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Human Reproduction, Vol.29, No.7 pp. 1380 –1386, 2014
Advanced Access publication on May 8, 2014 doi:10.1093/humrep/deu101
REVIEW Embryology
Can healthy babies originate from
oocytes with smooth endoplasmic
reticulum aggregates? A systematic
mini-review
Department of Gynaecology, CHU St-Pierre, Université Libre de Bruxelles, rue Haute 322, Brussels 1000, Belgium
*Correspondence address. Tel: +32-25-35-34-66; Fax: +32-25-35-34-09; E-mail: [email protected]
Submitted on January 23, 2014; resubmitted on March 31, 2014; accepted on April 8, 2014
study question: Is it time to reconsider whether oocytes affected by smooth endoplasmic reticulum aggregates (SERa) should still be
destroyed?
summary answer: At the time of writing, the literature shows that 171 apparently healthy babies have been born from SERa+ cycles
amongst which 22 were from SERa+ oocytes.
what is known already: The SER dysmorphism has been associated with negative embryological, clinical and neonatal outcomes,
which led to a recommendation in 2011 to avoid inseminating affected oocytes. The data in the literature are nevertheless conflicting and
some centres have continued using SERa+ oocytes.
study design, size, duration: A systematic mini-review of the literature to 7 November 2013 was performed with the keywords
‘Smooth Endoplasmic Reticulum’ and ‘oocyte’, limited to humans and written in English.
participants/materials, setting, methods: Articles (Pubmed) and major abstracts where the effect of the SER dysmorphism was studied as an individual feature on embryological, clinical or neonatal outcomes were included in this review.
main results and the role of chance: From a total of 297 publications identified, 13 were selected as being relevant to this
review. One hundred eighty-three babies have been reported to be born from SERa+ cycles, 171 were healthy, 8 live births presented malformations, 3 were neonatal deaths, 1 was a stillborn and additionally 4 terminations of pregnancy occurred.
limitations, reasons for caution: Data concerning SERa+ oocytes in the literature are scarce, the studies are small, heterogeneous and results are conflicting. The malformations observed could be due to over-reporting of scattered alarming results. Alternatively, an
under-reporting of complications cannot be excluded.
wider implications of the findings: Centres that have or that are including transfers of SERa+ embryos in their IVF procedures
should publish their clinical and neonatal outcomes as well as the follow-up of children. The birth of healthy babies from SERa+ embryos is
encouraging and might lead in the future to a revision of the current consensus on the SER dysmorphism. Further research is needed to understand
the origin of this dysmorphism and help avoid its occurrence. Therefore, until we have a better understanding of the situation, transfers of affected
embryos should be carried out with caution.
study funding/competing interest(s): We have no conflicts of interest to declare and no funding was received.
Key words: smooth endoplasmic reticulum aggregates / oocyte dysmorphism / clinical outcome / embryology / assisted reproduction
& The Author 2014. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved.
For Permissions, please email: [email protected]
Downloaded from http://humrep.oxfordjournals.org/ at South China Agricultural University on June 29, 2014
Chloë Shaw-Jackson*, Nina Van Beirs, Anne-Laure Thomas,
Serge Rozenberg, and Candice Autin
1381
Smooth endoplasmic reticulum aggregates: a mini-review
Introduction
Methods
A Pubmed systematic literature search using the keywords ‘Smooth Endoplasmic Reticulum’ and ‘oocyte’ limited to humans was performed (last
search on 21st October 2013), as well as in the Human Reproduction,
Fertility and Sterility and Reproductive Biomedicine Online Journals (last search
on 7th November 2013).
English articles identified by the search were selected for inclusion in the
review if they reported data concerning the effect of the SER dysmorphism
on at least one of the following outcomes: fertilization rate, pregnancy rate,
miscarriage rate, implantation rate, embryo quality and neonatal outcome.
Results
Design and limitations of the studies
The search identified a total of 297 records and 13 of these were selected
for this review (Fig. 2). These included 5 articles, 7 abstracts and 1 case
report. The design of the majority of the studies was retrospective
(n ¼ 9) (Table I), although for one of them, the authors claimed the
study to be randomized.
