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PID Curriculum
1
Pelvic Inflammatory Disease
(PID)
PID Curriculum
2
Learning Objectives
Upon completion of this content, the learner will be able to
Describe the epidemiology of PID in the U.S.;
Describe the pathogenesis of PID;
Discuss the clinical manifestations of PID;
Identify the clinical criteria used in the diagnosis of PID;
List CDC-recommended treatment regimens for PID;
Summarize appropriate prevention counseling messages
for a patient with PID; and
Describe public health measures to prevent PID.
PID Curriculum
3
Lessons
I. Epidemiology: Disease in the U.S.
II. Pathogenesis
III. Clinical manifestations
IV. PID diagnosis
V. Patient management
VI. Prevention
PID Curriculum
4
Lesson I: Epidemiology:
Disease in the U.S.
PID Curriculum
5
Pelvic Inflammatory Disease
• Clinical syndrome associated with ascending
spread of microorganisms from the vagina or
cervix to the endometrium, fallopian tubes,
ovaries, and contiguous structures.
• Comprises a spectrum of inflammatory
disorders, including any combination of
endometritis, salpingitis, tubo-ovarian
abscess, and pelvic peritonitis.
Epidemiology
PID Curriculum
6
Incidence and Prevalence
• Estimated to occur in 750,000 U.S. women annually.
• Annual cost exceeds $4.2 billion.
• No national surveillance or reporting requirements exist,
and national estimates are limited by insensitive clinical
diagnosis criteria.
• During 2001-2010, hospitalizations for acute PID overall
have shown modest declines, although hospitalizations
for acute PID increased by 44.3% (from 36.3 to 52.4 per
100,000) between 2009 and 2010. Hospitalizations for
chronic PID have also shown modest declines,
remaining relatively stable between 2007 and 2010.
• The estimated number of initial visits to physicians’
offices for PID from NDTI declined during 2003– 2012.
Epidemiology
PID Curriculum
7
Pelvic Inflammatory Disease—Hospitalizations of Women
Aged 15–44 Years, United States, 2001–2010
NOTE: The relative standard errors for acute and unspecified pelvic inflammatory disease (PID) cases ranges from
8%-18%. The relative standard error for chronic PID cases ranges from 12%–28%. Data only available through
2010.
SOURCE: 2010 National Hospital Discharge Survey [Internet]. Atlanta: Centers for Disease Control and Prevention.
Available from: http://www.cdc.gov/nchs/nhds.htm.
Epidemiology
PID Curriculum
8
Pelvic Inflammatory Disease—Initial Visits to Physicians’ Offices
by Women Aged 15–44 Years, United States, 2002–2012
NOTE: The relative standard errors for these estimates are 21.6–30% .
SOURCE: IMS Health, Integrated Promotional Services ™. IMS Health Report, 1966–2012.
Epidemiology
PID Curriculum
9
Risk Factors
• Adolescence
• History of PID
• Infected with or a history of gonorrhea or
chlamydia
• Male partners with gonorrhea or chlamydia
• Multiple sex partners
• Current douching
• Insertion of IUD
• Bacterial vaginosis
• Oral contraceptive use (in some cases)
• Demographics (socioeconomic status)
Epidemiology
PID Curriculum
10
Normal Cervix with Ectopy
Source: Seattle STD/HIV Prevention Training Center at the University of Washington/
Claire E. Stevens
Epidemiology
PID Curriculum
11
Lesson II: Pathogenesis
PID Curriculum
12
Microbial Etiology
• Most cases of PID are polymicrobial
• Most common pathogens
– N. gonorrhoeae: recovered from cervix in
30%–80% of women with PID
– C. trachomatis: recovered from cervix in
20%–40% of women with PID
– N. gonorrhoeae and C. trachomatis are
present in combination in approximately
25%–75% of patients
Pathogenesis
PID Curriculum
13
Pathway of Ascending Infection
Cervicitis
Endometritis
Salpingitis/
oophoritis/ tubo-
ovarian abscess
Peritonitis
Pathogenesis
PID Curriculum
14
Normal Human Fallopian Tube Tissue
Source: Patton, D.L. University of Washington, Seattle, Washington
Pathogenesis
PID Curriculum
15
C. trachomatis Infection (PID)
Source: Patton, D.L. University of Washington, Seattle, Washington
Pathogenesis
PID Curriculum
16
Lesson III: Clinical
Manifestations
PID Curriculum
17
PID Classification
Severe
symptoms
4%
Subclinical/
silent
60%
Mild to
moderate
symptoms
36%
Overt
40%
Clinical Manifestations
PID Curriculum
18
Sequelae
• Approximately 25% of women with a single
episode of PID will experience sequelae,
including ectopic pregnancy, infertility, or
chronic pelvic pain.
