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Roadmap. Breast Cancer Screening Colorectal Cancer Screening Cervical Cancer ScreeningAdult VaccinationsOsteoporosis ScreeningRecreational Activities"Lipid ScreeningAbdominal Aortic Aneurysm Screening. Breast Cancer. Projected 211,000 new cases in US and 40,400 deaths in women in 2005Secon
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1. Preventive Health Maintenance Common Ambulatory Topics
July 2007
Lisa L. Willett MD
J. R. Hartig MD
2. Roadmap Breast Cancer Screening
Colorectal Cancer Screening
Cervical Cancer Screening
Adult Vaccinations
Osteoporosis Screening
“Recreational Activities”
Lipid Screening
Abdominal Aortic Aneurysm Screening
3. Breast Cancer Projected 211,000 new cases in US and 40,400 deaths in women in 2005
Second cause of cancer related death in women
More common in older women
Risk 1 in 25 for ages 40-59
Risk 1 in 15 for ages 60-79
4. Question: Breast cancer screening 34 yoF presents for routine follow up. After spending the visit discussing her HTN and DM care, you turn to her health maintenance. She has a family history of breast cancer in her great aunt. You recommend which of the following?
Clinical breast exam
Screening mammography beginning at age 35
Screening mammography beginning at age 40
Screening mammography beginning at age 50
Screening breast ultrasound beginning at age 35
5. Methods of screening Clinical Breast Exam (CBE)
Breast Self Exam (BSE)
Mammography
6. Recommendations US Preventive Services Task Force (USPSTF)
Canadian Task Force of Preventive Health Care (CTFPHC)
Both evidence based, explicit methodology
Others: AMA, ACS, ACOG, AAFP
Literature review and expert opinion
7. Summary of Recommendations
8. USPSTF Grades and Recs
9. USPSTF Evidence is strongest for 50-69
Weaker for 40-49, but most studies show mortality benefit (but less than 50-69)
Difficult to account for delay in observed benefit
Insufficient evidence for optimal screening interval
Insufficient data for CBE, BSE (I)
10. Question: Breast cancer screening 34 yoF presents for routine follow up. After spending the visit discussing her HTN and DM care, you turn to her health maintenance. She has a family history of breast cancer in her great aunt. You recommend which of the following?
Clinical breast exam
Screening mammography beginning at age 35
Screening mammography beginning at age 40
Screening mammography beginning at age 50
Screening breast ultrasound beginning at age 35
11. Question: Breast cancer screening 34 yoF presents for routine follow up. After spending the visit discussing her HTN and DM care, you turn to her health maintenance. She has a family history of breast cancer in her great aunt. You recommend which of the following?
Clinical breast exam
Screening mammography beginning at age 35
Screening mammography beginning at age 40
Screening mammography beginning at age 50
Screening breast ultrasound beginning at age 35
12. FAQs When can I stop screening?
Evidence is strongest for 50-69
Can generalize to >70 without co-morbidities
higher absolute risk of breast cancer
What about high risk women (family history, previous abnormal breast biopsy, first childbirth >30)?
Start sooner, perhaps annually
13. Colorectal Cancer Epidemiology
3rd most common cancer in the U. S.
3rd leading cause of cancer death
At age 50 a person has 5% lifetime chance
Pathology
80% arise from adenomatous polyps
Screening Rates
~25% report FOBT in last 12 months
~38% report any form of endoscopy in 5 years 5% lifetime chance of being diagnosed with CR Ca
1 in 3 people who are diagnosed die from the disease
Average person dying with colorectal cancer loses 13 years of expected life
More than 80% of colorectal cancers arise from
adenomatous polyps. Although fewer than 1% of
adenomatous polyps less than 1 cm will eventually
develop into cancer, 10% of adenomatous polyps
greater than 1 cm become malignant within 10
years, and about 25% become malignant after 20
years.6 The prevalence of adenomatous polyps
increases from 20% to 25% at age 50 to 50% by age
75-80.5% lifetime chance of being diagnosed with CR Ca
1 in 3 people who are diagnosed die from the disease
Average person dying with colorectal cancer loses 13 years of expected life
More than 80% of colorectal cancers arise from
adenomatous polyps. Although fewer than 1% of
adenomatous polyps less than 1 cm will eventually
develop into cancer, 10% of adenomatous polyps
greater than 1 cm become malignant within 10
years, and about 25% become malignant after 20
years.6 The prevalence of adenomatous polyps
increases from 20% to 25% at age 50 to 50% by age
75-80.