Two studies were prospective, one specified that transfer of SERa+
embryo transfers was avoided (Ebner et al., 2008) and for the other
one, no information on embryo selection was provided (Yang et al., 2008).
Only two retrospective studies specified that embryos were selected
for transfer irrespective of the presence of SERa (Bielanska and Leveille
2011; Mateizel et al., 2013) and one specified that SERa+ embryo transfers were avoided (Otsuki et al., 2004).
In most studies, it was not mentioned whether information was provided to the patients concerning the presence of SERa nor if patients’
consent was obtained before transfer of affected embryos. In one
study however, patients were informed about the presence of SERa+
oocytes and the risk of a reduced pregnancy rate even when SERa2
embryos are transferred (Otsuki et al., 2004). In a second study, the
authors specified that the rare transfers of SERa+ embryos only
occurred after consultation with the patients (Ebner et al., 2008).
Preferential transfers of SERa2 over SERa+ embryos introduce a bias
for cycle comparisons and even more so for oocyte comparisons. When
studying the effect of oocyte morphology on clinical outcome, the endpoint should at least be childbirth. Data concerning neonatal outcomes
for SERa+ embryos and even SERa2 embryos from SERa+ cycles are
scarce in the literature. In 5 publications, mainly abstracts, no neonatal
Figure 1 Human metaphase II oocytes as viewed by light microscopy. (A) A metaphase II oocyte containing an SERa (arrow) (400× magnification).
(B) A metaphase II oocyte with a fluid-filled vacuole (arrow) (400× magnification).
Downloaded from http://humrep.oxfordjournals.org/ at South China Agricultural University on June 29, 2014
In 2011, it was recommended not to inseminate oocytes affected by
smooth endoplasmic reticulum aggregates (SERa), since they might be
associated with an increased risk of abnormal outcome (Alpha Scientists
in Reproductive Medicine and ESHRE Special Interest Group of
Embryology, 2011).
Several reports focusing specifically on SERa+ cycles/oocytes have
indeed shown negative outcomes in terms of fertilization, embryo development and pregnancy rates as well as compromised obstetric and neonatal outcomes (Otsuki et al., 2004; Ebner et al., 2008; Akarsu et al.,
2009; Wallbutton and Kasraie, 2010; Sá et al., 2011). However, a
recent publication demonstrated that healthy babies could be obtained
using oocytes that contain SERa (SERa+ oocytes) (Mateizel et al.,
2013). The data in the literature are controversial and some authors
present results for SERa+ cycles, others for SERa+ oocytes. Indeed,
oocytes that appear at first sight using light microscopy as negative for
SERa but which arise from the same cohort of SERa+ gametes
(defined as SERa+ cycles), may in fact also be affected when studied
using transmission electron microscopy (Otsuki et al., 2004). In order
to have a clear overview of what is known, we performed a systematic
mini-review analyzing clinical outcomes for SERa+ cycles and oocytes.
SERa can be clearly distinguished morphologically by light microscopy from
fluid-filled vacuoles as shown in Fig. 1.
1382
Shaw-Jackson et al.
data were available (Table I) and unfortunately, no full length articles
were published at a later date.
Methodology of studies on SERa
In 2 studies, fertilization was significantly decreased for SERa+ oocytes
and in one study for SERa+ cycles (Table II). There was a trend
towards lower clinical pregnancy (CP) rates in all studies for SERa+
oocytes compared with SERa2 oocytes but this decrease was only significant in one study. For SERa+ and SERa2 cycles, one report showed a
significant decrease in pregnancy rates for SERa+ cycles.
Effect of SERa on miscarriage and
implantation rates
Three studies reported data on the effect of SERa+ oocytes on
biochemical pregnancy and/or miscarriage rates. Transfer of SERa+
embryos was found to increase the risk of miscarriage by 20% in one
of the studies (Braga et al., 2013). For SERa+ cycles, 6 studies reported
data. One study showed that the combined biochemical pregnancy and
miscarriage rates were significantly higher for SERa+ cycles compared
with SERa2 cycles (Ebner et al., 2008). A second study reported an
increased biochemical pregnancy rate for SERa+ cycles compared
with SERa2 cycles (Otsuki et al., 2004). Four and 3 studies analyzed
the effects of SERa+ cycles and SERa+ oocytes, respectively, on
implantation rates. One study demonstrated a significant decrease of
implantation rates for SERa+ cycles (Otsuki et al., 2004).
