each included study were
graphically reported in Fig. 2.
Treatments
Seven studies showed that CRS significantly improved OS
compared to other treatments or association of treatments
without it [4, 6, 13, 15, 17, 19, 22]. This result was also
confirmed on multivariate analysis in five studies [4, 6, 15,
17, 19]. Guzel et al. did not show statistical significance
about this variable instead [25].
Regarding neoplastic residual, 11 studies showed that
CRS without residual (R0 CRS) had a significantly better
OS than CRS with residual (R + CRS) [6, 10–14, 18, 20,
21, 23, 24]. Six of these studies confirmed the finding on
multi-variate analysis [6, 10, 12, 14, 20, 24]. By contrast,
two studies showed no statistical significance about this vari-
able [7, 25].
CT was shown to significantly improve OS at uni- and
multi-variate analysis in five studies [4, 10, 14, 17, 19].
However, other five studies did not show statistical signifi-
cance for this variable [11, 18, 20, 22, 25].
Two articles compared CRS + CT against CT alone [7,
15]. In one study, CRS + CT showed significantly better OS
than CT alone [15], while in the other one no significant
difference was found [7].
The CRS + CT association was also compared with CRS
alone in two studies [14, 23]. In one study, the CRS + CT
protocol showed better results at both uni- and multi-variate
analysis [14]. Instead, the other one found no statistically
significant differences [23].
Regarding HIPEC, Rosa et  al. showed that
CRS + HIPEC + CT had a higher OS compared to CRS + CT,
and compared to CT alone, on both uni- and multi-variate
analysis [14]. Furthermore, Wu et  al. showed that the
CRS + HIPEC had better results than CRS alone, on both
uni- and multi-variate analysis [16]. Finally, Cheong et al.
found that there was no significant difference in OS between
patients treated with CRS + HIPEC and patients treated with
CRS + CT [22].
Only two studies assessed neoadjuvant CT in relation to
treatment protocols without it [5, 13]. Among these, Ganesh
et al. showed a significant lengthening of the OS at uni-
variate analysis, while Seow-En et al. showed no significant
differences.
Finally, Seow-en et al. found at univariate analysis that
the execution of the CRS in emergency regimen was related
to a minor OS compared to its execution in elective regimen.
Results about comparisons amongst OS related to the
treatment protocols are summarized in Table 2.
Discussion
Main finding and interpretation
Our study pointed out that several different therapeutic pro-
tocols are followed in the treatment of KT. The currently
available options for treating this neoplasm are CRS, adju-
vant CT, neoadjuvant CT and HIPEC; these treatments may
be used alone or in combination.
13

18

13
Table 1  Characteristics of the included studies, patients and KTs
Study (Refs.) Country Design Study period Mean age years (Range) Sample size Primary tumor site
Stomach Colorectal Mammary Others Unknown

