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Erschienen in: BMC Nephrology 1/2019

Open Access 01.12.2019 | Research article

Pregnancy outcomes in women with kidney transplant: Metaanalysis and systematic review

verfasst von: Silvi Shah, Renganathan Lalgudi Venkatesan, Ayank Gupta, Maitrik K. Sanghavi, Jeffrey Welge, Richard Johansen, Emily B. Kean, Taranpreet Kaur, Anu Gupta, Tiffany J. Grant, Prasoon Verma

Erschienen in: BMC Nephrology | Ausgabe 1/2019

Abstract

Background

Reproductive function in women with end stage renal disease generally improves after kidney transplant. However, pregnancy remains challenging due to the risk of adverse clinical outcomes.

Methods

We searched PubMed/MEDLINE, Elsevier EMBASE, Scopus, BIOSIS Previews, ISI Science Citation Index Expanded, and the Cochrane Central Register of Controlled Trials from date of inception through August 2017 for studies reporting pregnancy with kidney transplant.

Results

Of 1343 unique studies, 87 met inclusion criteria, representing 6712 pregnancies in 4174 kidney transplant recipients. Mean maternal age was 29.6 ± 2.4 years. The live-birth rate was 72.9% (95% CI, 70.0–75.6). The rate of other pregnancy outcomes was as follows: induced abortions (12.4%; 95% CI, 10.4–14.7), miscarriages (15.4%; 95% CI, 13.8–17.2), stillbirths (5.1%; 95% CI, 4.0–6.5), ectopic pregnancies (2.4%; 95% CI, 1.5–3.7), preeclampsia (21.5%; 95% CI, 18.5–24.9), gestational diabetes (5.7%; 95% CI, 3.7–8.9), pregnancy induced hypertension (24.1%; 95% CI, 18.1–31.5), cesarean section (62.6, 95% CI 57.6–67.3), and preterm delivery was 43.1% (95% CI, 38.7–47.6). Mean gestational age was 34.9 weeks, and mean birth weight was 2470 g. The 2–3-year interval following kidney transplant had higher neonatal mortality, and lower rates of live births as compared to > 3 year, and < 2-year interval. The rate of spontaneous abortion was higher in women with mean maternal age < 25 years and > 35 years as compared to women aged 25–34 years.

Conclusion

Although the outcome of live births is favorable, the risks of maternal and fetal complications are high in kidney transplant recipients and should be considered in patient counseling and clinical decision making.
Hinweise

Electronic supplementary material

The online version of this article (https://​doi.​org/​10.​1186/​s12882-019-1213-5) contains supplementary material, which is available to authorized users.
Abkürzungen
CI
Confidence interval
US
United States

Background

Women with end stage renal disease have impaired fertility due to disruption of hypothalamic gonadal axis. Pregnancy is therefore rare in women on dialysis with very low incidence of conception ranging from 0.9 to 7% [1]. Since there is rapid restoration of fertility, in some cases, within 6 months following transplantation, kidney transplantation offers the best hope to women with end-stage renal disease who wish to become pregnant [2].
Pregnancy in a kidney transplant recipient continues to remain challenging due to risk of adverse maternal complications of preeclampsia and hypertension, and risk of adverse fetal outcomes of premature birth, low birth weight, and small for gestational age infants [3]. Additionally, there is risk of side effects from immunosuppressive medication, and risk of deterioration of allograft function [4]. Therefore, preconception counseling, family planning and contraception are pertinent parts of the transplant counseling process.
Data on clinical outcomes of pregnancy in kidney transplant recipients is limited from case reports, single-center studies, and voluntary registries. The usefulness of the voluntary registries is further limited due to underreporting and incomplete data capture [58]. To the best of our knowledge, no comprehensive metanalysis on post-kidney transplant pregnancy outcomes has been performed in the recent years [9]. Since kidney transplant is common in women of child bearing age and most of the data on outcomes of pregnancy comes from these retrospective studies, our metaanalysis is both timely and important. The comprehensive analysis of various worldwide registries, single-center studies, and case series will provide generalizable inferences about post-kidney transplant pregnancy outcomes, and help guide the pregnancy in kidney transplant recipients. The primary goal of this study was to perform a meta-analysis to systematically identify all studies of pregnancy-related outcomes in kidney transplant recipients from all around the world, and estimate pooled incidences of pregnancy outcomes, maternal complications, and fetal complications. The secondary goals were to examine the impact of pregnancy on the kidney allograft loss, allograft rejection, identify ideal maternal age of conception, and determine ideal time of conception between kidney transplant and pregnancy.