• Tubal infertility occurs in 8% of women after
one episode of PID, in 20% of women after
two episodes, and in 50% of women after
three episodes.
Clinical Manifestations
PID Curriculum
19
Lesson IV: PID Diagnosis
PID Curriculum
20
Minimum Criteria in the
Diagnosis of PID
• Uterine tenderness, or
• Adnexal tenderness, or
• Cervical motion tenderness
Diagnosis
PID Curriculum
21
Additional Criteria to Increase
Specificity of PID Diagnosis
• Oral temperature >38.3°C (101°F)
• Abnormal cervical or vaginal mucopurulent
discharge
• Presence of abundant numbers of WBCs on
saline microscopy of vaginal fluid
• Elevated erythrocyte sedimentation rate
• Elevated C-reactive protein
• Cervical infection with gonorrhea or
chlamydia
Diagnosis
PID Curriculum
22
Mucopurulent Cervical Discharge
(Positive swab test)
Source:Seattle STD/HIV Prevention Training Center at the University of Washington/
Claire E. Stevens and Ronald E. Roddy
Diagnosis
PID Curriculum
23
More Specific Criteria Used in
Diagnosing PID
• Endometrial biopsy
• Transvaginal sonography or MRI
• Laparoscopy
Diagnosis
PID Curriculum
24
Lesson V: Patient
Management
PID Curriculum
25
General PID Management
Considerations
• Regimens must provide empiric broad-
spectrum coverage of likely pathogens
including N. gonorrhoeae, C. trachomatis,
anaerobes, Gram-negative bacteria, and
streptococci
• Treatment should be instituted as early as
possible to prevent long-term sequelae
Management
PID Curriculum
26
Criteria for Hospitalization
of Women with PID
• Inability to exclude surgical emergencies
• Pregnancy
• Non-response to oral therapy
• Inability to follow or tolerate an outpatient oral
regimen
• Severe illness, nausea and vomiting, high fever
• Tubo-ovarian abscess
Management
PID Curriculum
27
PID Treatment Regimens
– CDC-recommended oral regimen A
• Ceftriaxone 250 mg intramuscularly in a single dose, plus
• Doxycycline 100 mg orally two times a day for 14 days
with or without
• Metronidazole 500 mg orally two times a day for 14 days
– CDC-recommended oral regimen B
• Cefoxitin 2 g intramuscularly in a single dose, and Probenecid 1 g orally in a single
dose, plus
• Doxycycline 100 mg orally two times a day for 14 days
with or without
• Metronidazole 500 mg orally two times a day for 14 days
– CDC-recommended oral regimen C
• Other parenteral third-generation cephalosporin (e.g., Ceftizoxime, Cefotaxime), plus
• Doxycycline 100 mg orally two times a day for 14 days
with or without
• Metronidazole 500 mg orally two times a day for 14 days
Management
PID Curriculum
28
Follow-Up
• Patients should demonstrate substantial
improvement within 72 hours.
• Patients who do not improve usually require
hospitalization, additional diagnostic tests, and
possible surgical intervention.