14. Question: Colorectal Cancer According to USPSTF, which of the following strategies for colorectal cancer screening is acceptable?
Colonoscopy every 5-7 years after 50yo for low-risk individuals
Annual in-office DRE and FOBT after 50yo
Flex sig and DCBE every 5 years after 50yo
Annual home FOBT beginning age 50
Virtual colonoscopy every 10 years after 50yo
15. Methods of Screening FOBT should be used on three consecutive stool samples obtained at home by the patient and returned to the physician. Rehydration of samples increases sensitivity but also increases the false positive rates.
Sensitivity and specificity of a single test have been estimated at 40% and 96% to 98%, respectively. Hydration of specimen increases sensitivity (60%) but reduces specificity (90%).
Annual screening with hydrated specimens detected 49% of all incident cancers, but 38% of all subjects had at least 1 colonoscopy due to positive results. Programs using unrehydrated specimens and/or biennial testing detect a smaller proportion of cancers (27% to 39%) but require fewer colonoscopies (5% to 28%).
In 3 recent randomized trials, performing flexible sigmoidoscopy in addition to FOBT yielded approximately 7 additional cancers or large polyps per 1,000 patients compared to FOBT alone. Adding FOBT did not improve the yield over sigmoidoscopy alone at the initial screening in these studies, which used flexible sigmoidoscopy, but did in an earlier study that used rigid sigmoidoscopy.
Previous studies have reported high sensitivity (86% to 90%) of DCBE for colorectal cancer and polyps, and high specificity (95%). In the National Polyp Study, however, DCBE detected only 48% of polyps greater than 1 cm.15 Sensitivity might be higher in a typical screening population where the proportion of large polyps is higher. Specificity of DCBE in this study was 85%.
Neither DRE nor single office occult testing is recommended in colorectal cancer screening.
FOBT should be used on three consecutive stool samples obtained at home by the patient and returned to the physician. Rehydration of samples increases sensitivity but also increases the false positive rates.
Sensitivity and specificity of a single test have been estimated at 40% and 96% to 98%, respectively. Hydration of specimen increases sensitivity (60%) but reduces specificity (90%).
Annual screening with hydrated specimens detected 49% of all incident cancers, but 38% of all subjects had at least 1 colonoscopy due to positive results. Programs using unrehydrated specimens and/or biennial testing detect a smaller proportion of cancers (27% to 39%) but require fewer colonoscopies (5% to 28%).
In 3 recent randomized trials, performing flexible sigmoidoscopy in addition to FOBT yielded approximately 7 additional cancers or large polyps per 1,000 patients compared to FOBT alone. Adding FOBT did not improve the yield over sigmoidoscopy alone at the initial screening in these studies, which used flexible sigmoidoscopy, but did in an earlier study that used rigid sigmoidoscopy.
Previous studies have reported high sensitivity (86% to 90%) of DCBE for colorectal cancer and polyps, and high specificity (95%). In the National Polyp Study, however, DCBE detected only 48% of polyps greater than 1 cm.15 Sensitivity might be higher in a typical screening population where the proportion of large polyps is higher. Specificity of DCBE in this study was 85%.
Neither DRE nor single office occult testing is recommended in colorectal cancer screening.
17. Screening Methods and Trials FOBT should be used on three consecutive stool samples obtained at home by the patient and returned to the physician. Rehydration of samples increases sensitivity but also increases the false positive rates.
Sensitivity and specificity of a single test have been estimated at 40% and 96% to 98%, respectively. Hydration of specimen increases sensitivity (60%) but reduces specificity (90%).
Annual screening with hydrated specimens detected 49% of all incident cancers, but 38% of all subjects had at least 1 colonoscopy due to positive results. Programs using unrehydrated specimens and/or biennial testing detect a smaller proportion of cancers (27% to 39%) but require fewer colonoscopies (5% to 28%).