Methods

Data sources and searches

We performed a systematic review and meta-analyses reported according to PRISMA guidelines for studies exploring incidence and outcomes of pregnancy in women with kidney transplant (Fig. 1). We searched PubMed/MEDLINE, Elsevier EMBASE, Scopus, BIOSIS Previews, ISI Science Citation Index Expanded, and the Cochrane Central Register of Controlled Trials (CENTRAL) from their earliest date of inception through 8/31/2017, and abstracts from the annual American Transplant Congresses from 1/1/2013 through 8/31/2017. A health sciences librarian (E.K.) developed database-specific search strategies including a combination of subject headings (MeSH or Emtree) and keywords. The following key search terms were used in strategies specific to each database and organization: pregnancy complications, pregnancy outcome, maternal outcome, fetal outcome, birth outcome, kidney transplant, or renal transplant. A reproducible PubMed search strategy is provided in Additional file 1.

Study selection

We considered observational studies (prospective cohort, retrospective cohort, and cross-sectional), case series, and case reports (with n > 10 pregnancies) that explored the pregnancy, maternal, and fetal outcomes among women ≥18 years, and who received a kidney transplant. Studies of patients with multiple organ transplants, studies that analyzed the teratogenic effects of mycophenolate or sirolimus, and non–English language studies were excluded. Titles and abstracts of all identified citations were screened independently by two reviewers (S.S. and T.G.), who discarded studies that did not meet all inclusion criteria. The same reviewers independently screened the abstracts of all eligible studies. If eligibility was indeterminable from the abstract, the study was included in the full-text screen. All disagreements were adjudicated by the principal investigator (S.S).

Data extraction, quality assessment, and outcomes

Data extraction was carried out independently by three data extraction team members (A.G, L.R. and M.S.) using standard data extraction forms. Data elements were then rechecked for accuracy by all the three data extraction team members. When more than one publication of a similar patient population existed with more than 25% overlap, publication with higher number of pregnancy events and the most complete details was included. Disagreements in data extraction and quality assessment were resolved in consultation with an arbitrator (T.G.) and primary investigator (S.S.). For each included study, the following data was extracted: country of location, years of data collection, number of kidney transplant recipients, number of pregnancies, mean maternal age, mean interval between kidney transplant and pregnancy, pregnancy outcomes (number of live births, miscarriage, induced abortion, still birth and ectopic pregnancies), maternal outcomes (number of women with preeclampsia, pregnancy induced hypertension, and gestational diabetes mellitus, and number of cesarean sections), fetal outcomes (number of pre-term births, mean gestational age, mean gestational weight, and number of neonatal deaths); and graft outcomes (number of acute rejection during pregnancy, graft failure post pregnancy, mean serum creatinine pre and post pregnancy). To maintain consistency across extracted data, the number of pregnancies was used as a denominator for the outcomes of live births, miscarriages, induced abortions, stillbirths, neonatal deaths, preeclampsia, pregnancy induced hypertension, and gestational diabetes mellitus. The number of live births was used as the denominator for the outcome of preterm deliveries, and cesarean section. Preterm was defined as babies born alive before 37 weeks gestation.

Data synthesis and analysis

Patients characteristics were reported as frequencies. The pregnancy incidence was reported for women per 1000 live births. For each study, estimates were expressed as prevalence and 95% confidence intervals (CI). Prevalence estimates from individual studies were pooled using a random-effects model. Heterogeneity across included studies was analyzed formally using Cochran Q (heterogeneity 2) and I2 statistics. For binary outcomes, the DerSimonian-Laird method was used, and for continuous outcomes, a weighted average methodology was used to calculate the pooled estimates and 95% CI. Two-sample test of proportions was used to compare the pooled incidence for each analysis to the most recent United States (US) general population incidence. [1014] We determined the associations of maternal age, the interval between kidney transplant, and the pregnancy outcomes. Additonally, we performed a subgroup analysis for the pregnancy, maternal and fetal outcomes for studies published from 2000 to 2017. Analyses were performed using MS Excel and Comprehensive Meta-analysis packages in R software.