Seow-en et al. [5] Singapore Retrospective Jan 2004–Dec 2015 54.2 ( ± 11.7) 38 4 22 2 9 1
Yu et al. [6] China Retrospective Jan 2005–Dec 2014 43.4 152 152 – – – –
Xu et al. [10] China Retrospective 1994–2013 49.3 ( ± 13.3) 57 – 57 – – –
Kammar et al. [7] India Retrospective Jan 2012–Dec 2015 42 25 – 25 – – –
Ganesh et al. [13] USA Retrospective Jan 1999–Jan 2015 50 195 – 195 – – –
Wu et al. [4] China Retrospective Jan 1990–Dec 2010 48 128 41 58 8 13 8
Rosa et al. [14] Italia Retrospective Jan 1990–Dec 2012 48 63 63 – – – –
Cho et al. [15] Korea Retrospective Mar 2004–Feb 2012 43.4 216 216 – – – –
Wu et al. [16] China Retrospective Jan 2000–Dec 2010 44 62 62 – – – –
Lu et al. [17] Taiwan Retrospective Mar 2000–Jul 2010 44.4 85 85 – – – –
Guzel et al. [25] Turkey Retrospective Jan 2001–Jan 2009 50.1 48 10 20 5 6 7
Jun et al. [18] Korea Retrospective 1981–2008 48.6 22 22 – – – –
Kim et al. [19] Korea Retrospective 1994–2006 42 34 25 2 – 1 6
Jiang et al. [20] China Retrospective Mar 1997–Dec 2003 44 54 26 23 3 2 –
McCormick et al. [11] USA Retrospective 1980–2005 51.5 40 – 40 – – –
Ayhan et al. [21] Turkey Retrospective 1982–2004 45.2 ( ± 13.5) 154 35 33 35 33 18
Cheong et al. [22] S. Korea Retrospective 1987–1998 45.8 54 54 – – – –
Cheong et al. [12] S. Korea Retrospective 1987–2000 44 34 34 – – – –
Kim et al. [24] Korea Retrospective 1987–1996 41 34 34 – – – –
Rayson et al. [23] Canada Observational 1984–1998 55.8 39 – 39 – – –
Archives of Gynecology and Obstetrics (2019) 300:15–23
Archives of Gynecology and Obstetrics (2019) 300:15–23 19
Fig. 2  a Assessment of risk of bias. Summary of risk of bias for each
study; plus sign: low risk of bias; minus sign: high risk of bias; ques-
tion mark: unclear risk of bias. b Risk of bias graph about each risk
of bias item presented as percentages across all included studies
To date, it is still not clear which treatment protocol is the
most effective one, and the management of patients with KT
is not standardized.
Cytoreductive surgery
Many studies reported the effectiveness of CRS in length-
ening the OS compared to the absence of such surgical
treatment [4, 6, 13, 15, 17, 19, 22]. Furthermore, there is
evidence that a radical CRS, in the absence of residuals
(R0 CRS), is related to a significant improvement in OS [6,
10–14, 18, 20–24].
In our study, only two articles showed results contrary to
these just shown. The first one did not show statistically sig-
nificant OS improvement either for CRS or for R0 CRS, sug-
gesting that the execution of surgery in all its degree of radi-
calness is not advisable [25]. The second one analyzed the
prognostic value of R0 margins, showing no significant OS
improvement compared to R + CRS [7]. This discrepancy
in the results might be partly due to some biases in these
studies, as already shown in the risk of bias within studies
assessment. In particular, study by Guzel et al. seemed to be
affected by a selection bias, not differentiating KTs from all
other metastatic ovarian tumors in the study sample, while
results by Kammar et al. seemed to be affected by a follow-
up duration too short to evaluate the efficacy of the treat-
ment. Based on this evidence, it appears deducible that R0
CRS may be essential in the treatment of KT.
Adjuvant chemotherapy
Regarding CT, results about its impact on OS are conflicting.
While some studies showed that CT significantly increased
OS [4, 10, 14, 17, 19], other ones showed opposite results,
with no significant OS improvement [11, 18, 20, 22, 25].
The efficacy of CT was also evaluated in association with
CRS in some studies. Two of these studies compared such
protocol to CT alone [7, 15], and two others to CRS alone
[14, 23]. However, even in this regard, the results are mixed.
Compared to CT alone, Cho et  al. showed significantly
longer OS with the CRS + CT protocol, while Kammar
et al. showed no significant difference. Similarly, compared
to CRS alone, Rosa et al. showed a significant increase in
OS for the combined protocol, while Rayson et al. did not
show significant difference. Given these findings, it seems
to be not possible to draw any univocal conclusions about
effectiveness of CT alone or combined with CRS. Thus,
it might be considerable to spare systemic CT for patients
with KT, in particular taking account the severe adverse
effects and performance status worsening associated with
its administration.
Hyperthermic intraperitoneal chemotherapy
Taking into account the above-mentioned considerations
on CT, adjuvant therapy with HIPEC might be a good
compromise. In the literature, only few studies have been
analyzed HIPEC for KTs patients [14, 16, 22]. Rosa et al.
assessed the association of HIPEC with CRS and CT. They
showed that such association significantly increased OS
more than both CRS + CT protocol and CT alone protocol,
supporting the independent prognostic value of HIPEC.
On the other hand, Wu et al. evaluated the effectiveness
13

20

Table 2  Comparisons amongst OS related to the treatment protocols

Study CRS VS no-CRS R0 CRS VS R + CRS CT VS no-CT

13
Univariate Multivariate Univariate Multivariate Univariate Multivariate
HR (95% CI) P value HR (95% CI) P value HR (95% CI) P value HR (95% CI) P value HR (95% CI) P value HR (95% CI) P value

