Pena–Shokeir syndrome: current management strategies and palliative care

Abstract

Pena–Shokeir syndrome (PSS) type 1, also known as fetal akinesia deformation sequence, is a rare genetic syndrome that almost always results in intrauterine or early neonatal death. It is characterized by markedly decreased fetal movements, intrauterine growth restriction, joint contractures, short umbilical cord, and features of pulmonary hypoplasia. Antenatal diagnosis can be difficult. Ultrasound features are varied and may overlap with those of Trisomy 18. The poor prognosis of PSS is due to pulmonary hypoplasia, which is an important feature that distinguishes PSS from arthrogryposis multiplex congenital without pulmonary hypoplasia, which has a better prognosis. If diagnosed in the antenatal period, a late termination of pregnancy can be considered following ethical discussion (if the law allows). In most cases, a diagnosis is only made in the neonatal period. Parents of a baby affected with PSS require detailed counseling that includes information on the imprecise recurrence risks and a plan for subsequent pregnancies.

Keywords:

• fetal akinesia deformation sequence
• ultrasound
• comfort care

Introduction

Pena–Shokeir syndrome (PSS) is a lethal form of multiple congenital contractures with autosomal recessive inheritance implicated in 50% of cases.¹ However, heterogeneity makes recurrence risk calculations difficult.

Two types of PSS have been described:

• Type 1: It is a fetal akinesia/hypokinesia sequence that is characterized by multiple joint contractures, facial anomalies, and pulmonary hypoplasia. It has a prevalence of <1/1,000,000 births, with an autosomal recessive mode of inheritance.² About 100 cases have been described in the literature, with about 30% of fetuses dying in utero, and the vast majority of neonates succumbing in the early neonatal period due to pulmonary hypoplasia.

• Type 2: It is also known as cerebro-oculo-facio-skeletal (COFS) syndrome. It is a rapidly progressive neurological disorder resulting in brain atrophy, characterized by intracerebral calcifications, cataracts, microcornea, optic atrophy, progressive joint contractures, and growth failure. It is a very rare autosomal recessive disorder caused by mutations in ERCC6/CSB, although mutations in ERCC1, ERCC2, and ERCC5 have been linked to some cases. Death usually occurs by 5 years of age.³

Further discussion in this review will be restricted to PSS type 1.

Pathogenesis

PSS is a heterogeneous group of disorders characterized by a decrease or absence of intrauterine fetal movement. It is also called “fetal akinesia deformation sequence” (FADS). Arthrogryposis multiplex congenital (AMC), multiple pterygium syndrome (MPS), and lethal congenital contracture syndromes are conditions that have overlapping phenotypes and etiologies. The clinical phenotype initially described by Pena and Shokeir (1974, 1976) included camptodactyly; multiple contractures; facial anomalies consisting of a high nasal bridge, micrognathia, and a cleft palate; and pulmonary hypoplasia resulting in death in utero or shortly thereafter.^4,5 The initial description included multiple consanguineous families, and an autosomal recessive inheritance pattern was suggested. Sporadic and familial occurrences have been described subsequently depending on the underlying etiology. This has led to the identification of up to 30 different subgroups.^6,7 X-linked dominant inheritance has also been suggested.^8,9

The underlying etiology is dysfunction of the neuromuscular system resulting in decreased intrauterine fetal movements. It includes the brain and spinal cord, motor neuron, neuromuscular junction, and neurotransmitter defects.⁶ Muscle myopathic changes leading to the failure of development of normal mature muscle, including dystrophies and dysplasias, have also been implicated.⁷ Other causes include connective tissue abnormalities such as chondrodysplasias, conditions associated with joint limitation and laxity, as well as restricted skin (restrictive dermopathy).⁷ Environmental causes include antibodies to neurotransmitters and fetal acetylcholine receptor (AChR), as well as reduced intrauterine space such as that seen in multiple births, oligohydramnios, and uterine abnormalities. The earlier the effect, the more severe the phenotype. Maternal illness and drug use, as well as fetal ischemia, have also been described in isolated cases.⁶

A possible relation to maternal myasthenia gravis was described in 1994. Maternal anti-AChR antibody titers were increased in the absence of any clinical symptoms of myasthenia gravis in the mothers. In these cases, the recurrence risk was very high and all subsequent pregnancies were affected.^10,11 Other case reports have confirmed this and have suggested that the antibodies were different from those usually associated with myasthenia gravis. Adult anti-AChR antibodies replace fetal anti-AChR by 33 weeks of gestation. This explains why the fetus is markedly affected compared with their mothers.^10,12