Results

Among the 4134 citations that were retrieved, 136 full-text articles were reviewed and 87 were selected to be included in the final study cohort (Fig. 1). Three studies were from Africa, 31 from Asia, 31 from Europe, 10 from North America, 4 from Oceania, and 8 from South America (Table 1). Overall, there were 6712 pregnancies in 4174 kidney transplant recipients. Mean maternal age was 29.6 ± 2.4 years and mean interval between kidney transplant and pregnancy was 3.7 years.
Table 1
Studies included in the metaanalysis
 
Reference, Year Published
Study Years
Country
Recipients
Pregnancies
1
Devresse et al., 2017 [32]
1994–2010
Belgium
32
57
2
Yuksel et al., 2017 [33]
2009–2016
Turkey
25
na
3
Ajaimy et al., 2016 [34]
2009–2014
USA
11
11
4
Candido et al., 2016 [35]
2004–2014
Portugal
36
53
5
Cristelli et al., 2016 [36]
2004–2014
Brazil
36
53
6
El Houssni et al., 2016 [37]
na
Saudi Arabia
12
21
7
Lima et al., 2016 [38]
2004–2014
Brazil
36
53
8
Majak et al., 2016 [39]
1969–2013
Norway
na
119
9
Mishra et al., 2016 [40]
2004–2014
India
16
na
10
Orihuela et al., 2016 [41]
1986–2014
Uruguay
32
40
11
Piccoli et al., 2016 [42]
1978–2013
Italy
na
189
12
Saliem et al., 2016 [43]
2006–2011
Canada
na
264
13
Santos et al., 2016 [44]
2010–2014
Portugal
8
8
14
Sarween et al., 2016 [45]
2001–2015
UK
387
569
15
Stoumpos et al., 2016 [46]
1973–2013
UK
89
138
16
Yoshikawa et al., 2016 [47]
na
Japan
49
65
17
Aktrurk et al., 2015 [48]
2004–2014
Turkey
12
16
18
Arab et al., 2015 [49]
2003–2010
Canada
na
375
19
Erman et al., 2015 [50]
1987–2011
Turkey
43
43
20
Yeon et al., 2015 [51]
1995–2015
Korea
84
119
21
Debska – Slizien et al., 2014 [52]
1980–2012
Poland
17
22
22
Farr et al., 2014 [53]
1999–2013
Austria
12
12
23
Hebral et al., 2014 [54]
1969–2011
France
46
61
24
You et al., 2014 [55]
1995–2013
Korea
29
41
25
Blume et al., 2013 [56]
1988–2010
Germany
34
53
26
Guella et al., 2013 [57]
1992–2008
Saudi Arabia
15
33
27
Pietrzak et al., 2013 [58]
2001–2012
Poland
34
40
28
Rachdi et al., 2013 [59]
2003–2013
Tunisia
12
17
29
Ribeiro et al., 2013 [60]
1995–2007
Brazil
22
31
30
Rocha et al., 2013 [61]
1983–2009
Portugal
24
25
31
Wyld et al., 2013 [62]
1971–2010
Australia
447
692
32
Kennedy et al., 2012 [63]
na
Ireland
18
29
33
Neyatani et al., 2012 [64]
1975–2011
Japan
22
34
34
Van Buren et al., 2012 [65]
1971–2010
Netherlands
30
42
35
Celik et al., 2011 [66]
1998–2008
Turkey
24
31
36
Gerlei et al., 2011 [67]
1974–2010
Hungary
23
27
37
Lopez et al., 2011 [68]
1986–2010
Spain
20
24
38
Xu et al., 2011 [69]
1989–2008
China
25
38
39
Gorgulu et al., 2010 [70]
1983–2008
Turkey
19
22
40
Areia et al., 2009 [71]
1989–2007
Portugal
28
34
41
Gill et al., 2009 [20]
1990–2003
USA
483
530
42
Levidiotis et al., 2009 [8]
1966–2005
Australia
381
577
43
Rizvi et al., 2009 [72]
1985–2008
Pakistan
45
72
44
Sharma et al., 2009 [73]
1988–2006
Oman
42
82
45
Al Duraihimh et al., 2008 [74]
1996–2006
Middle East
140
234
46
Alfi A Yet al, 2008 [75]
1989–2005
Saudi Arabia
12
20
47
Cruz Lemini et al., 2007 [28]
1990–2005
Mexico
60
75
48
Oliveira et al., 2007 [76]
2001–2005
Brazil
52
52
49
Sibanda et al., 2007 [77]
1994–2001
UK
176
193
50
Yassaee et al., 2007 [78]
1996–2001
Iran
74
95
51
Kurata et al., 2006 [79]
1984–2003
Japan
42
53
52
Rahamimov et al., 2006 [80]
1983–1998
Israel
39
69
53
Galdo et al., 2005 [81]
1982–2002
Chile
30
37
54
Garcia - Donaire et al., 2005 [82]
1997–2004
Spain
16
19
55
Ghanem et al., 2005 [83]
1989–2004
Egypt
41
67
56
Pour-Reza-Gholi et al., 2005 [84]
1984–2004
Iran
60
74
57
Yildirim et al., 2005 [85]
1998–2005
Turkey
17
20
58
Keitel et al., 2004 [86]
1977–2001
Brazil
41
44
59
Pezeshki et al., 2004 [87]
1991–1998
Iran
18
20
60
Hooi et al., 2003 [88]
1984–2001
Malaysia
46
72
61
Queipo et al., 2003 [89]
1980–2000
Spain
29
40
62
Thompson et al., 2003 [90]
1976–2001
UK
24
48
63
Sgro et a,l 2002 [91]
1988–1998
Canada
26
44
64
Tan et al., 2002 [92]
1986–2000
Singapore
25
42
65
Park et al., 2001 [93]
na - 2000
South Korea
36
47
66
Kuvacic et al., 2000 [94]
1986–1996
Croatia
15
23
67
Little et al., 2000 [27]
1985–1998
Ireland
19
29
68
Moon et al., 2000 [95]
na - 1998
Korea
36
48
69
Ventura et al., 2000 [96]
1983–1999
Portugal
15
15
70
Arsan et al., 1997 [97]
na
France
20
33
71
Rahbar et al., 1997 [98]
1985–1993
Iran
13
14
72
Rieu et al., 1997 [99]
1970–1995
France
22
33
73
Al Hassani et al., 1995 [100]
1985–1993
Oman
25
44
74
Sabagh et al., 1995 [101]
1984–1994
Saudi Arabia
33
52
75
Saber et al., 1995 [102]
1968–1992
Brazil
19
25
76
Wong et al., 1995 [103]
1972–1992
New Zealand
9
16
77
Hadi et al., 1986 [104]
1969–1992
South Korea
11
13
78
Talaat et al., 1994 [105]
1977–1992
Sweden
19
25
79
Pahl et al., 1993 [106]
1969–1990
USA
21
32
80
Muirhead et al., 1992 [107]
1977–1988
UK
22
22
81
Brown et al., 1991 [108]
1965–1989
Ireland
14
27
82
Sturgiss et al., 1991 [109]
1967–1987
UK
17
22
83
O’ Connell et al., 1989 [110]
1974–1986
Australia
11
18
84
Ha et al., 1994 [111]
1970–1982
USA
13
17
85
Marushak et al., 1986 [112]
1972–1983
Denmark
20
24
86
O’ Donnell et al., 1985 [113]
1971–1984
South Africa
21
38
87
Waltzer et al., 1980 [114]
na
USA
12
15
na not available