Effect of SERa on embryo quality
The effect of SERa on embryo quality was studied in 10 publications.
These data included Day 3 and Day 5 analysis, cell fragmentation, cell
number, embryo cleavage rate, blastulation, inner cell mass quality and
cycle efficiency. Two studies found a significant decrease of embryo
quality for SERa+ cycles (Sá et al., 2011; Mateizel et al., 2013) and 3
for SERa+ gametes (Ebner et al., 2008; Sá et al., 2011; Braga et al.,
Figure 2 Flow chart for the systematic literature search on ‘Smooth
Endoplasmic Reticulum’ in humans.
Table I Methodology employed and outcomes studied when evaluating smooth endoplasmic reticulum aggregate positive
(SERa1) cycles in women.
Authors, Year published
Study design
SERa1 cycles (n)
SERa1 cycles (%)
SERa1 oocytes (%)
FR
PR
IR
MR
EQ
PO
.............................................................................................................................................................................................
Otsuki et al. (2004)
RS
18
9.4
De Los Santos et al. (2005)*
RS
107
9.2
Maldonado et al. (2006)*
RRS1
16
y
y
Yang et al. (2008)*
PS
71
2.8
19.0
y
y
30
6.2
25.0
y
y
y
y
y
y
Ebner et al. (2008)
POS
Munaswamy et al. (2008)*
RS
Akarsu et al. (2009)
CR
3
Sá et al. (2011)
RS
60
y
y
y
y
y
y
y
y
y
y
y
y
y
y
y
y
y
y
10.3
18.8
19.3
y
y
y
17.6
y
y
y
Bielanska and Leveille (2011)* RS
121
Mateizel et al. (2013)
394
5.4
RS
34.4
Braga et al. (2013)
CCS
Miwa et al. (2013)*
RS
86
7.3
y
Hattori et al. (2013)*
RS
102
7.8
y
y
y
y
y
y
y
y
y
y
y
y
20.4
y
y
y
RS, retrospective study; RRS, randomized retrospective study; PS, prospective study; POS, prospective observational study; CCS, case control study; CR, case report; FR, fertilization rate;
PR, pregnancy rate; IR, implantation rate; MR, miscarriage rate and/or BCR biochemical rate; EQ, embryo quality; PO, perinatal outcome; % SERa+ cycles ¼ n SERa+ cycles/n total
cycles; % SERa+ oocytes ¼ n SERa+ oocytes/n total oocytes in SERa + cycle; y ¼ yes, outcome studied.
*Abstracts. 1the authors claim that their study was an RR study, but we have no way to clarify this point.
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For 2 studies, the frequency of SERa was provided per embryo
(375/5516); (Braga et al., 2013) or per patient (53/510); (Munaswamy
et al., 2008) instead of per cycle (Table I). For 10 studies, authors
analyzed either differences between SERa+ and SERa2 cycles (n ¼ 3)
or between SERa+ and SERa2 oocytes in the same cycle (n ¼ 2) or
data from both (n ¼ 5). Two studies were only included for their data
provided on neonatal outcome (Akarsu et al., 2009; Miwa et al., 2013)
and finally a case– control study reported on blastocyst quality and
pregnancy outcomes per studied embryo (Braga et al., 2013).
Fertilization and clinical pregnancy rates for
SERa1 versus SERa2 cycles and oocytes
1383
Smooth endoplasmic reticulum aggregates: a mini-review
Table II Comparison of fertilization and CP rates between SERa1 and SERa2 cycles and oocytes in women.
Authors, year published
Fertilization rate
CP rate
........................................................................ ........................................................................
SERa1
cycles (%)
SERa2
cycles (%)
SERa1
oocytes (%)
SERa2
oocytes (%)
SERa1
cycles (%)
SERa2
cycles (%)
SERa1
oocytes (%)
SERa2
oocytes (%)
.............................................................................................................................................................................................