Genetics

Advances in molecular genetic research have improved our knowledge of the genetic causes of PSS and suggest that many cases are at the severe end of the spectrum of other recognized conditions involving the neuromuscular system. Alternatively, autosomal dominant neuromuscular conditions can present with PSS when the gene defect is in the homozygous state.⁷

Variations in the genes involved in the neuromuscular pathways for fetal movement cause PSS. Variations in RAPSN (Online Mendelian Inheritance in Man [OMIM] 601592), DOK7 (OMIM 610285), and MUSK (OMIM 601296) are also implicated in congenital myasthenic syndrome (CMS), but have been identified as some of the major genes involved in the etiology of PSS through deficient interaction in the neuromuscular junction.

RAPSN

RASPN is located on chromosome 11p11.2. It codes for a postsynaptic protein (rapsyn) that links the AChR to the agrin-binding dystrophin-associated glycoprotein complex and stabilizes the AChR at the neuromuscular junction.¹³ Homozygosity or compound heterozygosity for mutations results in AChR deficiency and FADS or CMS. Michalk et al reported the case of a brother and a sister in a non-consanguineous Pakistani family.¹⁴ Both siblings were born with severe respiratory problems, contractures, and subtle dysmorphisms. The male infant died at 10 months due to respiratory failure. He also had cryptorchidism. The female infant had a cleft palate but was still alive at 10 months. They both had compound heterozygous mutations of c.416T→C/c.566C→T. Vogt et al reported a homozygous mutation of c.1177_1178delAA in a consanguineous family (monozygotic twin males and a female).¹⁵ All the affected fetuses were terminated and showed FADS upon examination after delivery. A homozygous c.484G>A (p.Glu162Lys) variant was identified by Winters et al in consanguineous parents in their fifth pregnancy. Their fourth pregnancy was also affected, but they refused testing during the previous pregnancy.¹⁶

DOK7

DOK7 is involved in AChR clustering in synaptogenesis and binds with and phosphorylates MUSK. It is located at 4p16.3. In a consanguineous family with three affected children, Vogt et al identified a homozygous splice-site mutation (IVS3+1G>T or c.331+1G>T) in DOK7 causing lethal FADS.¹⁷ DOK7 variations are usually associated with CMS and with limb girdle weakness.¹⁸ This model illustrates that a partial loss of DOK7 function causes CMS but a complete loss of DOK7 function causes a lethal FADS phenotype.

MUSK

MUSK is located at 9q31.3. It forms and maintains the neuromuscular junction. Muscle cells produce and express AChR. Agrin, a proteoglycan released by motor nerves, binds to LRP4 and activates MUSK, which then signals via DOK7 and RAPSN to stabilize the AChR.¹⁹ Wilbe et al reported that a complete loss of MUSK causes autosomal recessive FADS.²⁰ A homozygous frameshift mutation (c.40dupA) in exon 1 leading to a premature stop codon was found in a non-consanguineous Swedish family with five affected fetuses. The mutation was identified through whole-exome sequencing followed by Sanger sequencing. In the same year, Tan-Sindhunata et al identified a homozygous Dutch family with FADS.²¹

Other variations in the genes involved in the neuromuscular pathways for fetal movement can cause PSS. There are, however, a large percentage of unknown cases. Next-generation sequencing (NGS) technologies will improve the diagnosis and enable accurate prognosis prediction, recurrence risk estimation, as well as genetic counseling. NGS panels are being developed to investigate heterogeneous conditions such as PSS where variants in different genes are causative. Whole-exome sequencing earlier in the diagnostic process will be a useful tool to identify new genes not previously described.

Details on the anatomical areas involved, genes (Mendelian Inheritance in Man [MIM] number), inheritance pattern, phenotype (MIM number), and references of all known gene variations associated with FADS are given in Table 1.