Pregnancy outcomes

Live birth rate was 72.9% (95% CI, 70.0–75.6), miscarriages rate was 15.4% (95% CI, 13.8–17.2), induced abortions rate was 12.4% (95% CI, 10.4–14.7), stillbirths rate was 5.1% (95% CI, 4.0–6.5) and rate of ectopic pregnancies was 2.4% (95% CI, 1.5–3.7). In our study cohort of kidney transplant recipients, live birth rates were higher as compared to the US general population (72.9% vs. 62%) and favorable across all geographic regions (Fig. 2) [10, 11]. Overall, miscarriage rate was slightly lower than that of the US general population (15.4% vs. 17.1%), but higher across Africa (21.0%; 95% CI, 14.3–29.9), and South America (20.2%; 95% CI, 15.6–25.7) (Fig. 3) [13]. Induced abortion rate was also lower than the US general population (12.4% vs. 18.6%) [13]. The rate of induced abortion was highest in South America (19.8%; 95% CI, 12.2–30.3), followed by Asia (13.3%; 95% CI, 9.6–18.3), Oceania (11.5%; 95% CI, 9.3–14.0), North America (10.9%; 95% CI, 5.9–19.2), Europe (10.0%; 95% CI, 7.3–13.5), and Africa (7.7, 95% CI, 1.4–32.6) (Fig. 4). Overall, stillbirth rate was higher than the US general population (5.1% vs. 0.6%) [14]. Worldwide, stillbirth rate was highest in Asia (6.6, 95% CI, 4.8–9.0%), and lowest in Africa (2.6, 95% CI; 0.4–16.5) (Fig. 5). The rate of ectopic pregnancy was slightly higher than the US general population (2.4% vs. 1.4%), with highest rate in Asia (3.3, 95% CI; 1.1–9.8) (Fig. 6) [15]. The results from the subgroup analyses (2000–2017) for pregnancy outcomes were consistent with the current findings (Additional file 2).