Otsuki et al. (2004)
81.6
85.2
Maldonado et al. (2006)
69.8
71.0
Munaswamy et al. (2008)
5.6*
47.1
86.0
Yang et al. (2008)
28.2*
50.1
88.0
32.0*
68.0*
73.0
36.5
45.2
71.9
58.9**
77.4**
26.7
41.1
73.0
77.0
21.0
36.0
Sá et al. (2011)
69.9*
76.0*
44.7*
75.8*
47.3
38.4
25.0
52.5
Mateizel et al. (2013)
76.2
73.5
72.9
77.0
33.0
32.4
22.6
32.4
Hattori et al. (2013)
68.9
70.7
62.6
70.2
25.4
21.0
13.5
29.2
Bielanska and Leveille (2011)***
Blanks in table reflect no available data.
CP: clinical pregnancy; P values refer to the comparisons between SERa+ and SERa2 cycles or oocytes. *P , 0.05 **P , 0.01 and *** no statistics.
A total of 171 healthy babies were born from SERa+ cycles and perinatal
complications occurred in 16 pregnancies (Table III). These complications included 1 stillborn, 2 neonatal deaths and 13 malformations,
which led to 4 pregnancy terminations and 1 neonatal death (Table III).
Altogether, 22 healthy babies were born specifically from SERa+
embryos, including fresh and cryopreserved transfers and also twin
births originating from mixed transfers. Malformations were observed
in 3 pregnancies with SERa+ embryos.
Three studies (Ebner et al., 2008; Sá et al., 2011; Mateizel et al., 2013)
allowed us to calculate the malformation rate per live birth for SERa+
cycles: a malformation rate of 5.6% (7/126) was obtained, compared
with 2.2% (38/1762) for SERa – cycles.
small SERa and associated mitochondria act as Ca2+ stores (Sá et al.,
2011; Sathananthan, 2013). The fundamental role of Ca2+ in fertilization
and early embryo development has been demonstrated by numerous
studies (Homa et al., 1993; Carroll et al, 1996). The presence of SERa disturbs Ca2+ stores and oscillations (Van Blerkom, 2011). When normal
metaphase II oocytes and SERa+ oocytes were loaded with a fluorescent Ca2+ reporter and activated with the Ca2+ ionophore A23187,
instead of a normal transient and uniform signal, free Ca2+ increases
occurred in distinct regions for longer durations in affected oocytes
(Van Blerkom, 2011). Otsuki et al. (2004) showed that SERa disappear
16 –20 h after ICSI. Indeed, when fertilization of an affected egg
occurs, the calcium release would be accompanied by the disappearance
of the aggregates. On the other hand, several authors describe the presence of SERa in unfertilized eggs after conventional IVF (Van Blerkom and
Henry, 1992; Meriano et al., 2001). In this case, the absence of a Ca2+
release might explain the unfertilized status of the egg and the continued
presence of the SERa. Although the rescue of unfertilized eggs containing
SERa with Ca2+ ionophores might be considered, extreme caution
should be taken, since calcium patterns may be far from normal.
A study in rabbits, where the first calcium rise was increased experimentally did not appear to affect preimplantation embryo development.
However, during the fetal stages, major developmental and differentiation defects in organogenesis were observed (Ozil and Huneau, 2001).
Discussion
Role of SERa in adverse clinical outcomes
2013). For SERa+ cycles, the first case described decreased embryo
cleavage and blastocyst formation (Sá et al., 2011). The second case
reported a reduced cycle efficiency (selection of embryos for transfer
or cryopreservation) when embryos were cultured to Day 5 (Mateizel
et al., 2013). Concerning SERa+ oocytes, a reduced cleavage rate (Sá
et al., 2011), blastocyst formation (Ebner et al., 2008; Sá et al., 2011),
inner cell mass quality (Braga et al., 2013) and blastocyst expansion
(Braga et al., 2013) were observed.
