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Revista médica del Hospital General de México

versión On-line ISSN 2524-177Xversión impresa ISSN 0185-1063

Rev. med. Hosp. Gen. Méx. vol.86 no.2 Ciudad de México abr./jun. 2023  Epub 16-Oct-2023

https://doi.org/10.24875/hgmx.22000056 

Clinical cases

Report of a case of liver rupture in preeclampsia and HELLP syndrome

Jésser M. Herrera-Salgado1 

María V. López-Parra1 

Ricardo Malagón-Reyes1 

Luis E. Reyes1 

María de J. Ángeles-Vázquez1 

Rubén Castorena-de Avila1 

Itzel C. Eláceo-Fernández1 

Jesús C. Briones-Garduño1  * 

Hugo Mendieta-Zerón1 

1Obstetric Intensive Care Unit, Hospital Materno Perinatal Mónica Pretelini, Toluca, State of Mexico, Mexico


Abstract

Liver rupture secondary to preeclampsia represents a complication that, if is not recognized early, can be fatal. Its presentation is rare, but very complex to treat, having options that are not clearly protocolized and usually derive from the experience of the surgeon who faces it. We present a case of liver rupture of a patient from Toluca, State of Mexico who was admitted by emergency air transfer with immediate puerperium complicated by severe preeclampsia, postpartum hemorrhage, liver rupture with hemodynamic instability, it was necessary to intervene surgically for a total of seven occasions to control the hemorrhage, as well as pharmacological, medical measures and multiple transfusions; however, she died on the eighteenth day of his hospitalization for septic shock.

Keywords Preeclampsia; HELLP syndrome; Liver rupture

Introduction

Liver rupture can occur due to different etiologies during pregnancy, including tumors, traumatic causes, and secondary rupture due to severe preeclampsia1, cases of rupture without any identifiable pathology are exceptional2. Some cases have been reported where only subcapsular hematoma is present, without total rupture, in which there is a less severe evolution3,4 also, there is cases reported where there is only rupture of the hepatic capsule but complicated with necrosis and fulminant liver failure with subsequent multi-organ deterioration mainly cerebral and pulmonary5. However, its clinical presentation is usually catastrophic6. The frequency of presentation varies from one in 45,000 to one in 250,000 pregnancies complicated by liver rupture7,8. In Mexico, the most numerous case reports were reported by Murillo and Hernández, a series of 79 patients from 1985 to 1999 in which a frequency of one in 128,927 births was documented9. Pathophysiology is usually explained by periportal hemorrhage, intravascular fibrin deposits, which cause sinusoidal obstruction, intrahepatic vascular congestion with increased tissue volume, ischemia, and tension rupture trapped with the hepatic capsule, of complicated preeclampsia with HELLP syndrome10,11.

The treatment described for liver rupture goes from packing12,13, selective hepatectomy14, patch use with omentum15, selective embolization with interventional radiology16, and liver transplantation in extreme cases17 generally, the combination of different techniques is more effective. Prognosis is variable, but usually fatal18 with mortality of 60-70% of reported cases19. Mortality may be higher if severe bleeding develops, shock state with liver necrosis and complications added to acute liver failure and others associated with the clinical phenomenon of preeclampsia20.

Clinical cases

We present the case of a 23-year-old patient, with 4 h of immediate puerperium, send from Texcoco General Hospital, on air ambulance occurred on March 2022.

Anthropometrics: weight 50.0 kg, Size 1.53 m, BMI: 24.6 kg/m2, Predicted weight 45.68 kg, Ideal theoretical weight 47.1 kg; Body surface area 1.53 m2. Mestizo ethnic group.

Obstetric history: a previous pregnancy complicated by early onset preeclampsia.

Motive of hospital transfer was HELLP syndrome and liver rupture. Important, mention a previous pregnancy end by cesarean section, indicated by severe preeclampsia at 38 weeks of gestational age, with total remission in puerperium period. No history of chronic diseases. History of sudden onset 10 h of evolution of the following symptoms: intermittent frontal and temporal headache, intense 10/10, pain in the upper right abdominal quadrant, pulsatile and very intense 10/10, associated with noninvasive high blood pressure 170/120 mm Hg, severe preeclampsia, HELLP syndrome, integrated by lactate dehydrogenase 918 UI/L, GOT 121 UI/L, GPT 108 UI/L, platelets 90,000/mm3. Pregnancy of 25 weeks of gestational age, fetal death Cesarean section and damage control surgery was performed trans cesarean section (liver packing) in her unit of origin, transfer was made by air transport. She was received in Shock area with sedation based in propofol, and midazolam, invasive mechanical ventilation in volume controlled mode, shock state, hemoperitoneum detected by FAST ultrasound, and evidence of bleeding by drainage type Penrose, protocol for mass transfusion was started, stabilization with quality volume and vasopressor support, because she was in hypovolemic shock status with MAP of 35 mm Hg, meriting new damage control surgery.

