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==Overview==
==Overview==
== Historical Perspective ==
Hydrops fetalis was first discovered by Dr. John William Ballantyne, a Scottish physician and obstetrician, in 1892.


==Classification==
==Classification==
Hydrops Fetalis may be classified into two groups based on the presence or absence of rhesus iso-immunization:


*Hydrops fetalis may be classified according to the cause into:
* '''Immune Hydrops Fetalis'''
**Immune hydrops fetalis
* '''Non-Immune Hydrops Fetalis (NIHF)'''
**Non-immune hydrops fetalis (NIHF)


==Pathophysiology==
==Pathophysiology==
Line 23: Line 26:


==Causes==
==Causes==
Hydrops Fetalis is caused by either immune or non-immune conditions.


*Immune hydrops fetalis
*'''Immune hydrops fetalis'''
*Causes of non-immune hydrops fetalis (NIHF) include:  
**Antibodies may occur due to the exposure of non-self RBC antigens during the previous pregnancy or transfusion. In the next pregnancy, these antibodies may attack the fetal erythrocytes if the fetus has that antigen. Following the red blood cell destruction, hemolytic disease of the fetus and newborn (HDFN) may occur with a wide range of clinical outcome from only mild anemia to high output heart failure and hydrops fetalis.<ref name="pmid30097223">{{cite journal| author=Webb J, Delaney M| title=Red Blood Cell Alloimmunization in the Pregnant Patient. | journal=Transfus Med Rev | year= 2018 | volume= 32 | issue= 4 | pages= 213-219 | pmid=30097223 | doi=10.1016/j.tmrv.2018.07.002 | pmc= | url=https://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=30097223  }}</ref>
**Structural cardiac malformations (especially hypoplastic left heart, endocardial cushion defect)
***Rh disease is the major cause for immune mediated hydrops fetalis; however, owing to preventative methods developed in the 1970s, the incidence of Rh disease has markedly declined. Rh disease can be prevented by administration of anti-D IgG (Rho (D) Immune Globulin) injections to RhD-negative mothers during pregnancy and/or within 72 hours of the delivery. 
**Arrhythmias
*'''Non-immune hydrops fetalis (NIHF)'''
**Congenital lymphatic dysplasia
**Currently, with the decreased prevelance of Rh disease, non-immune causes are responsible for up to 90% of cases. The non-immune form of hydrops fetalis has many causes including:  
**Turner Syndrome
***Structural cardiac malformations (especially hypoplastic left heart, endocardial cushion defect)
**Trisomy 18
***Arrhythmias
**Trisomy 21
***Congenital lymphatic dysplasia
**Alpha-thalassemia
***Chromosomal abnormalities (Turner Syndrome, trisomy 13, trisomy 18, trisomy 21)
**Fetomaternal transfusion
***Alpha-thalassemia
**Infections (Parvo-B19, CMV, Adenovirus, Enterovirus)
***Fetomaternal transfusion
**Twin to twin transfusion syndrome (both donor and recipient fetus)
***Infections (Parvo-B19, CMV, Adenovirus, Enterovirus)
**Congenital cystic adenomatoid malformation
***Twin to twin transfusion syndrome (both donor and recipient fetus)
**Diaphragmatic hernia
***Congenital cystic adenomatoid malformation
**Extrapulmonary sequestration
***Diaphragmatic hernia
**Hydrothorax
***Extrapulmonary sequestration
**Chylothorax
***Hydrothorax
**Noonan Syndrome
***Chylothorax
**Urethral Obstruction
***Noonan Syndrome
**Prune belly syndrome
***Urethral Obstruction
**Lysosomal storage disease
***Prune belly syndrome
**Vascular tumors
***Lysosomal storage disease
**Teratoma
***Vascular tumors
**Leukemia
***Teratoma
**Hepatic tumors
***Leukemia
**Neuroblastoma
***Hepatic tumors
**Meconium peritonitis
***Neuroblastoma
**Gastrointestinal obstructions
***Meconium peritonitis
***Gastrointestinal obstructions


==References==
==References==
<references /><br />
<references /><br />

Revision as of 13:46, 23 April 2021

Hydrops Fetalis

Overview

Historical Perspective

Hydrops fetalis was first discovered by Dr. John William Ballantyne, a Scottish physician and obstetrician, in 1892.