In 3 recent randomized trials, performing flexible sigmoidoscopy in addition to FOBT yielded approximately 7 additional cancers or large polyps per 1,000 patients compared to FOBT alone. Adding FOBT did not improve the yield over sigmoidoscopy alone at the initial screening in these studies, which used flexible sigmoidoscopy, but did in an earlier study that used rigid sigmoidoscopy.
Previous studies have reported high sensitivity (86% to 90%) of DCBE for colorectal cancer and polyps, and high specificity (95%). In the National Polyp Study, however, DCBE detected only 48% of polyps greater than 1 cm.15 Sensitivity might be higher in a typical screening population where the proportion of large polyps is higher. Specificity of DCBE in this study was 85%.
Neither DRE nor single office occult testing is recommended in colorectal cancer screening.
FOBT should be used on three consecutive stool samples obtained at home by the patient and returned to the physician. Rehydration of samples increases sensitivity but also increases the false positive rates.
Sensitivity and specificity of a single test have been estimated at 40% and 96% to 98%, respectively. Hydration of specimen increases sensitivity (60%) but reduces specificity (90%).
Annual screening with hydrated specimens detected 49% of all incident cancers, but 38% of all subjects had at least 1 colonoscopy due to positive results. Programs using unrehydrated specimens and/or biennial testing detect a smaller proportion of cancers (27% to 39%) but require fewer colonoscopies (5% to 28%).
In 3 recent randomized trials, performing flexible sigmoidoscopy in addition to FOBT yielded approximately 7 additional cancers or large polyps per 1,000 patients compared to FOBT alone. Adding FOBT did not improve the yield over sigmoidoscopy alone at the initial screening in these studies, which used flexible sigmoidoscopy, but did in an earlier study that used rigid sigmoidoscopy.
Previous studies have reported high sensitivity (86% to 90%) of DCBE for colorectal cancer and polyps, and high specificity (95%). In the National Polyp Study, however, DCBE detected only 48% of polyps greater than 1 cm.15 Sensitivity might be higher in a typical screening population where the proportion of large polyps is higher. Specificity of DCBE in this study was 85%.
Neither DRE nor single office occult testing is recommended in colorectal cancer screening.
18. Summary of Recommendations 1 http://www.ahrq.gov/clinic/3rduspstf/colorectal/colorr.pdf
19. USPSTF Clinical factors influencing recommendations:
Cost effectiveness – likely any strategy ok
Choice of strategy individualized based on patient and availability of services
Cost effective for prevention is generally defined as = $30,000 per additional year of life gained.
Cost effective for prevention is generally defined as = $30,000 per additional year of life gained.
20. Question: Colorectal Cancer According to USPSTF, which of the following strategies for colorectal cancer screening is acceptable?
Colonoscopy every 5-7 years after 50yo for low-risk individuals
Annual in-office DRE and FOBT after 50yo
Flex sig and DCBE every 5 years after 50yo
Annual home FOBT beginning age 50
Virtual colonoscopy every 10 years after 50yo
21. Question: Colorectal Cancer According to USPSTF, which of the following strategies for colorectal cancer screening is acceptable?
Colonoscopy every 5-7 years after 50yo for low-risk individuals
Annual in-office DRE and FOBT after 50yo
Flex sig and DCBE every 5 years after 50yo
Annual home FOBT beginning age 50
Virtual colonoscopy every 10 years after 50yo
22. Colorectal Cancer FAQs Screening for colon cancer should begin…?
Screen all adults beginning at age 50
Earlier if family history or personal risks exist
When can I stop screening?
FOBT has been proven effective 50-80yo
How should I screen for colorectal cancer?
Depends on patient and situation. Insurance!!!
At what interval should I screen for this method?
Depends on method used. FOBT q1, Flex sig q5, ACBE q5-10, Colon q10. There are few data to determine optimal age for starting or stopping screening. FOBT has been proven effective for persons aged 50-80 and sigmoidoscopy is associated with reduced mortality in persons older than 45. One cost-effectiveness model suggests that beginning screening at age 40 rather than at age 50 would offer less than a 1-day average improvement in life expectancy. Randomized trials suggest that a life expectancy of at least 5 years may be required to realize the benefits of screening.