Maternal outcomes

Overall, rates of preeclampsia was 21.5% (95% CI, 18.5–24.9; US mean, 3.8%), cesarean section was 62.6% (95% CI, 57.6–67.3; US mean, 31.9%), gestational diabetes was 5.7% (95% CI, 3.7–8.9; US mean, 9.2%), and pregnancy induced hypertension was 24.1% (95% CI, 18.1–31.5). [12, 16] Preeclampsia rate was highest in Oceania (27.0%; 95% CI, 23.6–30.8), followed by North America (25.5%; 95% CI, 14.5–40.8), and lowest in Africa (10.5%; 95% CI, 4.0–24.9%) (Fig. 7). Cesarean section rate was highest in South America (88.8%; 95% CI, 49.3–98.5), followed by Africa (77.5%; 95% CI, 6.3–99.4) (Fig. 8). Worldwide, Oceania had the lowest rates of gestational diabetes (1.0%; 95% CI, 0.5–2.3%) (Fig. 9). With regards to pregnancy induced hypertension, highest rate was reported in South America (48.0, 95% CI, 15.1–82.7), while lowest rate was in Africa (16.1, 95% CI, 9–26.9) (Fig. 10). The results from the subgroup analyses (2000–2017) for maternal outcomes were consistent with the current findings (Additional file 2).

Fetal outcomes

Overall, rate of preterm birth was 43.1% (95% CI, 38.7–47.6) defined by babies born alive before 37 weeks of gestation, and neonatal mortality was 3.8% (95% CI, 2.8–5.2). Rates of preterm birth was highest in South America (55.0%), and lowest in North America (35.4%) (Fig. 11). The mean gestational age for newborns was 34.9 weeks (US mean, 38.7 weeks) and the mean birth weight was 2470 g (US mean, 3389 g). [12, 17] Neonatal mortality was high across all geographical regions as compared to the US mean (3.8% vs. 0.4%), with highest rate in Africa (18.4%; 95% CI, 9.1–33.9) and lowest rate in North America (1.3, 95% CI, 0.2–8.9) (Fig. 12) [18]. The results from the subgroup analyses (2000–2017) for fetal outcomes were consistent with the present findings except for neonatal mortality which was slighly lower in the subgroup analysis (2.9% vs. 3.8%) (Additional file 2).

Graft outcomes

The overall acute rejection rate during pregnancy among 822 kidney transplant recipients was 9.4% (95% CI, 6.4–13.7), which was comparable to the US mean of 9.1%. [19] Rates of acute renal allograft rejection were highest in Asia (11.0%), followed by South America (10.7%), Oceania (9.1%), Europe (7.3%), North America (6.7%), and Africa (4.8%) (Fig. 13). With regards to graft failure, there was large variability in the follow up period ranging from 1 year to 14 years. However among 489 recipients in 12 studies where two-year post pregnancy graft loss was reported, there were 32 cases of graft loss (9.2%). The change in preconception creatinine and post-pregnancy creatinine, was statistically significant (1.23 ± 0.16 mg/dl vs. 1.37 ± 0.27 mg/dl, p = 0.007).