• Repeat testing of all women who have been
diagnosed with chlamydia or gonorrhea is
recommended 3–6 months after treatment.
• All women diagnosed with clinical acute PID
should be offered HIV testing.
Management
PID Curriculum
29
PID Parenteral Regimens
• CDC-recommended parenteral regimen A
– Cefotetan 2 g intravenously every 12 hours, or
– Cefoxitin 2 g intravenously every six hours, plus
– Doxycycline 100 mg orally or intravenously every 12 hours
• CDC-recommended parenteral regimen B
– Clindamycin 900 mg intravenously every eight hours, plus
– Gentamicin loading dose intravenously or intramuscularly (2
mg/kg), followed by maintenance dose (1.5 mg/kg) every eight
hours. Single daily gentamicin dosing (3–5 mg/kg) may be
substituted.
Management
PID Curriculum
30
Alternative Parenteral Regimen
• Ampicillin/Sulbactam 3 g intravenously every six hours, plus
Doxycycline 100 mg orally or intravenously every 12 hours
• It is important to continue either regimen A or B or alternative
regimens for 24 hours after substantial clinical improvement
occurs, and also to complete a total of 14 days of therapy with
– Doxycycline 100 mg orally twice a day, or
– Clindamycin 450 mg orally four times a day
Management
PID Curriculum
31
Lesson VI: Prevention
PID Curriculum
32
Screening
• Screen and treat for chlamydia or gonorrhea to reduce the
incidence of PID.
• Chlamydia screening is recommended for
– Sexually-active women 25 and under annually;
– Sexually-active women >25 at high risk;
– Pregnant women in the first trimester; and
– Retest pregnant women 25 and under and those at increased risk for chlamydia
during the third trimester
• Gonorrhea screening is recommended for
– Sexually-active women 25 and under;
– Previous gonorrhea infection;
– Diagnosed with another STD;
– New or multiple sex partners;
– Inconsistent condom use;
– Engaged in commercial sex work or drug use.
Prevention
PID Curriculum
33
Partner Management
• Male sex partners of women with PID
should be examined and treated:
– If they had sexual contact with the patient
during the 60 days preceding the patient’s
onset of symptoms
– If a patient’s last sexual intercourse was >60
days before onset of symptoms or diagnosis,
the patient’s most recent partner should be
treated
Prevention
PID Curriculum
34
Partner Management (continued)
• Male partners of women who have PID caused
by C. trachomatis or N. gonorrhoeae are often
asymptomatic.
• Sex partners should be treated empirically with
regimens effective against both C. trachomatis
and N. gonorrhoeae, regardless of the apparent
etiology of PID or pathogens isolated from the
infected woman.
Prevention
PID Curriculum
35
Reporting
• Report cases of PID to the local STD
program in states where reporting is
mandated.
• Gonorrhea and chlamydia are
reportable in all states.
Prevention
PID Curriculum
36
Patient Counseling and Education
• Nature of the infection
• Transmission
• Risk reduction
– Assess patient's behavior-change potential
– Discuss prevention strategies
– Develop individualized risk-reduction plans
– Discuss cessation of the practice of
douching
Prevention
PID Curriculum
37
Case Study
PID Curriculum
38
History: Jane Wheels
Case Study
• 24-year-old female who reports lower abdominal pain,
cramping, slight fever, and dysuria for four days.
• G1P1, LMP two weeks ago (regular without dysmenorrhea).
Uses oral contraceptives (for two years).
• Reports gradual onset of symptoms of lower bilateral
abdominal discomfort, dysuria (no gross hematuria),
abdominal cramping and a slight low-grade fever in the
evenings for four days. Discomfort has gradually worsened.
• Denies GI disturbances or constipation. Denies vaginal
discharge.
• States that she is happily married in a monogamous
relationship. Plans another pregnancy in about six months.
No condom use.
• No history of STDs. Reports occasional yeast infections.