There are few data to determine optimal age for starting or stopping screening. FOBT has been proven effective for persons aged 50-80 and sigmoidoscopy is associated with reduced mortality in persons older than 45. One cost-effectiveness model suggests that beginning screening at age 40 rather than at age 50 would offer less than a 1-day average improvement in life expectancy. Randomized trials suggest that a life expectancy of at least 5 years may be required to realize the benefits of screening.
24. Cervical Cancer 13,000 new cases and 4,100 deaths in the US in 2002
Mean age of diagnosis: 47 yrs
Risks: early onset of sexual activity, greater number of lifetime partners, HIV, cigarette smoking
25. HPV infection Human papilloma virus (HPV) necessary precursor plus host factors
High risk types 16,18
Peak incidence and prevalence in women <25, but most are transient
Less prevalent in older women
26. Question: Cervical cancer screening 22 yoF presents for primary care. She has been sexually active since 19, with 2-4 partners per year and uses oral contraception. Her college medical records show a normal pap 1 year ago. You recommend which of the following?
Cervical smear for HPV testing
Cervical smear for HSV testing
Colonoscopy
Pap smear now
Pap smear in three years
27. Summary of Recommendations
28. Cervical cytology: Pap Smear Sensitivity for single test is 60-80%
Most organizations recommend annual screening until 2-3 normal
29. Human papillomavirus (HPV) Human papillomavirus (HPV) testing
Limited evidence to determine risk/benefits
Trials underway will clarify
Useful in decision making for ASCUS
If HPV negative with ASCUS, annual screening
If HPV positive with ASCUS, refer for colposcopy
30. Question: Cervical cancer screening 22 yoF presents for primary care. She has been sexually active since 19, with 2-4 partners per year and uses oral contraception. Her college medical records show a normal pap 1 year ago. You recommend which of the following?
Cervical smear for HPV testing
Cervical smear for HSV testing
Colonoscopy
Pap smear now
Pap smear in three years
31. Question: Cervical cancer screening 22 yoF presents for primary care. She has been sexually active since 19, with 2-4 partners per year and uses oral contraception. Her college medical records show a normal pap 1 year ago. You recommend which of the following?
Cervical smear for HPV testing
Cervical smear for HSV testing
Colonoscopy
Pap smear now
Pap smear in three years
32. Cervical Cancer FAQs Do I screen women with a total hysterectomy?
NO, if done for benign purposes
Do I screen women never sexually active?
Although unlikely, most recommend screen >21
At what age can I stop doing pap smears?
If adequate prior screening, normal paps and not otherwise high risk: >65 USPSTF or >70 ACS
34. Adult Vaccinations Rates of immunization are improving?
1989 to 2003 in adults >65 years of age
Pneumococcal vaccine 15% to 64%
Influenza vaccine 33% to 70%
1995 data on younger adults 18-49 years old
12% with indications had received pneumococcal
20% with indications had received influenza
Tetanus/diphtheria
Only 47% adults had protective antibody levels Overall immunization rates are improving in older adults (age 65)
However rates in younger adults at risk for disease / with indications for vaccination are still poor
Adult rates lag behind pediatrics rates which are overall >80% and for many diseases well into the 90% range
Less than 500 children a year die from vaccine preventable illnesses.
In contrast it is estimated that between 50000 to 70000 adults die annually from these two vaccine preventable diseases.
Only 47% of adults >20 years old had protective antibody levels to both tetanus and diphtheria in a large serologic survey published in Annals in 2002. This is compared to 91% of children age 6-11yo. Overall immunization rates are improving in older adults (age 65)
However rates in younger adults at risk for disease / with indications for vaccination are still poor
Adult rates lag behind pediatrics rates which are overall >80% and for many diseases well into the 90% range
Less than 500 children a year die from vaccine preventable illnesses.
In contrast it is estimated that between 50000 to 70000 adults die annually from these two vaccine preventable diseases.