Seow-en et al. – – – – – – – – – – – –
[5]
Yu et al. [6] 0.467 (0.318–  < 0.001 0.486 (0.323–  < 0.001 –  < 0.001 – – – – – –
0.685) 0.729)
Xu et al. [10] – – – – –  < 0.001 0.135 0.001 – 0.006 0.345 0.012
Kammar et al. – – – – – NS – – – – – –
[7]
Ganesh et al. – 0.003 – – – NR – NR – – – –
[13]
Wu et al. [4] 9.346 (4.950–  < 0.001 4.878 (1.572– 0.0060 – – – – 0.293 (0.195–  < 0.001 0.626 (0.371– NS
17.544) 15.15) 0.440) 1.057)
Rosa et al. [14] – – – – –  < 0.0001 –  < 0.0001 – 0.0005 – NS
Cho et al. [15] 0.404 (0.302–  < 0.001 0.458 (0.287– 0.001 – – – – – – – –
0.539) 0.732)
Wu et al. [16] – – – – – – – – – – – –
Lu et al. [17] 0.43 (0.26– 0.002 0.36 (0.19–0.68) 0.002 – – – – 0.14 (0.07–  < 0.001 0.21 (0.08– 0.002
0.73) 0.27) 0.57)
Guzel et al. [25] – NS – – – NS – NS – NS – –
Jun et al. [18] – – – – – 0.0003 – – – NS – –
Kim et al. [19] 1.258*(1.042– 0.017 1.311*(1.084– 0.005 – – – – 2469* (1.425– 0.001 2.347*(1.309– 0.004
1.520) 1.587) 4.273) 4.219)
Jiang et al. [20] – – – – –  < 0.01 –  < 0.01 – NS – –
McCormick – – – – –  < 0.0001 – – – NS – –
et al. [11]
Ayhan et al. – – – – – 0.0039 – – – – – –
[21]
Cheong et al. – 0.001 – – – – – – – NS – –
[22]
Cheong et al. – – – – – 0.0001 –  < 0.0001 – – – –
[12]
Kim et al. [24] – – – – 0.40* (1.17– 0.036 – – – – – –
0.94)
Rayson et al. – – – – – 0.014 – – – – – –
[23]
Archives of Gynecology and Obstetrics (2019) 300:15–23
 Table 2  (continued)
Study CRS + CT VS CRS + CT VS CRS + HIPEC + CT CRS + HIPEC VS CRS CRS + HIPEC Neoadjuvant Emergency
CT CRS VS CRS + CT VS CT VS CRS + CT CT VS no Neo- VS elective
adjuvant CT regimen
Univariate Univariate Univariate Univariate Multivariate Univariate Univariate Univariate
P value P value P value HR (95% CI) P value HR (95% CI) P value P value P value P value

Seow-en et al. [5] – – – – – – – – NS 0.027

Yu et al. [6] – – – – – – – – – –
Xu et al. [10] – – – – – – – – – –
Kammar et al. [7] NS – – – – – – – – –
Ganesh et al. [13] – – – – – – – – 0.02 –
Wu et al. [4] – – – – – – – – – –
Rosa et al. [14] – 0.0005 0.0005 – – – – – – –
Cho et al. [15] 0.002 – – – – – – – – –
Archives of Gynecology and Obstetrics (2019) 300:15–23

Wu et al. [16] – – – – 0.018 2996 (1.245– 0.014 – – –

7.208)
Lu et al. [17] – – – – – – – – – –
Guzel et al. [25] – – – – – – – – – –
Jun et al. [18] – – – – – – – – – –
Kim et al. [19] – – – – – – – – – –
Jiang et al. [20] – – – – – – – – – –
McCormick et al. – – – – – – – – – –
[11]
Ayhan et al. [21] – – – – – – – – – –
Cheong et al. [22] – – – – – – – NS** – –
Cheong et al. [12] – – – – – – – – – –
Kim et al. [24] – – – – – – – – – –
Rayson et al. [23] – NS** – – – – – – – –

HR hazard ratio, CRS cytoreductive surgery, R0 CRS CRS without residual, R + CRS CRS with residual, CT adjuvant chemotherapy, HIPEC hyperthermic intraperitoneal chemotherapy, NS non-
significant, * relative risk (no hazard ratio)