In the first surgical intervention performed in this hospital unit, hepatic rupture of segments V, VI, VI, and VIII was found, requiring packaging and placement of MALA bag with open abdomen. She presented torpid evolution, requiring a total of six interventions, with five packings and finally definitive closure with total abdominal hysterectomy, right oophorectomy, due to data of endomyometritis and unilateral salpingooophoritis (Figs. 1-11). The patient developed hepatic-metabolic failure, circulatory, renal, hematological, neurological failure, and septic shock (Tables 1-4). She was maintained with hemodynamic support, 18 days of mechanical ventilation, six renal sessions of hemodialysis, hematological (received total of 20 erythrocyte concentrates, seven platelet apheresis, 73 cryoprecipitates, 24 fresh frozen plasmas, 5 g of fibrinogen, 7000 mcg of recombinant factor VII, tranexamic acid 3 g), initially presented improvement of his state of coagulopathy, renal, hepatic, and circulatory failure between days 13 and 16 of hospitalization based on platelet values of 207,000/mm3, having previously been up to levels of 27,000/mm3, INR 1.39 previously reporting 1.88, hematocrit of 32.4%, with previous 20%, glucose controls of 85 to 140 mg/dL, with the previous hypoglycemia of up to 37 mg/dL, serum lactate 2 mmol/L, with previous 7-10 mmol/L. fibrinogen of 207 mg/dL, with previous up to 95 mg/dL. pH of 7.41, when previously presented acidemia with pH up to 7.2, bicarbonate of 22.9 mMol/L, with the previous of up to 16 mMol/L. creatinine of 1.5 mg/dL, with previous of up to 7 mg/dL. LDH of 515 IU/L, with preamps up to 10,813 IU/L, ast and ALT of 125 and 72 IU/L, with preamps up to 7000 IU/L both. Deterioration in her past 2 days of life with fatal outcome after 18 days of hospitalization with multi-organ failure induced by sepsis, demonstrated by result of culture of blood sample with the same germ as in peritoneal culture and hemodynamic profile (systemic vascular resistance 549 dyna-sec/cm5 and increased cariac output 12 L/min). Enterococcus faecium was isolated in peritoneal fluid culture and hematic sample, culture of bronchial secretions and urine were negative. Multidisciplinary treatment involved critical medicine, internal medicine, general surgery, anesthesiology, nephrology, infectiology, and nutrition staff.

Figure 1 First laparotomy. 

Figure 2 Second laparotomy. 

Figure 3 Third laparotomy. 

Figure 4 Fourth laparotomy. 

Figure 5 Fifth laparotomy. 

Figure 6 Sixth laparotomy. 

Figure 7 Uterus. 

Figure 8 Uterus with necrosis. 

Figure 9 Uterus removed. 

Figure 10 Use of MALA bag. 

Figure 11 MALA bag. 

Table 1 Arterial gasometry results 

Day 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18
Ph 7.29 7.24 7.36 7.26 7.3 7.3 7.39 7.4 7.37 7.44 7.38 7.35 7.31 7.41 7.49 7.37 7.35 6.9
HCO3 17.2 16.9 19.5 19.4 21.1 21.7 16.7 20.7 21.1 21.1 19.6 20 21.8 22.9 22.6 22.3 20.7 6.7
PCO2 34.2 40 35.2 44 44 46 20 30 37 27 30 34 44 34 26 38 32 36
PO2 122 101 127 100 110 97 96 88 72 77 70 95 111 122 104 47 38 61
D base 8 9.4 4.8 7.8 5.1 2.4 12.2 6.2 5.3 4.9 7.4 6.9 4 3.1 3.5 3.3 5.2 25
Lactate 4 7 4 2 3 2 3 4 2 3 2 2 3 4 2 2 4 10

Source: Clinical record.

Table 2 Hematological results 

Día 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18
INR 1 1.33 1.66 1.88 1.85 1.59 1.63 1.55 1.59 1.59 1.5 1.59 1.55 1.44 1.39 1.49 1.43 1.59
PT 14 15.2 11.6 20.7 20.4 17.8 18.2 17.3 17.8 16.8 17.8 17.3 16.2 11.6 16.2 16.7 16.3 17
PTT 34 60 30 25 32.5 32.3 35.8 49.3 34.3 33.6 37.1 42 44 75.5 25.6 25.6 40.2 32.6
Hematocrit 37 31.5 25.7 25.7 23.1 22.9 21.6 25.1 29.1 29.5 21.6 30.6 32.4 31.5 19.1 21.6 34.7 31.3
Platelets 90 75 26 66 51 57 69 67 56 63 60 67 207 75 78 100 102 120
WBC 12 15.1 5 5.4 8.9 11.5 9.4 8 8.8 8.4 9.4 7.5 21.1 15.1 22.4 11.6 7.7 2.7

Source: Clinical record.

