Posts Tagged ‘Baby Genital Herpes’

Baby Genital Herpes

Thursday, March 12th, 2009
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With Special Reference To Pregnancy

is a sexually transmitted disease (STD) caused by viruses type 1 (HSV-1) and type 2 (HSV-2). The anxiety for a pregnant woman is that she may transfer the virus to her baby during pregnancy and childbirth with potentially severe consequences. In this article measures to avoid such disaster are discussed.

virus type 1 and type 2 are common infections worldwide. virus type 2 is the cause of most and is almost always sexually transmitted whereas the type 1 virus is more commonly associated with sores around the . There is no exclusivity with some ulcers around the being caused by the type 2 virus and some infections being related to the type 1 virus. These are probably related to sex.

Baby Genital Herpes

 

infections can be diagnosed by visual inspection by a doctor. Swabs from the affected area can be taken and the virus cultured in the laboratory. When a person contracts infection, the immune system produces antibodies that can be measured in the serum (blood with its cells removed).

In the USA one adult in five has antibodies to type 2 . The number of people who have been diagnosed with the condition rose from 10% to 14% between 1988 and 1999. Seroprevalence of HSV-1 decreased from 62.0% in 1988-1994 to 57.7% in 1999-2004, a relative decrease of 6.9%.

atypical genital herpes infections may be primary, secondary, recurrent or asymptomatic with viral shedding. In a primary infection, the infection is apparent but there are as yet no antibodies to either HSV-1 or HSV-2 at the time of the indicating no prior exposure. Typically, lesions appear 2-14 days after contact. Without antiviral therapy, the lesions last for 20 days. Viral shedding lasts 12 days, with the highest rates of shedding occurring before develop and during the first half of the . Viral shedding ceases before complete resolution of the lesion. Antibody response occurs 3-4 weeks after the primary infection and is life-long. However, unlike protective antibodies to other viruses, antibodies to HSV do not prevent local recurrences. The associated with local recurrences tend to be milder than those occurring with primary disease.

The lesions of a primary infection begin as tender vesicles (), which may burst to become ulcers. The vagina is commonly inflamed and the cervix is involved in 80% of patients. Pre-existing HSV-1 antibodies can alleviate clinical manifestations of subsequently acquired HSV-2. More than 75% of patients with primary HSV infection are asymptomatic. Asymptomatic primary HSV infections in pregnant at term are responsible for most neonatal (newborn) HSV infections.

genital herpes research associated with primary infections may be local and constitutional. Local include intense pain, dysuria (pain passing urine), itching, discharge, and lymphadenopathy (swelling of the lymph glands). Constitutional include fever, headache, nausea, malaise, and myalgia (aching muscles).

A non-primary first episode infection is a first HSV in a woman who has HSV type 1 antibodies. Because of the partial protection of the pre-existing antibodies, these tend to have fewer and shorter systemic . The duration of lesions is shorter, averaging 15 days, and viral shedding lasts for approximately 7 days.

A recurrent infection is defined as a HSV in a woman with type 2 antibodies. Recurrent HSV outbreaks may be symptomatic or asymptomatic. Lesions typically last for 9 days, and viral shedding lasts for approximately 4 days. The viral load tends to be lower in recurrent outbreaks than with primary lesions, and shedding tends to occur during the prodrome (pre-symptomatic phase) and early stage of the clinical .

home remedies for genital herpesPrimary infections in pregnancy are over diagnosed. Correct classification of gestational infections can only be accomplished when clinical evaluation is combined with viral isolation and serologic testing using a type-specific assay. Most severe first clinical episodes of infections among in the second and third trimesters of pregnancy are not primary infections and are not commonly associated with perinatal morbidity.

Most affected babies acquire the virus at the time of delivery. Just 5% of all cases of neonatal (newborn) HSV infection result from transplacental transmission during pregnancy. In this regard, it is one of the TORCH (toxoplasmosis, rubella, cytomegalovirus, and ) infections, which are associated with microcephaly (small head), microphthalmia (small eyes), intracranial (within the brain) calcifications, and chorioretinitis (inflammation in the eyes). The acquisition of during pregnancy has been associated with spontaneous miscarriage, prematurity and congenital and neonatal .

Neonatal is a severe systemic (involving all the body) viral infection with a high morbidity (illness) and mortality. Neonatal can cause skin, eye or infections, damage to the central nervous system and other internal organs and mental retardation. It is relatively uncommon in the UK with an incidence of 1.65 per 100 000 live births annually, which compares to 11 per 100, 000 deliveries in the USA.