Table 1 Summary of the genetic causes of Pena–Shokeir phenotype

Anatomical localization	Gene (MIM number)	Gene action	Inheritance pattern	Phenotype	Reference
Brain	TUBB2B (612850)	Beta form of tubulin – major component of microtubules	AD	FADS with MLE	Laquerriere et al (2016)^Citation22
Motor neuron/spinal cord	SMN1 (600354)/SMN2 (601627)	Survival motor neuron protein (SMN1 and 2)	AR	Type 0 SMA	Grotto et al (2016)^Citation23 Devriendt et al (1996)^Citation24
	ERBB3 (190151)	Epidermal growth factor receptor 3	AR	LCCS2	Narkis et al (2004,^Citation25 2007^Citation26)
	GLE1 (603371) – not always lethal	Defective mRNA processing with tissue-specific dysregulation of gene expression causing motor neuron disease	AR	AMC – LCCS1 (253310) and LAAHD (611890) AAHD	Kalampokas et al (2012)^Citation27 Nousiainen et al (2008)^Citation28 Smith et al (2017)^Citation29 Hurt and Silver (2008)^Citation30 Said et al (2017)^Citation31
	PIP5K1C (606102)	Production of phosphatidylinositol- 4,5-biphosphate	AR	LCCS3	Narkis et al (2007)^Citation32
	UBE1 (314370)	Ubiquitin-activating enzyme 1	X-linked	X-L SMA	Ramser et al (2008)^Citation33
Peripheral nerves	EGR2 (129010) MPZ (159440)	Early growth response Myelin protein zero gene		CHN	Warner et al (1998)^Citation34 Warner et al (1996)^Citation35
Neuromuscular junction (embryonal AChR)	CHRNA1 (601592)	AChR α-subunit	AR	LMPS, FADS	Vogt et al (2008)^Citation15 Michalk et al (2008)^Citation14
	CHRNB1 (100710)	AChR β-subunit	AR	LMPS, FADS	Michalk et al (2008)^Citation14
	CHRND (100720)	AChR δ-subunit	AR	LMPS, FADS	Michalk et al (2008)^Citation14
	CHRNG (100730)	AChR γ-subunit	AR	LMPS, AR escobar syndrome, FADS	Morgan et al (2006)^Citation36 vogt et al (2012)^Citation37 Hoffman et al (2006)^Citation38
	RAPSN (601592)	Clustering and anchoring AChR in the postsynaptic membrane of the NMJ	AR	CMS, FADS	Vogt et al (2008)^Citation15 Winters et al (2017)^Citation16
	CNTN1 (600016)	Contactin 1 – NMJ adhesion	AR	FADS, Compton–North congenital myopathy	Compton et al (2008)^Citation39
	DOK7 (610285)	Synaptogenesis through interaction with MUSK	AR	FADS/CMS, familial limb- girdle myasthenia	Vogt et al (2009)^Citation17
	SYNE1 (608441)	Synaptic nuclear envelope protein-1	AR	FADS, myogenic AMC	Attali et al (2009)^Citation40
	ECEL1 (605896)	Endothelin-converting enzyme- like 1	AR	AMC/DA type 5	Dohrn et al (2015)^Citation41
Fetal myostructural proteins	MYH3 (160270)	Myosin heavy chain, embryonic	AD	DA2A, DA2B	Toydemir et al (2006)^Citation42
	MYH8 (160741)	Myosin heavy chain, perinatal	AD	TPS (DA7)	Veugelers et al (2004)^Citation43 Toydemir et al (2006)^Citation44
	MYBPC1 (160794)	Myosin-binding protein C1, skeletal muscle slow type	AD/AR	DA1/LCCS type 4	Gurnett et al (2010)^Citation45
Adult skeletal muscle	NEB (161650)	Sarcomere protein – nebulin	AR	NM/FADS/LMPS	Abdalla et al (2017)^Citation46 Lehtokari et al (2014)^Citation47 Todd et al (2015)^Citation48 Feingold-Zadok et al (2017)^Citation49 Ahmed et al (2018)^Citation50
	RYR1 (180901)	Ryanodine receptor-1	AR, AD	FADS/LMPS/ CCD	McKie et al (2014)^Citation51 Michalk et al (2008)^Citation14 Romero et al (2003)^Citation52
	ACTA1 (102610)	Actin 1, skeletal muscle alpha	AD	NM/FADS	Schroder et al (2004)^Citation53 Ahmed et al (2018)^Citation50
	BICD2 (609797)	Dynein-mediated transport	AD	SMALED	Ahmed et al (2018)^Citation50
	MYOD1 (159970)	MyoD/Myf-5 – myogenic factor	AR	FADS	Watson et al (2016)^Citation54
	DMPK (605377)	Dystrophia myotonica protein kinase	AD	FADS	Winters et al (2017)^Citation16
	MUSK (601296)	Muscle-specific tyrosine kinase	AR	FADS/CMS	Wilbe et al (2015)^Citation20 Tan-Sindhunata et al (2015)^Citation21
	KLHL40 (615340)	Kelch-like 40	AR	NM/FADS	Chen et al (2016)^Citation55
	BIN1 (601248)	Amphiphysin 2	AR	CNM	Nicot et al (2007)^Citation56
	DMPK (160900)	Dystrophia myotonica protein kinase	AD	MD/FADS	Lidang Jensen et al (1995)^Citation57
	FKRP (606596)	Fukutin-related protein	AR	Walker–Warburg syndrome/FADS	Van Reeuwijk et al (2010)^Citation58
	MTM1 (300415)	Myotubularin	X-linked	MTM	Winters et al (2017)^Citation16
	TPM2 (190990)	Tropomyosin 2	AR/AD	MPS escobar variant, DA type 1/2B	Winters et al (2017)^Citation16
	TNNI2 (191042)	Troponin 1 – fast twitch skeletal muscle	AD	DA type 1, DA type 2B	Winters et al (2017)^Citation16
	TNNT3 (600692)	Troponin 3 – fast skeletal muscle	AD	DA type 1, DA type 2B	Winters et al (2017)^Citation16
Chanelopathy	SCN4A (603967)	Sodium channel, voltage-gated type iv, alpha	AR	FADS/CM	Winters et al (2017)^Citation16
	NALCN (611549)	Sodium leak channel, nonselective	AD	CLIFAHDD	Winters et al (2017)^Citation16
Neurometabolic disorders	GBE1 (607839)	Glycogen branching enzyme	AR	GSD iv/FADS	Ravenscroft et al (2013)^Citation59
	PDHA1 (300502)	Pyruvate dehydrogenase alpha-1	X-linked	X-D PDHA/FADS	Winters et al (2017)^Citation16
	DPAGT1 (191350)	Dolichyl-phosphate N-acetylglucosamine phosphotransferase 1	AR	CDG 1J	Ganetzky et al (2015)^Citation60
Immunological causes	FOXP3 (300292)	Forkhead box P3 protein	X-linked	IPEX/FADS	Rae et al (2015)^Citation61
Connective tissue	LMNA (150330)	Lamin A and Lamin C	AR	RD	Smigiel et al (2010)^Citation62
	ZMPSTE24 (606480)	Zinc metalloproteinase involved in the processing of farnesylated proteins	AR	RD	Smigiel et al (2010)^Citation62
Other	FGFR2 (176943)	Fibroblast growth factor receptor 2	AD	Pfeiffer syndrome/LMPS	Baynam et al (2008)^Citation63