Only 47% of adults >20 years old had protective antibody levels to both tetanus and diphtheria in a large serologic survey published in Annals in 2002. This is compared to 91% of children age 6-11yo.
35. Advisory Committee on Immunization Practices (ACIP) Group of physicians/scientists at CDC
Responsible for vaccine recommendations
Schedules
Notification of changes / shortages
Reports published in MMWR
www.cdc.gov/mmwr
Generally in concert with other medical societies (ACP, AAP, ACOG, AAFP) Part of the CDC that produces the guidelines and recommends immunization schedules and practices in the US.
Morbidity and Mortality Weekly ReportPart of the CDC that produces the guidelines and recommends immunization schedules and practices in the US.
Morbidity and Mortality Weekly Report
36. The National Childhood Vaccine Injury Act of 1986 Requires healthcare providers to follow directives, record and maintain records and report adverse events
Provide appropriate Vaccine Information Statements (VIS)
Vaccine Adverse Event Reporting System
(VAERS) www.vaers.org (800) 822-7967
Vaccine Injury Compensation Program
www.hrsa.gov/osp/vicp (800) 338-2382 Requires health providers to provide VIS for all shots given during childhood. And Td. Influenza and Pneumococcal VIS are available but not required by law.
VAERS requires certain reactions to be reported to CDC. Other less serious reactions are optional to report.
VICP is a ‘no-fault’ system intended to compensate individuals that have had adverse reactions to vaccines. It was created to avoid civil litigations.Requires health providers to provide VIS for all shots given during childhood. And Td. Influenza and Pneumococcal VIS are available but not required by law.
VAERS requires certain reactions to be reported to CDC. Other less serious reactions are optional to report.
VICP is a ‘no-fault’ system intended to compensate individuals that have had adverse reactions to vaccines. It was created to avoid civil litigations.
37. Vaccine Information Sheets (VIS) Produced by the CDC and freely available over the internet in pdf format.
Use has been required since 1994Produced by the CDC and freely available over the internet in pdf format.
Use has been required since 1994
38. VIS – available in many languages The same Td VIS in Arabic
Reference for the other languages is provided at the end of this section and freely available on the internet in pdf formatting.The same Td VIS in Arabic
Reference for the other languages is provided at the end of this section and freely available on the internet in pdf formatting.
39. Question: Immunizations A 66yo M with a 7 year history of diet controlled-DM comes to your office for a routine visit. After providing appropriate care for his DM, you review his immunization record:
Last Pneumococcal vaccine: 7 years ago.
Last tetanus: he cannot recall, none documented
Your best plan today is:
Obtain old records and update shots at next visit
Td today, IM Flu if season, and Pneum. in 3 years
Td today, IM Flu if season, Pneum. today
Td today, Intranasal Flu if season, Pneum. today
Td later, Intranasal Flu if season, Pneum. in 3 years
40. Adult Immunization Schedule Only going to discuss the top three vaccines on the chart.
Other vaccines may be appropriate for individual patients but… that’s another noon conference in itself
In fact Dr. Stamm gave an excellent Update on Vaccines in May 2003 available at our website.
Only going to discuss the top three vaccines on the chart.
Other vaccines may be appropriate for individual patients but… that’s another noon conference in itself
In fact Dr. Stamm gave an excellent Update on Vaccines in May 2003 available at our website.
41. Pneumococcal Vaccines Capsular polysaccharide vaccine
First used in 1945
Currently use 23 valent vaccine (1983)
Pneumococcal Polysaccharide Vaccine (PPV23)
Nonrandomized studies – significant benefit
Cochrane Review1
not effective in preventing death or pneumonia
Does reduce invasive pneumococcal disease 1 Dear KB G, Andrews RR, Holden J, Tatham DP. Vaccines for preventing pneumococcal infection in adults. The Cochrane Database of Systematic Reviews 2003, Issue 4. Art. No.: CD000422. DOI: 10.1002/14651858.CD000422. First vaccine derived from a capsular polysaccharide.
First used in 1945 – which was around the same time as penicillin was discovered.
Originally not very popular because the prevailing thought was “Why give a vaccine when we have adequate antibiotics to treat the problem?”