Neonatal may be caused by type 1 (HSV-1) or type 2 (HSV-2), as either viral type can cause . The risks are greatest when a woman acquires a primary infection during late pregnancy, so that the baby is delivered before the development of protective maternal antibodies. All should be asked at their first antenatal visit if they or their partner have ever had . Female partners of with , who themselves give no history of , should be advised about reducing their risk of acquiring this infection.

hsv-1 genital herpes who report a history of can be reassured that, in the event of an HSV recurrence during pregnancy, the risk of transmission to the neonate is extremely small, even if lesions are present at delivery. with no history of may reduce their risk of acquiring during pregnancy by avoiding sexual intercourse at times when their partner has an HSV recurrence. The impact of this intervention is limited because sexual transmission of HSV commonly results from sexual contact during periods of asymptomatic viral shedding.

Aciclovir is well tolerated in late pregnancy and there is no clinical or laboratory evidence of maternal or fetal toxicity. Aciclovir has been used extensively in pregnancy and it appears to be safe. The use of intravenous aciclovir may reduce the risk of neonatal by minimising maternal viraemia and reducing exposure of the fetus to HSV for who develop first episode within six weeks of delivery. A randomised controlled trial for with recurrent was unable to demonstrate that acyclovir in late pregnancy significantly reduces the number of caesarean sections. The conclusion was that there is little evidence to suggest that acyclovir should be used for the suppression of recurrent infection during pregnancy.

Where first-episode Lesions are present at the time of delivery and the baby is delivered vaginally, the risk of neonatal is about 40%. The risk of transmission is associated with duration of rupture of the membranes, the risk increasing considerably after the membranes had been ruptured for more than four hours.

Caesarean section is recommended for all presenting with first-episode lesions at the time of delivery, but is not indicated for who develop first episode lesions earlier in the pregnancy. If the first episode of lesions within six weeks of the expected date of delivery or onset of preterm labour, elective caesarean section may be considered at term, or as indicated, and the paediatricians should be informed.

In the 1980s, it was common practice to take swabs for viral cultures weekly from with a history of during the last six weeks of pregnancy and if the results were positive delivery would be by elective caesarean section. This practice is no longer recommended as it has been demonstrated that antenatal swabbing did not predict the shedding of virus at the onset of labour.

For presenting with recurrent lesions at the onset of labour, the risks to the baby of neonatal are negligible with two major studies showing no transmission to the baby. In one study, one baby in 34 with active recurrent was affected. The practice of caesarean delivery for with a history of lesions that recur at delivery would result in more than 1580 excess caesarean deliveries being performed for every poor neonatal outcome prevented at a cost per neonatal case averted of $2.5 million at 1993 rates. Furthermore, there could well be more maternal deaths by this practice than newborn babies saved. In Holland, caesarean sections have not been routinely performed for this indication since 1987 and there has been no increase in the reported incidence of neonatal .

Mother with Unwittingly Kills Baby with a Kiss – Strollerderby

"Most is caused by HSV-2, although HSV-1 accounts for about _half_ of new cases in developed countries. The prevalence of virus (HSV) type 2 infections in the general population ranges from 10% to 60%"    Read more…

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Prevent Female | Get Rid Of Warts

In rare cases, female warts can be passed from a mother to her baby. The warts may show up on the baby’s throat or on the genitals. female. Female warts can be prevented. The best method is abstinence,    Read more…

Essential Facts About and Outbreaks and Causes

Essential Facts About and Outbreaks and Causes That you need to know all about. is a virus and the two main types of this.   Read more…

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If you have , speak to your gynecologist about a Cesarean. Section. Don’t panic. Many hospitals around the world have highly developed ultrasound and other techniques available to evaluate your baby’s development.    Read more…

Trendy Science: Viruses: Cold Sores and

HSV-2, on the other hand, affects between 5 and 10% of the population (including many individuals who are also infected with HSV-1), and is more often associated with , although either virus can cause a similar disease at both …. These antibodies will be passed to the developing baby before it is born, greatly reducing the risk of transmission. The baby should, however, be monitored closely when it is first born for any that it may have picked up…   Read more…

By: David A Viniker

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David A Viniker MD FRCOG is a London Consultant in OB/GYN who strongly supports patient choice. You are welcome to visit his websites which explain the pros and cons of the various options for ‘s health, pregnancy and childbirth: www.2womenshealth.com/31_Disorders_Of_The_Vulva/31-03_Herpes.htm">www.2womenshealth.com