Abbreviations: MIM, Mendelian inheritance in Man; AD, autosomal dominant; FADS, fetal akinesia deformation sequence; MLE, microlissencephaly; AR, autosomal recessive; SMA, spinal muscular atrophy; LCCS, lethal congenital contracture syndrome; AMC, arthrogryposis multiplex congenital; LAAHD, lethal arthrogryposis with anterior horn cell disease; AAHD, arthrogryposis with anterior horn cell disease; X-L SMA, X-linked spinal muscular atrophy (301830); CHN, congenital hypomyelination neuropathy; AChR, acetylcholine receptor; LMPS, lethal multiple pterygium syndrome; NMJ, neuromuscular junction; CMS, congenital myasthenic syndrome; DA, distal arthrogryposis; TPS, trismus-pseudocamptodactyly syndrome; NM, nemalin myopathy; CCD, central core disease; SMALED, autosomal dominant spinal muscular atrophy with lower extremity predominance; CNM, centronuclear myopathy; MD, myotonic dystrophy; MTM, myotubular myopathy; MPS, multiple pterygium syndrome; CM, congenital myopathy; CLIFAHDD, congenital contractures of the limbs and face with hypotonia and developmental delay; GSD, glycogen storage disease; X-D PDHA, X-linked dominant pyruvate dehydrogenase E1-alpha deficiency; CDG IJ, Congenital disorder of glycosylation type Ij; IPEX, immune dysregulation, polyendocrinopathy, enteropathy, X-linked syndrome; RD, rare disease; FADS, fetal akinesia deformation sequence; AMC, arthrogryposis multiplex congenital; DA, distal arthrogryposis.