Dr. Robert Austin in the 1970s promoted a 14 valent vaccine, which later evolved into the 23 valent vaccine that we now use since 1983
Pneumococcal Polysaccharide Vaccine 23 valent (PPV23)
More people die from pneumococal disease than any other vaccine preventable disease. Estimated to be 40,000 per year. Thought that as many as half of these deaths could be prevented with increased use of the PPV23.
Efficacy of 57%
Effects ages <2yo or >65yo primarily
Vaccination rates are improving 1989 15% to 2003 64%
2 available preparations Merck: Pneumovax. Lederle: Pnu-Immune 23 with phenol or thimerosal as a preservative
Efficacy
Nonrandomized studies have demonstrated significant benefit:
Cochrane Review mention also
Efficacy of 50% then corresponds to a number-needed-to-treat (NNT) of 20,000 vaccinations per infection avoided, and perhaps 50,000 per death avoided.
First vaccine derived from a capsular polysaccharide.
First used in 1945 – which was around the same time as penicillin was discovered.
Originally not very popular because the prevailing thought was “Why give a vaccine when we have adequate antibiotics to treat the problem?”
Dr. Robert Austin in the 1970s promoted a 14 valent vaccine, which later evolved into the 23 valent vaccine that we now use since 1983
Pneumococcal Polysaccharide Vaccine 23 valent (PPV23)
More people die from pneumococal disease than any other vaccine preventable disease. Estimated to be 40,000 per year. Thought that as many as half of these deaths could be prevented with increased use of the PPV23.
Efficacy of 57%
Effects ages <2yo or >65yo primarily
Vaccination rates are improving 1989 15% to 2003 64%
2 available preparations Merck: Pneumovax. Lederle: Pnu-Immune 23 with phenol or thimerosal as a preservative
Efficacy
Nonrandomized studies have demonstrated significant benefit:
Cochrane Review mention also
Efficacy of 50% then corresponds to a number-needed-to-treat (NNT) of 20,000 vaccinations per infection avoided, and perhaps 50,000 per death avoided.
42. Indications for Pneumococcal Vaccine Adapted from MMWR 2003; 52:739-40 Asthma – Yes for flu. No for Pneumococcal
Functional or anatomic asplenia (i.e. patients with sickle cell disease)
No one should receive more than 2 doses of the vaccine unless they started as a child <10 years old
Contraindications include:
Previous anaphylactic reaction to vaccine or component
Relative contraindication during pregnancyAsthma – Yes for flu. No for Pneumococcal
Functional or anatomic asplenia (i.e. patients with sickle cell disease)
No one should receive more than 2 doses of the vaccine unless they started as a child <10 years old
Contraindications include:
Previous anaphylactic reaction to vaccine or component
Relative contraindication during pregnancy
43. Influenza Vaccines Epidemiology
Annually 36,000 deaths/year in 1990-1999
Complications highest in = 2yo, = 65yo and individuals with certain diseases (DM, asthma)
School absenteeism >25%, Lost work productivity, increased medical burden
Vaccine products
Whole virus vs Split product - intramuscular
Live attenuated influenza vaccine (LAIV) In the US accounts for approx. 36,000 deaths/year during the 1990s.
90% of those deaths occurred in people older than 65years
However during the last pandemics of flu, those 18-65 accounted for nearly half of deaths (1972)
30 million seek medical care for the flu each year
300K hospitalizations for flu related illnesses.
Tremendous cost to the US each year.
Children have the highest rates of infection overall for any age groups but complications such as hospitalization, pneumonia and death occur primarily in individuals less than 2 or older than 65.
Both whole virus and split product vaccines are appropriate for use in adults and children over the age of 12. Whole virus vaccines tend to cause a greater reaction in children under 12 though.
But for us, it is little concern as only split product vaccines are available currently in the US.
LAIV is approved for use in healthy individuals 5-49 years of age.
Inactivated intramuscular vaccine is for 6 months and older.
In 2005 there will be a thimerosal-free vaccine for influenza available.
When the vaccine and circulating viruses are antigenically similar, influenza vaccine prevents influenza illness among approximately 70%–90% of healthy adults aged <65 years. Vaccination of healthy adults also has resulted in decreased work absenteeism and decreased use of health-care resources, including use of antibiotics, when the vaccine and circulating viruses are well-matched.