Classification

Hydrops Fetalis may be classified into two groups based on the presence or absence of rhesus iso-immunization:

  • Immune Hydrops Fetalis
  • Non-Immune Hydrops Fetalis (NIHF)

Pathophysiology

  • It is thought that hydrops fetalis is caused by conditions with an increased rate of fluid transudation from the vascular compartment or decreased lymphatic return to the circulation, chiefly because of the developmental defects in microcirculation and lymphatic system, respectively.
  • While these conditions may be both immune and non-immune, they often result in anemia and further hypoxia.
  • The sympathetic system becomes activated due to hypoxia, and it causes blood redistribution with decreased blood flow to the liver and kidneys.
  • It results in decreased albumin, increased ADH, and increased activity of RAAS.
  • Through these changes, the central venous pressure increases, which further results in decreased lymphatic return.
  • As a result, severe and progressive edema occurs in a fetus.
  • The pathophysiology of non-immune causes also depend on the underlying conditions, include:
    • Decreased ventricular filling during diastole (i.e. tachyarrhythmias)
    • Increased central venous pressure due to the increased right heart pressure (i.e. cardiac tumors and subendocardial fibroelastosis)
    • Obstruction of lymphatic drainage due to a mass (i.e. cystic hygroma)

Causes

Hydrops Fetalis is caused by either immune or non-immune conditions.

  • Immune hydrops fetalis
    • Antibodies may occur due to the exposure of non-self RBC antigens during the previous pregnancy or transfusion. In the next pregnancy, these antibodies may attack the fetal erythrocytes if the fetus has that antigen. Following the red blood cell destruction, hemolytic disease of the fetus and newborn (HDFN) may occur with a wide range of clinical outcome from only mild anemia to high output heart failure and hydrops fetalis.[1]
      • Rh disease is the major cause for immune mediated hydrops fetalis; however, owing to preventative methods developed in the 1970s, the incidence of Rh disease has markedly declined. Rh disease can be prevented by administration of anti-D IgG (Rho (D) Immune Globulin) injections to RhD-negative mothers during pregnancy and/or within 72 hours of the delivery.
  • Non-immune hydrops fetalis (NIHF)
    • Currently, with the decreased prevelance of Rh disease, non-immune causes are responsible for up to 90% of cases. The non-immune form of hydrops fetalis has many causes including:
      • Structural cardiac malformations (especially hypoplastic left heart, endocardial cushion defect)
      • Arrhythmias
      • Congenital lymphatic dysplasia
      • Chromosomal abnormalities (Turner Syndrome, trisomy 13, trisomy 18, trisomy 21)
      • Alpha-thalassemia
      • Fetomaternal transfusion
      • Infections (Parvo-B19, CMV, Adenovirus, Enterovirus)
      • Twin to twin transfusion syndrome (both donor and recipient fetus)
      • Congenital cystic adenomatoid malformation
      • Diaphragmatic hernia
      • Extrapulmonary sequestration
      • Hydrothorax
      • Chylothorax
      • Noonan Syndrome
      • Urethral Obstruction
      • Prune belly syndrome
      • Lysosomal storage disease
      • Vascular tumors
      • Teratoma
      • Leukemia
      • Hepatic tumors
      • Neuroblastoma
      • Meconium peritonitis
      • Gastrointestinal obstructions

References

  1. Webb J, Delaney M (2018). "Red Blood Cell Alloimmunization in the Pregnant Patient". Transfus Med Rev. 32 (4): 213–219. doi:10.1016/j.tmrv.2018.07.002. PMID 30097223.


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