13
21

22
of HIPEC in combination with CRS, showing that this
association increased the OS about three times on average
compared to CRS alone. Finally, Cheong et al. investi-
gated the difference about OS between the CRS + HIPEC
protocol and CRS + CT protocol. They did not show any
significant difference between the two protocols, conclud-
ing that CT and HIPEC might have the same effectiveness
if associated with CRS. Despite the low number of studies,
HIPEC seems to be effective both alone and in combina-
tion with CRS. Furthermore, HIPEC has shown an effec-
tiveness at least equal to CT. Therefore, also given the less
severe adverse effects compared to CT, HIPEC seems to
be a preferable adjuvant approach for KT.
Neoadjuvant chemotherapy
Little data have been collected on neoadjuvant CT, which
seems to be rarely used in KT therapeutic protocols. In the
literature, only two studies assessed it, showing conflict-
ing results. In particular, Ganesh et al. showed increased
OS with preoperative chemotherapy, while Seow-En et al.
did not show statistically significant difference. Therefore,
there is no sufficient evidence to advocate or discourage
the use of neoadjuvant CT. However, it appears reasonable
that neoadjuvant CT might be indicated when R0 CRS is
not feasible due to the local extension of KT.
Strengths and limitations
To our knowledge, this may be the first systematic review
about treatments of KT. The study aim was to assess which
treatment or combination of treatments may be the most
effective in terms of increased OS. In fact, to date, treat-
ment of KT is not standardized. Despite the rarity of the
disease, this appears as a serious wealth problem, consid-
ering the poor prognosis of such patients, due to tumor
aggressiveness, advanced stage, diagnostic difficulties
and poor treatment efficacy. The low quality of evidence
about treatment protocols to be followed, partly due to the
tumor rarity itself, also contributes to the poor prognosis.
Thus, we tried to improve the quality of evidence, pro-
viding a systematic analysis on a relatively large sample
(N = 1533).
A limit of our study might be the retrospective design of
the included studies. Nevertheless, this appears as the only
possible study design due to the rarity of KT. In fact, pro-
spective trials would be difficult to perform. Another limit
may be the lack of a multi-variate analysis in some included
studies. Moreover, the lack of a sufficient number of studies
that compared the same treatment or combination of treated
precluded the feasibility of a meta-analysis.
13
Archives of Gynecology and Obstetrics (2019) 300:15–23
Conclusion
CRS and in particular R0 CRS are the treatments that show
the clearest results in improving OS in KT patients. Regard-
ing adjuvant CT, results about its effectiveness are conflict-
ing, but it seems that CT cannot replace surgery in a satisfac-
tory way. By contrast, despite being assessed in few studies,
HIPEC seems to be not only effective both alone and in
combination with CRS, but also related to fewer adverse
effect than CT. The usefulness of neoadjuvant CT is still
unclear, and seems to be advisable only to try a R0 CRS.
Finally, the association of R0 CRS with HIPEC seems to
be the most effective and safe therapeutic protocol for KT
patients.
Author contributions  RL: study conception, electronic search, eligi-
bility of the studies, inclusion criteria, risk of bias, data extraction
and data analysis. MDL: electronic search, eligibility of the studies,
inclusion criteria, risk of bias, data extraction and data analysis, and
manuscript preparation. AT, AR: study conception, disagreement reso-
lution, and manuscript preparation. GS: electronic search, eligibility
of the studies, inclusion criteria, risk of bias, data extraction and data
analysis. MM: methods supervision and manuscript preparation. LI:
study design, methods supervision, and manuscript preparation. MDA:
study design, manuscript preparation, and whole study supervision. FZ:
study design, methods supervision, and whole study supervision. FC:
study conception and whole study supervision.
Funding  No financial support was received for this study.
Compliance with ethical standards 
Conflict of interest  The authors report no conflict of interest.
References
1. Al-Agha OM, Nicastri AD (2006) An in-depth look at Krukenberg
tumor: an overview. Arch Pathol Lab Med 130(11):1725–1730