In a randomized study among children aged 1–15 years, inactivated influenza vaccine was 77%– 91% effective against influenza respiratory illness and was 44%–49%, 74%–76%, and 70%–81% effective against influenza seroconversion among children aged 1–5, 6–10, and 11–15 years, respectively.
In the US accounts for approx. 36,000 deaths/year during the 1990s.
90% of those deaths occurred in people older than 65years
However during the last pandemics of flu, those 18-65 accounted for nearly half of deaths (1972)
30 million seek medical care for the flu each year
300K hospitalizations for flu related illnesses.
Tremendous cost to the US each year.
Children have the highest rates of infection overall for any age groups but complications such as hospitalization, pneumonia and death occur primarily in individuals less than 2 or older than 65.
Both whole virus and split product vaccines are appropriate for use in adults and children over the age of 12. Whole virus vaccines tend to cause a greater reaction in children under 12 though.
But for us, it is little concern as only split product vaccines are available currently in the US.
LAIV is approved for use in healthy individuals 5-49 years of age.
Inactivated intramuscular vaccine is for 6 months and older.
In 2005 there will be a thimerosal-free vaccine for influenza available.
When the vaccine and circulating viruses are antigenically similar, influenza vaccine prevents influenza illness among approximately 70%–90% of healthy adults aged <65 years. Vaccination of healthy adults also has resulted in decreased work absenteeism and decreased use of health-care resources, including use of antibiotics, when the vaccine and circulating viruses are well-matched.
In a randomized study among children aged 1–15 years, inactivated influenza vaccine was 77%– 91% effective against influenza respiratory illness and was 44%–49%, 74%–76%, and 70%–81% effective against influenza seroconversion among children aged 1–5, 6–10, and 11–15 years, respectively.
44. Indications for Influenza Vaccine * If 6mo=x<9yo and first-ever dose, repeat in 1 month. <36 mo use 0.25ml dose. If LAIV 2nd dose 6-10wks later
Adapted from MMWR June 29, 2007 internet release These recommendations are from the MMWR just released the week of July 13th for the upcoming 2005-06 flu season.
Vaccination is associated with reductions in influenza-related respiratory illness and physician visits among all age groups, hospitalization and death among persons at high risk, otitis media among children, and work absenteeism among adults.
Added this year are individuals with spinal cord injuries, neuromuscular diseases, aspiration syndromes, seizure disorder or any condition that can impair respiratory function or clearance of secretions.
TABLE 4. Inactivated influenza vaccine* dosage, by age group
— United States, 2005–06 season
Age group† Dose No. of doses Route§
6–35 mos 0.25 mL 1 or 2¶ Intramuscular
3–8 yrs 0.50 mL 1 or 2¶ Intramuscular
>9 yrs 0.50 mL 1 IntramuscularThese recommendations are from the MMWR just released the week of July 13th for the upcoming 2005-06 flu season.
Vaccination is associated with reductions in influenza-related respiratory illness and physician visits among all age groups, hospitalization and death among persons at high risk, otitis media among children, and work absenteeism among adults.
Added this year are individuals with spinal cord injuries, neuromuscular diseases, aspiration syndromes, seizure disorder or any condition that can impair respiratory function or clearance of secretions.
TABLE 4. Inactivated influenza vaccine* dosage, by age group
— United States, 2005–06 season
Age group† Dose No. of doses Route§
6–35 mos 0.25 mL 1 or 2¶ Intramuscular
3–8 yrs 0.50 mL 1 or 2¶ Intramuscular
>9 yrs 0.50 mL 1 Intramuscular
45. Contraindications to Influenza Vaccine Anaphylactic hypersensitivity to eggs
Anaphylactic history to vaccine or component
Acute febrile illness (relative)
Guillain-Barré syndrome
1976 swine influenza vaccine
High risk – probably vaccinate; low risk – probably not
No LAIV – if age <5 or >50, or essentially any true indication to receive influenza vaccine 1976 vaccine had increased association with GBS.