Time of conception

Outcomes were also stratified by interval of < 2 years, 2–3 years, and > 3 years between pregnancy and kidney transplant (Table 2). Adverse pregnancy outcomes of induced abortion rates and neonatal deaths were highest in the 2–3 year interval following kidney transplant as compared to < 2 year interval and > 3 year interval (16% vs. 11% vs. 10, and 9% vs. 3% vs. 4% respectively). Cesarean section rate and live birth rate were also less favorable in this interval of 2–3 years than > 3 year, and < 2 year interval (68% vs. 75% vs. 74, and 73% vs. 65% vs. 42% respectively). Maternal complication of preeclampsia was higher in the 2–3 interval, and > 3 year interval than < 2 year interval (24% vs. 23% vs. 13%). Spontaneous abortion rates were highest in > 3 year interval followed by 2–3 interval, and < 2 interval (16% vs. 14% vs. 10%).
Table 2
Pregnancy-related outcomes stratified by study mean interval between transplant and pregnancy
 
< 2 years
> 2–3 years
> 3 years
Number of papers
4
15
44
Number of pregnancies
149
835
3182
Mean maternal age (year)
28.3
29.4
29.1
Pregnancy Outcomes
 Live birth
73.8%
68.3%
75.4%
 Induced abortion
10.7%
16.1%
10.2%
 Spontaneous abortion
10.3%
14.0%
16.3%
 Still birth
6.7%
5.1%
3.7%
 Neonatal deaths
3.4%
9.3%
3.7%
 Cesarean section
41.8%
72.7%
64.5%
Maternal Outcomes
 Preeclampsia
13.2%
24.3%
22.8%
 Pregnancy induced hypertension
12.1%
30.8%
23.0%
 Gestational diabetes
0.0%
8.8%
7.2%
Fetal Outcomes
 Pre-term delivery
41.9%
41.6%
45.4%
 Mean gestation time (weeks)
36.1
34.5
34.9
 Birth weight (grams)
2349.00
2533.21
2460.79
Graft Outcomes
 Acute rejection
8.1%
5.1%
3.0%
 Graft loss
16.7%
14.6%
6.3%

Maternal age for conception

We further stratified the pregnancy, maternal, fetal, and graft outcomes by maternal age categories (Table 3). Lower live birth rate was observed in women with maternal age 29–34 years than those < 29 years (74% vs. 76%). Rates of spontaneous abortion were highest in women < 25 years and > 35 years followed by women with maternal age 25–34 years (20% vs. 18% vs. 11%). Preeclampsia rates were higher in women with maternal age > 35 years (27%) and 29–34 years (26%) followed by < 25 years (17%) and 25–29 years (14%).
Table 3
Pregnancy-related outcomes stratified by study mean maternal age
Study mean maternal age (years)
 
< 25
25–29
30–34
≥35
Number of papers
3
22
35
1
Number of pregnancies
103
723
3474
11
Mean maternal age (year)
23.3
27.4
30.2
36.0
Pregnancy Outcomes
 Live birth
75.8%
75.8%
73.9%
na
 Induced abortion
14.0%
11.3%
11.0%
na
 Spontaneous abortion
19.8%
16.0%
13.3%
18.2%
 Still birth
2.9%
5.3%
3.6%
9.1%
 Neonatal deaths
na
5.4%
3.0%
na
 Cesarean section
48.0%
68.3%
63.6%
na
Maternal Outcomes
 Preeclampsia
17.1%
13.7%
26.5%
27.3%
 Pregnancy induced hypertension
16.5%
25.2%
23.4%
na
 Gestational diabetes
na
5.8%
7.0%
na
Fetal Outcomes
 Pre-term delivery
na
46.4%
47.4%
na
 Mean gestation time (weeks)
35.5
35.5
34.6
na
 Birth weight (grams)
2460.0
2607.7
2456.9
na
Graft Outcomes
 Acute rejection
3.8%
3.3%
5.8%
na
 Graft loss
na
12.1%
10.4%
27.3%
*na not available