Perinatal outcomes, for embryos, originating
from SERa1 cycles
Origin of SERa and the role of calcium
The appearance of SERa may be due to ovary hyper-stimulation (Van
Blerkom and Henry, 1992). Indeed, several studies have demonstrated
that the duration of ovarian stimulation was found to be longer and the
total amount of gonadotrophins administered higher for cycles with
affected gametes (Otsuki et al., 2004; Ebner et al., 2008; Sá et al.,
2011). Analysis of the occurrence of SERa in spontaneous cycles as
well as determining the effect of a change of stimulation protocol on
aggregate recurrence would help our understanding of the origin of
this pathology (Ebner et al., 2013). In normal oocytes, SER vesicles,
Even though there are conflicting results in the literature, the data show
that SERa do affect clinical and embryological outcomes to a certain
extent. Variation in population, fertility etiology, stimulation protocols
and study design and size can probably explain part of these discrepancies. In terms of perinatal complications, a total of 16 incidents out of
187 pregnancies were found in the literature when studying SERa.
One must keep in mind though, that the majority of transfers included
in these studies concern SERa2 embryos originating from SERa+
cycles. The largest study by Mateizel et al. (2013) described a major malformation rate per live birth for SERa 2 cycles of 2.1%. If we include
pregnancy terminations and stillborns, this rate is increased to 4.2%
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72.0
72.8
Ebner et al. (2008)
1384
Shaw-Jackson et al.
Table III Perinatal outcomes for babies born from fresh or cryopreserved SERa1 cycles.
Authors, year published
Type of embryo transfer
Perinatal outcomes
..............................................................................................
HB
PC
Type of PC
.............................................................................................................................................................................................
Akarsu et al. (2009)
SERa+
Sá et al. (2011)
SERa+
Bielanska and Leveille (2011)
SERa+
1
Mateizel et al. (2013)
SERa+
10
Hattori et al. (2013)
SERa+
4
SERa2
SERa2
3
Bielanska and Leveille (2011)
SERa2
16
Sá et al. (2011)
SERa2
23
Miwa et al. (2013)
SERa2
14
Mateizel et al. (2013)
SERa2
59
Ebner et al. (2008)
Mix
Sá et al. (2011)
Mix
52
Bielanska and Leveille (2011)
Mix
Mateizel et al. (2013)
Mix
Total
2 multiple malformations (1 PT, 1 neonatal death)
1
1 ventricular septal defect
1
1 Beckwith-Wiedemann syndrome
1
1 diaphragmatic hernia
4
1 stillborn, 3 malformations*
2
2 neonatal deaths
133
2
1 heart defect + omphalocele (PT) and 1
Down syndrome (PT)
232
3
1 47 XX+18 (PT), 2 malformations*
171
16
HB, healthy babies; PC, perinatal complications; Mix, mixed transfer of SERa+ and SERa2 embryos; PT, pregnancy termination.
2,3
Twin pregnancies for mixed transfers are specified: 22 twin pregnancies; 33 twin pregnancies.
*Included the following: 1 47 XY+21, 1 duplicated kidney; 2 brachialis paresis, 1 hypospadias.
(63/1490) compared with 8.6% for SERa+ cycles reported in this
review. Amongst the variety of pathologies detected, one case of a
Beckwith – Wiedemann syndrome was found. An increased incidence
of imprinting diseases may be correlated with the use of assisted reproduction techniques (Manipalviratn et al., 2009). Whether there is an association between SERa and imprinting disorders is unknown. Akarsu
et al. (2009) published a case report where multiple fetal malformations
were found for two pregnancies where the patient systematically had all
oocytes affected in 3 consecutive cycles. In a second case report (Wallbutton and Kasraie, 2010), a patient had fertilization failure by conventional IVF and practically all of her 15 oocytes displayed large SERa
(.25 mm). In two subsequent ICSI cycles, again most oocytes were
affected and poor fertilization, embryonic arrest and no pregnancies
were reported. In this study, polscope analysis did not detect a
displacement of the meiotic spindle and the authors concluded that
a genetic element would help to explain the relative homogeneity of
SERa formation within successive oocyte cohorts. These observations
raise the question of whether a threshold exists between the frequency
and/or size of the aggregates for which the risk of a negative outcome
might exist (Ebner et al., 2013). On the other hand, malformations
have been reported for transfers of non-affected embryos originating
from SERa+ cycles (Otsuki et al., 2004; Ebner et al., 2008; Mateizel
et al., 2013).