• Douches regularly after menses and intercourse; last
douched this morning.
PID Curriculum
39
Physical Exam
• Vital signs: blood pressure 104/72, pulse 84,
temperature 38°C, weight 132 lbs.
• Neck, chest, breast, heart, and musculoskeletal exam
within normal limits. No flank pain on percussion. No
CVA tenderness.
• On abdominal exam the patient reports tenderness in
the lower quadrants with light palpation. Several small
inguinal nodes palpated bilaterally.
• Normal external genitalia without lesions or discharge.
• Speculum exam reveals minimal vaginal discharge with
a small amount of visible cervical mucopus.
• Bimanual exam reveals uterine and adnexal tenderness
as well as pain with cervical motion. Uterus anterior,
midline, smooth, and not enlarged.
Case Study
PID Curriculum
40
Questions
1. What should be included in the
differential diagnosis?
2. What laboratory tests should be
performed or ordered?
Case Study
PID Curriculum
41
Laboratory
Results of office diagnostics:
• Urine pregnancy test: negative
• Urine dip stick for nitrates: negative
• Vaginal saline wet mount: vaginal pH was 4.5.
Microscopy showed WBCs >10 per HPF, no clue
cells, no trichomonads, and the KOH wet mount
was negative for budding yeast and hyphae.
3. What is the presumptive diagnosis?
4. How should this patient be managed?
5. What is an appropriate therapeutic regimen?
Case Study
PID Curriculum
42
Partner Management
Sex partner: Joseph (spouse)
• First exposure: four years ago
• Last exposure: one week ago
• Frequency: two times per week
(vaginal only)
6. How should Joseph be managed?
Case Study
PID Curriculum
43
Follow-Up
• On follow-up three days later, Jane had improved
clinically. The nucleic acid amplification test (NAAT) for
gonorrhea was positive. The NAAT test for chlamydia was
negative.
• Joseph (Jane’s husband) came in with Jane at follow-up.
He was asymptomatic but did admit to a "one-night stand"
while traveling. He was treated. They were offered HIV
testing which they accepted.
7. Who is responsible for reporting this case to the local
health department?
8. What are appropriate prevention counseling
recommendations for this patient?
Case Study

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Pelvic Inflammatory Disease - Case study, patterns and association

  • 2. PID Curriculum 2 Learning Objectives Upon completion of this content, the learner will be able to Describe the epidemiology of PID in the U.S.; Describe the pathogenesis of PID; Discuss the clinical manifestations of PID; Identify the clinical criteria used in the diagnosis of PID; List CDC-recommended treatment regimens for PID; Summarize appropriate prevention counseling messages for a patient with PID; and Describe public health measures to prevent PID.
  • 3. PID Curriculum 3 Lessons I. Epidemiology: Disease in the U.S. II. Pathogenesis III. Clinical manifestations IV. PID diagnosis V. Patient management VI. Prevention
  • 4. PID Curriculum 4 Lesson I: Epidemiology: Disease in the U.S.