Discussion

The results of our meta-analysis show that although majority of pregnancies in women after kidney transplant result in live birth, both maternal and fetal adverse events are common. Rates of preeclampsia, still birth, and cesarean section were significantly higher than in the general population. In the cohort considered for the analysis, a quarter of women had serious pregnancy complications, defined as at least one of preterm delivery, first or second trimester loss, stillbirth, or neonatal death. Additionally, rates of preterm delivery, still births, and neonatal mortality were higher as compared with the US recent national data.
The live birth rates in women after kidney transplant were higher than in the general population (73% vs. 62%) and this trend was consistent throughout the globe [10]. Our study confirms the findings from The National Transplant Pregnancy Registry from the United States that reported a live birth rate of 71–76% [7]. Similarly, meta-analysis done by Deshpande et al. examined pregnancy outcomes of 4706 pregnancies in women with kidney transplant and reported a live birth rate of 73.5% [9]. The higher live birth rate, although appears encouraging, may reflect a reporting bias or a selection bias in which relatively healthy women decided to pursue pregnancy, and subsequently received better medical support by multiple specialties. It is also important to consider that there are inconsistencies in definition of live birth rate used in various studies, for example live birth rate was defined as per 1000 female transplant recipients in some studies, whereas per 1000 pregnancies in transplant recipients in others [7, 20]. Live birth rate in general population (comparison group) is defined by Centers for Disease Control as live births per 1000 population [10]. Additionally, it remains unclear how the multiple gestation pregnancy outcomes were evaluated in these studies. Contrary to the above findings of successful pregnancies, a US health utilization study found a much lower live birth rate of 55% in kidney transplant recipients. They attributed this finding of low live birth rate to underestimation of fetal loss [20]. Davison et al. estimated that just under 40% of conceptions do not go beyond the first trimester, but of those that do, greater than 90% end successfully [21]. Another explanation of high live birth rate in our study could be the exclusion of studies that reported pregnancy outcomes with teratogenic immunosuppressive medications of mycophenolate and sirolimus.
Our study highlights the significantly higher risk of maternal and fetal complications in women with kidney transplants. About a quarter of women developed preeclampsia, and the rates of preeclampsia were almost six fold higher as compared to the general US population (21.5% vs. 3.8%) [16]. Vannevel et al. in an international multicenter retrospective cohort of 52 women who underwent kidney transplantation reported preeclampsia rate of as high as 38%, and chronic hypertension rate of 27% [22]. Hypertension is common in kidney transplant recipients prior to conception with a reported incidence of 52 to 69% [1]. Several factors can contribute to the onset of hypertension after renal transplantation, including but not limited to the type of immunosuppressive therapy (calcineurin inhibitors and corticosteroids), allograft function, donor type, obesity, alcohol, smoking, and presence of a native kidney (increased production of renin) [23]. Diagnosis of superimposed preeclampsia can be difficult in kidney transplant patients due to higher frequency of preexisting hypertension and proteinuria [1, 24].
We found significant differences in rates of gestational diabetes mellitus between various geographical location, for example rates were as high as 8.9% in Europe and as low as 1% in Oceania. Although, the increased rate of gestational diabetes in kidney transplant patients can be well explained by the use of immunosuppressive medications like steroids and calcineurin inhibitors, the striking differences between rates of gestational diabetes according to geographic location also highlights the importance of predisposition to diabetes due to ethnicity. Unfortunately, it was not possible to evaluate the differences in immunosuppressive medications as usually they are individualized to the needs of the patients and transplant center protocol [1, 25].
Rates of stillbirth and neonatal mortality were significantly higher in our study as compared to the general population. While prior studies have not reported higher rates of neonatal mortality and stillbirths in kidney transplant recipients, the current study finding is highly significant. Possible reasons could be prematurity, preeclampsia or presence of other risk factors like hypertension, proteinuria, and serum creatinine of 1.5 mg/dl or higher [2628]. While it was not possible to determine the exact cause for stillbirth or neonatal mortality, this study finding is critical for counselling of women of child bearing age contemplating pregnancy. In our study, the rate of cesarean section was higher than two folds as compared to general population in United States, and varied from 60 to 77% across different geographical locations. Bramham et al. reported that more than three quarters of the deliveries in kidney transplant recipients were by cesarean section, but only 3% were performed for the indication of renal transplant [3]. Vaginal delivery should not be impaired in kidney transplant patients, as the pelvic allograft does not obstruct the birth canal in most patients [1]. This exceptionally higher rates of cesarean sections in kidney transplant recipients can be attributed to fetal and maternal complications, but warrants further study. There was a high rate of premature births in the transplant population in the present study and close to half of the live births were premature deliveries. Prior studies have showed a preterm birth rate of 40–60% in kidney transplant recipients [9, 29]. Fetal complications, suspected renal compromise or preeclampsia are some of the common indications of early iatrogenic delivery. Interestingly, only quarter of preterm deliveries in renal transplant recipients are induced [3, 7].
The optimal time to conception after renal transplant continues to remain an area of contention. The ideal time of conception in women with renal transplant is between 1 and 2 years after transplantation according to guidelines by American Society of Transplantation, whereas European best practice guidelines recommend delaying pregnancy for a period of 2 years after transplantation [30, 31]. In our study, live birth rate was lowest and neonatal deaths were highest in the 2–3 year interval following kidney transplant. Maternal complication of cesarean section and preeclampsia were higher in the 2–3 and > 3 year interval. In contrast, Deshpande et al. reported both the highest maternal complications of preeclampsia, cesarean section, and gestational diabetes, and least favorable delivery outcome of preterm births in the < 2 year interval as compared to > 2 year interval between kidney transplant and pregnancy [9]. However their analysis was limited by inclusion of only 3 studies in the < 2 interval following kidney transplant. Overall, fetal outcomes in < 2 year interval seem most favorable in our study but merits further investigation due to limitation of the retrospective study design, small numbers, and possible reporting bias associated with data from voluntary registries.
A significant strength of our study is that it involves a large number of pregnant renal transplant recepients from all around the globe, thus providing us with information about pregnancy outcomes for a heterogenous population. Additionally, we have analyzed region specific outcomes and identified outcomes which may require intensive management pertaining to that region. This will help in making future region specific guidelines for follow up and management of pregnancy in kidney transplant recpients. The following limitations should be considered when interpreting the findings of our study. We examined pregnancy outcomes over several decades in the present study. While it is expected for the outcomes to change due to improvement in obstetric care in kidney transplant recipients over the course of time, subgroup analysis for studies from 2000 to 2017 showed consistent results. There were inconsistencies in the definition of live birth rate amongst different studies that may have affected the results. Reporting bias may have affected the miscarriage rate. We were unable to account for differences in socioeconomics, and healthcare conditions among the different geographic regions. Due to lack of individual patient data, we were not able to assess pregnancy outcomes in relation to immunosuppression regimens.