Antenatal diagnosis

It is not easy to diagnose PSS as it has a variable phenotype and shares many ultrasonographic features with Trisomy 18 and other syndromes (Table 2).⁶

Table 2 Differential diagnosis of conditions with markedly decreased intrauterine fetal movements⁶

• Adenylosuccinate lyase deficiency

• Cerebro-oculo-facial syndrome (Pena–Shokeir type 2)

• Congenital myopathies

• Congenital myasthenia gravis

• Fetal akinesia deformation sequence (Pena–Shokeir type 1)

• Fukuyama muscular dystrophy

• Glycosylation type 1A deficiency

• Infantile Pick’s disease

• Lethal Larsen syndrome

• Lethal pterygium syndrome

• Lissencephaly III

• Maternal antibodies to fetal acetylcholine receptor

• Mucopolysaccharidosis III

• Neu–Laxova syndrome

• Progressive encephalopathy, edema, hypsarrhythmia, optic atrophy syndrome

• Phosphofructokinase deficiency (glycogenosis VII)

• Potter syndrome

• Restrictive dermopathy

• Trisomy 18

○ walker–Warburg syndrome

The presence of pulmonary hypoplasia is helpful in distinguishing PSS from AMC which has a better prognosis. Invasive testing for chromosomal analysis is advised when a diagnosis is suspected. If the karyotype is normal, and other conditions have been excluded, a presumptive diagnosis of PSS can be made.

Antenatal diagnosis of PSS can be made on ultrasound as early as 12 weeks of gestation if decreased intrauterine fetal movements, fetal edema, and fixed limb posturing are observed. Polyhydramnios is invariably present in the latter half of pregnancy, with a proportion of fetuses developing hydrops fetalis, and becoming more prone to death in utero.

Antenatal ultrasonographic features include decreased fetal movements, intrauterine growth restriction, joint contractures, short umbilical cord, and features of pulmonary hypoplasia. Limbs may be in contraction or extension – knees are usually extended and elbows are flexed. Feet may have severe equinovarus or rocker bottom deformity. Facial features include hypertelorism, low-set ears, depressed tip of the nose, and micrognathia. A disproportionately large head in relation to the body is usually described.⁶ Three-dimensional ultrasound and fetal magnetic resonance imaging (MRI) may be considered as an adjunct to fetal imaging.⁶⁴

Obstetric management

The ideal way to convey bad news to a patient remains controversial. Adequate counseling often requires multiple consultations with various health care professionals, including maternal and fetal specialists, geneticists, and neonatologists. The consultation process should include the patient’s partner or family who can assist with the decision-making process, as well as offering emotional support. Counseling should include information on the diagnosis and prognosis (antenatal, intrapartum, postnatal, and long term), and information regarding future pregnancies.^65,66

The fetus diagnosed with PSS has a poor prognosis. Close to term, the obstetric management would usually continue to be supportive, with delivery via cesarean section reserved for obstetric indications. The patient should be counseled that no intrapartum fetal heart rate monitoring to be carried out due to the poor prognosis, and that the neonate will be evaluated after birth by a neonatologist and geneticist. Palliative care following secondary postnatal assessment should be discussed with the patient. Due to the dismal prognosis of PSS, late termination of pregnancy can be offered as a management option in countries/states where it is legal and acceptable.

Postnatal care

PSS must be differentiated from other causes of FADS as the level of care offered after delivery may be dependent on the expected prognosis. If the diagnosis of PSS is made during the antenatal period, the parents may choose to terminate the pregnancy. Alternatively, the patient may opt for comfort care postdelivery or may choose full resuscitative intervention postdelivery. However, not all patients will have an antenatal diagnosis, and decision making regarding lifesaving interventions in the immediate postdelivery period may be difficult.

The postnatal diagnosis of PSS can be made when there is a combination of prenatal-onset growth restriction, multiple ankyloses (elbows, knees, hips, and ankles), typical facial features, and pulmonary hypoplasia.⁶⁷ Additional findings may include camptodactyly, absent palmar creases, rocker bottom feet, talipes equinovarus, cryptorchidism, short neck, small mouth, and a cleft palate.⁶⁷ The craniofacial abnormalities, skeletal abnormalities, and pulmonary hypoplasia are all secondary to decreased or absent fetal movement in utero.^68–70 The differential diagnosis includes Trisomy 18, MPS, and COFS. A normal karyotype, and the absence of pterygia causing flexion contractures, microphthalmia, and microcephaly allow differentiation of PSS from Trisomy 18, MPS, and COFS.^71,72