  • 5. PID Curriculum 5 Pelvic Inflammatory Disease • Clinical syndrome associated with ascending spread of microorganisms from the vagina or cervix to the endometrium, fallopian tubes, ovaries, and contiguous structures. • Comprises a spectrum of inflammatory disorders, including any combination of endometritis, salpingitis, tubo-ovarian abscess, and pelvic peritonitis. Epidemiology
  • 6. PID Curriculum 6 Incidence and Prevalence • Estimated to occur in 750,000 U.S. women annually. • Annual cost exceeds $4.2 billion. • No national surveillance or reporting requirements exist, and national estimates are limited by insensitive clinical diagnosis criteria. • During 2001-2010, hospitalizations for acute PID overall have shown modest declines, although hospitalizations for acute PID increased by 44.3% (from 36.3 to 52.4 per 100,000) between 2009 and 2010. Hospitalizations for chronic PID have also shown modest declines, remaining relatively stable between 2007 and 2010. • The estimated number of initial visits to physicians’ offices for PID from NDTI declined during 2003– 2012. Epidemiology
  • 7. PID Curriculum 7 Pelvic Inflammatory Disease—Hospitalizations of Women Aged 15–44 Years, United States, 2001–2010 NOTE: The relative standard errors for acute and unspecified pelvic inflammatory disease (PID) cases ranges from 8%-18%. The relative standard error for chronic PID cases ranges from 12%–28%. Data only available through 2010. SOURCE: 2010 National Hospital Discharge Survey [Internet]. Atlanta: Centers for Disease Control and Prevention. Available from: http://www.cdc.gov/nchs/nhds.htm. Epidemiology
  • 8. PID Curriculum 8 Pelvic Inflammatory Disease—Initial Visits to Physicians’ Offices by Women Aged 15–44 Years, United States, 2002–2012 NOTE: The relative standard errors for these estimates are 21.6–30% . SOURCE: IMS Health, Integrated Promotional Services ™. IMS Health Report, 1966–2012. Epidemiology
  • 9. PID Curriculum 9 Risk Factors • Adolescence • History of PID • Infected with or a history of gonorrhea or chlamydia • Male partners with gonorrhea or chlamydia • Multiple sex partners • Current douching • Insertion of IUD • Bacterial vaginosis • Oral contraceptive use (in some cases) • Demographics (socioeconomic status) Epidemiology
  • 10. PID Curriculum 10 Normal Cervix with Ectopy Source: Seattle STD/HIV Prevention Training Center at the University of Washington/ Claire E. Stevens Epidemiology
  • 12. PID Curriculum 12 Microbial Etiology • Most cases of PID are polymicrobial • Most common pathogens – N. gonorrhoeae: recovered from cervix in 30%–80% of women with PID – C. trachomatis: recovered from cervix in 20%–40% of women with PID – N. gonorrhoeae and C. trachomatis are present in combination in approximately 25%–75% of patients Pathogenesis
  • 13. PID Curriculum 13 Pathway of Ascending Infection Cervicitis Endometritis Salpingitis/ oophoritis/ tubo- ovarian abscess Peritonitis Pathogenesis
  • 14. PID Curriculum 14 Normal Human Fallopian Tube Tissue Source: Patton, D.L. University of Washington, Seattle, Washington Pathogenesis
  • 15. PID Curriculum 15 C. trachomatis Infection (PID) Source: Patton, D.L. University of Washington, Seattle, Washington Pathogenesis
  • 16. PID Curriculum 16 Lesson III: Clinical Manifestations
  • 17. PID Curriculum 17 PID Classification Severe symptoms 4% Subclinical/ silent 60% Mild to moderate symptoms 36% Overt 40% Clinical Manifestations
  • 18. PID Curriculum 18 Sequelae • Approximately 25% of women with a single episode of PID will experience sequelae, including ectopic pregnancy, infertility, or chronic pelvic pain. • Tubal infertility occurs in 8% of women after one episode of PID, in 20% of women after two episodes, and in 50% of women after three episodes. Clinical Manifestations
  • 20. PID Curriculum 20 Minimum Criteria in the Diagnosis of PID • Uterine tenderness, or • Adnexal tenderness, or • Cervical motion tenderness Diagnosis
  • 21. PID Curriculum 21 Additional Criteria to Increase Specificity of PID Diagnosis • Oral temperature >38.3°C (101°F) • Abnormal cervical or vaginal mucopurulent discharge • Presence of abundant numbers of WBCs on saline microscopy of vaginal fluid • Elevated erythrocyte sedimentation rate • Elevated C-reactive protein • Cervical infection with gonorrhea or chlamydia Diagnosis