Conclusions

This meta analysis of pregnancy outcomes in 6712 pregnancies in 4174 kidney transplant recipients with data spread over different decades from all over the world shows favorable outcomes with live birth rates exceeding that in the recent national population. Majority of patients preserve their graft. However, pregnancy after renal transplant confers significant risk in terms of maternal and fetal adverse events, including increased rates of preeclampsia, gestational diabetes, cesarean section rates, and pregnancy induced hypertension. The risk of prematurity and low birth rate are also high. Areas which need to be studied in the future include type of immunosuppression and its correlation with specific pregnancy outcomes; and evaluation of risk factors associated with specific maternal and fetal adverse events. The definitions used in evaluating these outcomes also need to be standardized. The results of this study can help the health care providers with appropriate counseling and individualized management of this high risk population.

Acknowledgements

None.

Author contributions

SS initiated the study, designed the study and wrote the initial manuscript. RV, Ayank Gupta, RJ and MS contributed to the study design, and study figures, analyzed and interpreted the data, and did the manuscript review. JW contributed to the sudy design, data analysis, interpretation of data, and manuscript review. EK contibuted to literature search, and manuscript review. TK contributed in study design and manuscript review. Anu Gupta contributed in manuscript writing and manuscript review. TG contributed to the study design, implementation of the study, study figures, and manuscript review. PV assisted SS with study design and implementation, revision of the manuscript and did the final approval of the manuscript. All authors reviewed the manuscript.

Funding

This work was supported by grant awarded to SS from University of Cincinnati’s College of Medicine-Health Sciences Library.

Availability of data and materials

The datasets used and/or analysed during the current study are available from the corresponding author on reasonable request.
Not applicable.
Not applicable.

Competing interests

All the authors have no disclosures and competing interests. The results presented in this paper have not been published previously in whole or part, except in abstract format.

Publisher’s Note

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Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://​creativecommons.​org/​licenses/​by/​4.​0/​), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://​creativecommons.​org/​publicdomain/​zero/​1.​0/​) applies to the data made available in this article, unless otherwise stated.
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Metadaten
Titel
Pregnancy outcomes in women with kidney transplant: Metaanalysis and systematic review
verfasst von
Silvi Shah
Renganathan Lalgudi Venkatesan
Ayank Gupta
Maitrik K. Sanghavi
Jeffrey Welge
Richard Johansen
Emily B. Kean
Taranpreet Kaur
Anu Gupta
Tiffany J. Grant
Prasoon Verma
Publikationsdatum
01.12.2019
Verlag
BioMed Central
Erschienen in
BMC Nephrology / Ausgabe 1/2019
Elektronische ISSN: 1471-2369
DOI
https://doi.org/10.1186/s12882-019-1213-5

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