2. Kubeček O, Laco J, Špaček J et al (2017) The pathogenesis, diag-
nosis, and management metastatic tumors to the ovary: a compre-
hensive review. Clin Exp Metastasis 34(5):295–307
3. Novak E, Gray LA (1938) Krukenberg tumors of the ovary:
clinical and pathological study of 21 cases. Surg Gynecol Obstet
66:157–167
4. Wu F, Zhao X, Mi B et al (2015) Clinical characteristics and
prognostic analysis of Krukenberg tumor. Mol Clin Oncol
3(6):1323–1328
5. Seow-En I, Hwarng G, Tan GHC, Ho LML, Teo MCC (2018)
Palliative surgery for Krukenberg tumors—12-year experience
and review of the literature. World J Clin Oncol 9(1):13–19
6. Yu P, Huang L, Cheng G et al (2017) Treatment strategy and
prognostic factors for Krukenberg tumors of gastric origin: report
of a 10-year single-center experience from China. Oncotarget
8(47):82558–82570
7. Kammar PS, Engineer R, Patil PS, Ostwal V, Shylasree TS, Sak-
lani AP (2017) Ovarian metastases of colorectal origin: treatment
Archives of Gynecology and Obstetrics (2019) 300:15–23 23
patterns and factors affecting outcomes. Indian J Surg Oncol
8(4):519–526
8. Moher D, Shamseer L, Clarke M et al (2015) Preferred report-
ing items for systematic review and meta-analysis protocols
(PRISMA-P) 2015 statement. Syst Rev 4:1
9. Slim K, Nini E, Forestier D et al (2003) Methodological index for
non-randomized studies (minors): development and validation of
a new instrument. ANZ J Surg 73(9):712–716
10. Xu KY, Gao H, Lian ZJ, Ding L, Li M, Gu J (2017) Clinical analy-
sis of Krukenberg tumours in patients with colorectal cancer—a
review of 57 cases. World J Surg Oncol 15(1):25
11. McCormick CC, Giuntoli RL 2nd, Gardner GJ et al (2007) The
role of cytoreductive surgery for colon cancer metastatic to the
ovary. Gynecol Oncol 105(3):791–795
12. Cheong JH, Hyung WJ, Chen J, Kim J, Choi SH, Noh SH (2004)
Surgical management and outcome of metachronous Krukenberg
tumors from gastric cancer. J Surg Oncol 87(1):39–45
13. Ganesh K, Shah RH, Vakiani E et al (2017) Clinical and genetic
determinants of ovarian metastases from colorectal cancer. Cancer
123(7):1134–1143
14. Rosa F, Marrelli D, Morgagni P et al (2016) Krukenberg tumors
of gastric origin: the rationale of surgical resection and periopera-
tivetreatments in a multicenter western experience. World J Surg
40(4):921–928
15. Cho JH, Lim JY, Choi AR et  al (2015) Comparison of sur-
gery plus chemotherapy and palliative chemotherapy alone for
advanced gastric cancer with krukenberg tumor. Cancer Res Treat
47(4):697–705
16. Wu XJ, Yuan P, Li ZY et al (2013) Cytoreductive surgery and
hypertermic intraperitoneal chemotherapy improves the survival
of gastric cancer patients with ovarian metastasis and peritoneal
dissemination. Tumour Biol 34(1):463–469
17. Lu LC, Shao YY, Hsu CH et al (2012) Metastasectomy of Kruke-
nberg tumors may be associated with survival benefits in patients
with metastatic gastric cancer. Anticancer Res 32(8):3397–3401
18. Jun SY, Park JK (2011) Metachronous ovarian metastases fol-
lowing resection of the primary gastric cancer. J Gastric Cancer.
11(1):31–37
19. Kim WY, Kim TJ, Kim SE et al (2010) The role of cytoreductive
surgery for non-genital tract metastatic tumors to the ovaries. Eur
J Obstet Gynecol Reprod Biol 149(1):97–101
20. Jiang R, Tang J, Cheng X, Zang RY (2009) Surgical treatment for
patients with different origins of Krukenberg tumors: outcomes
and prognostic factors. Eur J Surg Oncol. 35(1):92–97
21. Ayhan A, Guvenal T, Salman MC, Ozyuncu O, Sakinci M, Basa-
ran M (2005) The role of cytoreductive surgery in nongenital can-
cers metastatic to the ovaries. Gynecol Oncol 98(2):235–241
22. Cheong JH, Hyung WJ, Chen J, Kim J, Choi SH, Noh SH (2004)
Survival benefit of metastasectomy for Krukenberg tumors from
gastric cancer. Gynecol Oncol 94(2):477–482
23. Rayson D, Bouttell E, Whiston F, Stitt L (2000) Outcome after
ovarian/adnexal metastectomy in metastatic colorectal carcinoma.
J Surg Oncol 75(3):186–192
24. Kim HK, Heo DS, Bang YJ, Kim NK (2001) Prognostic factors
of Krukenberg’s tumor. Gynecol Oncol 82(1):105–109
25. Guzel AB, Kucukgoz G, Paydas S et al (2012) Preoperative evalu-
ation, clinical characteristics and prognostic factors of nongenital
metastatic ovarian tumors: review of 48 patients. Eur J Gynaec
Oncol 33(5):493–497
Publisher’s Note Springer Nature remains neutral with regard to
jurisdictional claims in published maps and institutional affiliations.
13