  • 22. PID Curriculum 22 Mucopurulent Cervical Discharge (Positive swab test) Source:Seattle STD/HIV Prevention Training Center at the University of Washington/ Claire E. Stevens and Ronald E. Roddy Diagnosis
  • 23. PID Curriculum 23 More Specific Criteria Used in Diagnosing PID • Endometrial biopsy • Transvaginal sonography or MRI • Laparoscopy Diagnosis
  • 24. PID Curriculum 24 Lesson V: Patient Management
  • 25. PID Curriculum 25 General PID Management Considerations • Regimens must provide empiric broad- spectrum coverage of likely pathogens including N. gonorrhoeae, C. trachomatis, anaerobes, Gram-negative bacteria, and streptococci • Treatment should be instituted as early as possible to prevent long-term sequelae Management
  • 26. PID Curriculum 26 Criteria for Hospitalization of Women with PID • Inability to exclude surgical emergencies • Pregnancy • Non-response to oral therapy • Inability to follow or tolerate an outpatient oral regimen • Severe illness, nausea and vomiting, high fever • Tubo-ovarian abscess Management
  • 27. PID Curriculum 27 PID Treatment Regimens – CDC-recommended oral regimen A • Ceftriaxone 250 mg intramuscularly in a single dose, plus • Doxycycline 100 mg orally two times a day for 14 days with or without • Metronidazole 500 mg orally two times a day for 14 days – CDC-recommended oral regimen B • Cefoxitin 2 g intramuscularly in a single dose, and Probenecid 1 g orally in a single dose, plus • Doxycycline 100 mg orally two times a day for 14 days with or without • Metronidazole 500 mg orally two times a day for 14 days – CDC-recommended oral regimen C • Other parenteral third-generation cephalosporin (e.g., Ceftizoxime, Cefotaxime), plus • Doxycycline 100 mg orally two times a day for 14 days with or without • Metronidazole 500 mg orally two times a day for 14 days Management
  • 28. PID Curriculum 28 Follow-Up • Patients should demonstrate substantial improvement within 72 hours. • Patients who do not improve usually require hospitalization, additional diagnostic tests, and possible surgical intervention. • Repeat testing of all women who have been diagnosed with chlamydia or gonorrhea is recommended 3–6 months after treatment. • All women diagnosed with clinical acute PID should be offered HIV testing. Management
  • 29. PID Curriculum 29 PID Parenteral Regimens • CDC-recommended parenteral regimen A – Cefotetan 2 g intravenously every 12 hours, or – Cefoxitin 2 g intravenously every six hours, plus – Doxycycline 100 mg orally or intravenously every 12 hours • CDC-recommended parenteral regimen B – Clindamycin 900 mg intravenously every eight hours, plus – Gentamicin loading dose intravenously or intramuscularly (2 mg/kg), followed by maintenance dose (1.5 mg/kg) every eight hours. Single daily gentamicin dosing (3–5 mg/kg) may be substituted. Management
  • 30. PID Curriculum 30 Alternative Parenteral Regimen • Ampicillin/Sulbactam 3 g intravenously every six hours, plus Doxycycline 100 mg orally or intravenously every 12 hours • It is important to continue either regimen A or B or alternative regimens for 24 hours after substantial clinical improvement occurs, and also to complete a total of 14 days of therapy with – Doxycycline 100 mg orally twice a day, or – Clindamycin 450 mg orally four times a day Management
  • 32. PID Curriculum 32 Screening • Screen and treat for chlamydia or gonorrhea to reduce the incidence of PID. • Chlamydia screening is recommended for – Sexually-active women 25 and under annually; – Sexually-active women >25 at high risk; – Pregnant women in the first trimester; and – Retest pregnant women 25 and under and those at increased risk for chlamydia during the third trimester • Gonorrhea screening is recommended for – Sexually-active women 25 and under; – Previous gonorrhea infection; – Diagnosed with another STD; – New or multiple sex partners; – Inconsistent condom use; – Engaged in commercial sex work or drug use. Prevention