Frequency of SERa1 cycles/oocytes
and ethical considerations
This review shows that up to 10% cycles can present SERa, and a range of
19– 34% of oocytes per affected cycle are shown to be positive for
aggregates by observation under light microscopy. These percentages
are underestimates since oocytes that are fertilized by conventional
IVF would generally not show the dysmorphism at the time of fertilization
assessment (Van Blerkom and Henry, 1992; Meriano et al., 2001; Otsuki
et al., 2004). In addition, more subtle re-organization of the SER might
go unnoticed by light microscopy (Otsuki et al., 2004). Cases other
than those described above (Akarsu et al., 2009; Wallbutton and
Kasraie, 2010) where a whole cohort of oocytes is affected by this dysmorphism have been reported. Indeed, Maldonado et al., (2006) published 16 cycles where patients had mixed ICSI/IVF cycles. All oocytes
were affected in the ICSI cycles, but the status regarding SERa of
oocytes treated by conventional IVF could not be assessed before
Day 1. The chances that all oocytes were affected by SERa are high.
Mateizel et al. (2013) reported a healthy birth from one patient in
whom all 3 oocytes were affected. Finally, our own unpublished data
revealed that over a period of 2 years, 24 cycles occurred with all
oocytes affected. The majority of patients had few oocytes, though 7
women had over 3. Additionally, 11 transfers took place with affected
embryos since no other embryo of equivalent quality was available
(Shaw-Jackson et al., unpublished data). Eight healthy births and 2
ongoing pregnancies occurred from these affected embryo transfers.
Taking into account the fact that the presence of SERa+ oocytes has
been shown to be recurrent in just under 40% of subsequent cycles
(Ebner et al., 2006; Sá et al., 2011), if the ESHRE and Alpha guidelines
were to be followed, some couples would have to consider oocyte donation or adoption to achieve a family. Although, these patients represent a minority of those undergoing treatment, each couple should
be treated as unique and offered a fair chance of conceiving with their
own gametes. This is especially relevant in countries where the
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Otsuki et al. (2004)
Ebner et al. (2008)
2
Smooth endoplasmic reticulum aggregates: a mini-review
number of fertilized oocytes is restricted. Moreover, supernumerary
affected embryos of good quality in larger oocyte cohorts, capable of
possibly developing into healthy babies could be cryopreserved and
transferred in frozen cycles.
Oocyte dysmorphisms affect an important proportion of oocytes.
The majority of studies in the past has analyzed pooled data for different
dysmorphisms and has not allowed determining which ones are relevant
in embryo selection (Rienzi et al., 2011). There is clearly a need to clarify
the issue concerning clinical outcomes for SERa+ embryos in order, on
the one hand, to reassure the couples involved and on the other hand, to
avoid oocyte or embryo wastage.
Data in the literature concerning clinical outcomes for SERa as a unique
feature are sparse and controversial. It remains unclear whether there is
truly an association between SERa and fetal malformations. It is possible
that only scattered alarming results are published and that they might not
be related to SERa, thus resulting in a biased conclusion. Alternatively, an
under-reporting of complications cannot be excluded.
Laboratories should record information concerning SERa, and report
the clinical outcome or destroy affected gametes. Data should be published with details on frequency and size of aggregates, and a follow-up
of babies carried out, in order to determine whether SERa transfers
are associated with adverse outcomes. As recently suggested in a
letter to the editor (Ebner et al., 2013), the birth of apparently healthy
babies from affected gametes might lead to a revision of the current
consensus in the future. In the meanwhile, if transfers of affected
embryos are performed, they should take place with caution and only
when no alternative embryos of sufficient quality are available.
Acknowledgements
The authors are grateful to Evelyne Bertrand, Jérôme Colin and
Bénédicte Becker for helpful scientific discussions.
Authors’ roles
C.S.-J. did the literature search, data analysis and wrote the manuscript.
A.-L.T. and N.V.B. helped with the literature search, C.A. and S.R. were
involved in the data analysis. All authors contributed to the scientific
discussions.
Funding
No funding was received for this study.
Conflict of interest
None declared.
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