Table 3 Blood chemistry results 

Day 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18
Glucose 87 158 82 84 37 147 68 53 89 121 83 108 148 85 133 118 95 105
Creatinin 0.8 1.17 1.85 3.09 5.15 3.09 5.15 6 6.42 6.42 7.15 3.84 2.26 2.07 2.22 1.59 1.58 2.73
BUN 10 26 26 34 43 53 67 81 81 99 111 140 121 82 94 126 122 70
Urea 21 32 52 72.8 92 113 143.4 173 173 211 237 299 258 175 201 269 149 218
Bilirrubin 0.4 3.28 3.9 4.58 5.55 5.15 5.81 6.12 7.08 7.27 8.51 5 11.5 12.89 10.15 13.72 13.9 12.9
AST 121 1000 1000 6000 7336 2800 846 450 227 144 125 121 162 167 125 166 131 138
ALT 108 1100 1100 7000 4366 2524 881 398 229 130 87 80 80 72 72 66 97 11
LDH 918 1343 750 4500 10813 4500 1036 870 704 947 1250 886 860 515 663 652 690 688

Source: Clinical record.

Table 4 Seric electrolytes 

Day 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18
Sodium 137 137 139 141 142 141 142 142 137 138 139 139 141 140 140 141 142 142
Potassium 6.3 6.13 7.18 7.18 6.26 6.47 6.19 6.19 7.65 6.78 6.57 5.1 4.6 4.26 4.78 4.77 4.77 4.53
Chlorine 108 106 107 108 108 107 108 106 106 106 107 103.37 108 109 108 108 104 103
Calcium 7.3 8.2 7.9 7.8 7.3 6.6 6.8 6.7 6.8 6.9 6.7 7.5 8.41 7.6 8.2 8.1 7.9 7.9

Source: Clinical record.

Discussion

It has been documented since the nineties that liver rupture due to preeclampsia is a condition of very low incidence but high mortality, as described in numerous clinical case reports above1-6, This case is one of the few that have been documented in the world, since its incidence is very low, generally the reported cases are hematomas and not complete rupture7-9.

In the example mentioned, it initially evolved with severe hypertension and later with hemorrhagic shock, due to the massiveness of bleeding after liver rupture and consequent bleeding10,11.

In the reported case, a damage control surgery protocol was made with six interventions in total, which were performed by the most trained personnel; however, there were some of the available options known in the literature, such as selective embolization, liver transplantation, interventional radiology measures, etc.12-17.

However, due to the complications of concomitant preeclampsia, such as disseminated intravascular coagulation and the massive endothelial lesion developed, a series of events occurred that led to the need for multiple surgical reinterventions and with it the fearsome complication of intra-abdominal sepsis, which was finally the cause of her death, resulting similar to that described in multiple case reports and literature reviews cited18-20.

Conclusion

Liver rupture is a deadly complication of preeclampsia and represents a challenge for the surgeon facing this clinical entity, as well as for the multidisciplinary team that performs the organic support during hospitalization in intensive care. The case of the patient presented had a fatal outcome; however, all possible medical and surgical interventions were performed, as well as multidisciplinary management of each of the organic failures that manifested themselves during the clinical course of her condition. Early detection of preeclampsia and its timely treatment can prevent such tragic and costly social and economic outcomes.

References

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FundingThe authors declare that there was no funding for this article.

Ethical disclosures

Protection of human and animal subjects. The authors declare that the procedures followed were in accordance with the regulations of the relevant clinical research ethics committee and with those of the Code of Ethics of the World Medical Association (Declaration of Helsinki).

Confidentiality of data. The authors declare that they have followed the protocols of their work center on the publication of patient data.

Right to privacy and informed consent. The authors have obtained the written informed consent of the patients or subjects mentioned in the article. The corresponding author is in possession of this document.

Received: August 30, 2022; Accepted: January 23, 2023

* Correspondence: Jesús C. Briones-Garduño E-mail: drcarlosbriones@yahoo.com.mx

Conflicts of interest

The authors declare that they have no conflicts of interest.

Creative Commons License Sociedad Médica del Hospital General de Mexico. Published by Permanyer. This is an open ccess article under the CC BY-NC-ND license