  • 33. PID Curriculum 33 Partner Management • Male sex partners of women with PID should be examined and treated: – If they had sexual contact with the patient during the 60 days preceding the patient’s onset of symptoms – If a patient’s last sexual intercourse was >60 days before onset of symptoms or diagnosis, the patient’s most recent partner should be treated Prevention
  • 34. PID Curriculum 34 Partner Management (continued) • Male partners of women who have PID caused by C. trachomatis or N. gonorrhoeae are often asymptomatic. • Sex partners should be treated empirically with regimens effective against both C. trachomatis and N. gonorrhoeae, regardless of the apparent etiology of PID or pathogens isolated from the infected woman. Prevention
  • 35. PID Curriculum 35 Reporting • Report cases of PID to the local STD program in states where reporting is mandated. • Gonorrhea and chlamydia are reportable in all states. Prevention
  • 36. PID Curriculum 36 Patient Counseling and Education • Nature of the infection • Transmission • Risk reduction – Assess patient's behavior-change potential – Discuss prevention strategies – Develop individualized risk-reduction plans – Discuss cessation of the practice of douching Prevention
  • 38. PID Curriculum 38 History: Jane Wheels Case Study • 24-year-old female who reports lower abdominal pain, cramping, slight fever, and dysuria for four days. • G1P1, LMP two weeks ago (regular without dysmenorrhea). Uses oral contraceptives (for two years). • Reports gradual onset of symptoms of lower bilateral abdominal discomfort, dysuria (no gross hematuria), abdominal cramping and a slight low-grade fever in the evenings for four days. Discomfort has gradually worsened. • Denies GI disturbances or constipation. Denies vaginal discharge. • States that she is happily married in a monogamous relationship. Plans another pregnancy in about six months. No condom use. • No history of STDs. Reports occasional yeast infections. • Douches regularly after menses and intercourse; last douched this morning.
  • 39. PID Curriculum 39 Physical Exam • Vital signs: blood pressure 104/72, pulse 84, temperature 38°C, weight 132 lbs. • Neck, chest, breast, heart, and musculoskeletal exam within normal limits. No flank pain on percussion. No CVA tenderness. • On abdominal exam the patient reports tenderness in the lower quadrants with light palpation. Several small inguinal nodes palpated bilaterally. • Normal external genitalia without lesions or discharge. • Speculum exam reveals minimal vaginal discharge with a small amount of visible cervical mucopus. • Bimanual exam reveals uterine and adnexal tenderness as well as pain with cervical motion. Uterus anterior, midline, smooth, and not enlarged. Case Study
  • 40. PID Curriculum 40 Questions 1. What should be included in the differential diagnosis? 2. What laboratory tests should be performed or ordered? Case Study
  • 41. PID Curriculum 41 Laboratory Results of office diagnostics: • Urine pregnancy test: negative • Urine dip stick for nitrates: negative • Vaginal saline wet mount: vaginal pH was 4.5. Microscopy showed WBCs >10 per HPF, no clue cells, no trichomonads, and the KOH wet mount was negative for budding yeast and hyphae. 3. What is the presumptive diagnosis? 4. How should this patient be managed? 5. What is an appropriate therapeutic regimen? Case Study
  • 42. PID Curriculum 42 Partner Management Sex partner: Joseph (spouse) • First exposure: four years ago • Last exposure: one week ago • Frequency: two times per week (vaginal only) 6. How should Joseph be managed? Case Study
  • 43. PID Curriculum 43 Follow-Up • On follow-up three days later, Jane had improved clinically. The nucleic acid amplification test (NAAT) for gonorrhea was positive. The NAAT test for chlamydia was negative. • Joseph (Jane’s husband) came in with Jane at follow-up. He was asymptomatic but did admit to a "one-night stand" while traveling. He was treated. They were offered HIV testing which they accepted. 7. Who is responsible for reporting this case to the local health department? 8. What are appropriate prevention counseling recommendations for this patient? Case Study