Despite the poor survival rate, most patients with PSS receive complete resuscitation after delivery and full postnatal care, including antimicrobials, inotropes/vasopressors, and repeated cardiopulmonary resuscitation until death.⁶⁹ There are, however, cases describing redirection of care from life-sustaining treatment (invasive ventilation) to comfort care after discussion with the parents.^72,73

If full resuscitative efforts are agreed upon, the resuscitation team must anticipate that the newborn will have respiratory distress secondary to pulmonary hypoplasia and be prepared for a difficult intubation⁷⁴ due to edema of the head,^75,76 a short neck,⁷⁶ and micrognathia.^75,76 Various airway devices must be available, including a face mask, oral and nasal airways, laryngeal mask airways, and endotracheal tubes with the addition of a fiber optic or video laryngoscope, if possible.²

No specific treatment is available for those with PSS, and management is largely supportive.⁷⁷ A karyotype should be done on all neonates with this phenotype to exclude Trisomy 18 as the two conditions share many common phenotypic features.^73,76,78 For those undergoing continued care, prolonged mechanical ventilation can be expected and a tracheostomy may have to be considered if extubation is not possible.⁷⁴ In addition, pulmonary hypertension may be present and may require treatment with sildenafil or iloprost to decrease the pulmonary pressures.⁷⁴ Echocardiography should be performed to exclude congenital cardiac abnormalities.^79,80

As PSS may be associated with central nervous system abnormalities,^72,77 it is recommended to perform an MRI of the brain and to screen for endocrine abnormalities such as central hypothyroidism.⁷⁴ The presence of cerebral malformations may also increase the risk of seizures, which require anticonvulsive therapy.^69,73,75 These patients may also sustain fractures postnatally as the bones are hypoplastic with decreased calcification.⁷⁸

Enteral feeding is often delayed due to short-gut syndrome^67,70 and intestinal malrotation,⁷⁹ necessitating pro longed parenteral nutrition. In addition, oral feeding may be impossible due to impaired swallowing,⁸⁰ and patients may require the surgical placement of a feeding gastrostomy tube.

Because of the wide array of physical abnormalities, a multidisciplinary approach is appropriate for those patients surviving the neonatal period who may require repeated surgical procedures for various craniofacial and skeletal deformities. Members of the team should include a pediatrician/ neonatologist, occupational therapist, physiotherapist, speech therapist, and surgeons from various disciplines, including pediatric surgery, orthopedic surgery, maxillofacial surgery, and ENT surgery.

Patients with PSS are at an increased risk of malignant hyperthermia and bronchospasm during anesthesia. However, the use of sevoflurane for induction and maintenance, and rocuronium or vecuronium for muscle relaxation has been successful without adverse events reported in many patients.^74,75

Prognosis

Although the ultimate prognosis of PSS is dependent on the underlying cause, this condition has been described as almost uniformly lethal, with 30% of fetuses being stillborn and live-born infants usually dying within the first month of life.^68,72,77 However, survival beyond 12 months of age has been described, indicating that early mortality is not always inevitable. Of interest is a 9-year-old girl who underwent repeated surgical procedures for skeletal deformities⁷⁷ and a 21-year-old pregnant female who underwent cesarean section at 38 weeks of gestation with a normal fetus.⁸¹ Early death is usually a result of primary cerebral malformations⁶⁸ or acute respiratory failure secondary to pulmonary hypoplasia.^68,72 The degree of lung hypoplasia and the ability of the lungs to sustain life are dependent on the timing of onset, with early-onset akinesia associated with severe hypoplasia and demise.⁷⁸ After death, it is essential to request a postmortem as this will help describe the features of this rare condition even further.⁶⁹

Subsequent pregnancies

Patients who have delivered a fetus with PSS should have close fetal surveillance in subsequent pregnancies. This will allow the early recognition of anomalies. However, since the phenotypic condition is derived from heterogeneous causes, the counseling and recurrence risk calculation are imprecise. It has been estimated that the recurrence risk varies between 0% and 25%.⁸²

Author contributions

All authors contributed toward data analysis, drafting and critically revising the paper, gave final approval of the version to be published, and agree to be accountable for all aspects of the work. SA was responsible for the introduction, differential diagnosis, and obstetric management sections, and compiled the final manuscript. EMH was responsible for sections on pathophysiology and genetics. MC was responsible for sections on postnatal care and prognosis.

Disclosure

The authors report no conflicts of interest in this work.