Annual rate of GBS is 10-20cases/1million
Subsequent studies have failed to demonstrate an association except one study of the 1992-93, 1993-94 seasons with the overall RR of 1.7 (95% CI 1.0 to 2.8 p=0.04) representing approx 1 additional case per 1 million vaccinated.
Recent data from VAER system have documented decreased occurences with increasing immunization rates.1976 vaccine had increased association with GBS.
Annual rate of GBS is 10-20cases/1million
Subsequent studies have failed to demonstrate an association except one study of the 1992-93, 1993-94 seasons with the overall RR of 1.7 (95% CI 1.0 to 2.8 p=0.04) representing approx 1 additional case per 1 million vaccinated.
Recent data from VAER system have documented decreased occurences with increasing immunization rates.
46. Indications for Tetanus Vaccine Described by Esdall in 1976 as “The inexcusable disease”
Incidence in the US 0.16 per million (43/year) Wonderful case review and comments by Drs. Smallheiser and Deb Levine in the Annals not too long ago.
Annual incidence of 0.16/million or about 43 cases per year.
But very poor levels of immunity in the elderly – who are also at great risk of disease.
Contraindications are primarily related to sever hypersensitivity to vaccine or its components in pastWonderful case review and comments by Drs. Smallheiser and Deb Levine in the Annals not too long ago.
Annual incidence of 0.16/million or about 43 cases per year.
But very poor levels of immunity in the elderly – who are also at great risk of disease.
Contraindications are primarily related to sever hypersensitivity to vaccine or its components in past
47. Stop sign insertStop sign insert
48. Tdap Don’t forget…
Everyone should receive one Tdap in place of the usual Td booster vaccine…
49. Question: Immunizations A 66yo M with a 7 year history of diet controlled-DM comes to your office for a routine visit. After providing appropriate care for his DM, you review his immunization record:
Last Pneumococcal vaccine: 7 years ago.
Last tetanus: he cannot recall, none documented
Your best plan today is:
Obtain old records and update shots at next visit
Td today, IM Flu if season, and Pneum. in 3 years
Td today, IM Flu if season, Pneum. today
Td today, Intranasal Flu if season, Pneum. today
Td later, Intranasal Flu if season, Pneum. in 3 years
50. Question: Immunizations A 66yo M with a 7 year history of diet controlled-DM comes to your office for a routine visit. After providing appropriate care for his DM, you review his immunization record:
Last Pneumococcal vaccine: 7 years ago.
Last tetanus: he cannot recall, none documented
Your best plan today is:
Obtain old records and update shots at next visit
Td today, IM Flu if season, and Pneum. in 3 years
Tdap today, IM Flu if season, Pneum. today
Td today, Intranasal Flu if season, Pneum. today
Td later, Intranasal Flu if season, Pneum. in 3 years
51. Common Resources Internet
www.immunize.org
www.cdc.gov
Palm OS Based and PC versions
Shots 2007
52. Question: Osteoporosis screening 58 yo AAF postmenopausal for 3 years, presents for routine visit without complaint. In regards to osteoporosis screening, which of the following are true?
She needs a DEXA now
She needs 1200 mg of Calcium daily
She needs a DEXA at age 60
She needs a DEXA at age 65
53. Osteoporosis Screening Women aged 65 and older (B)
Begin at age 60 if increased risk (B)
Weight <70kg (154 lbs)- single best predictor
Smoking, family history, alcohol, caffeine, low calcium/vitamin D
DEXA minimum of 2 years
No data on when to stop
54. Question: Osteoporosis screening 58 yo AAF postmenopausal for 3 years, presents for routine visit without complaint. In regards to osteoporosis screening, which of the following are true?
She needs a DEXA now
She needs 1200 mg of Calcium daily
She needs a DEXA at age 60
She needs a DEXA at age 65
55. Question: Osteoporosis screening 58 yo AAF postmenopausal for 3 years, presents for routine visit without complaint. In regards to osteoporosis screening, which of the following are true?
She needs a DEXA now
She needs 1200 mg of Calcium daily
She needs a DEXA at age 60
She needs a DEXA at age 65
56. “Recreational Activities” Sexually Transmitted Diseases
Tobacco
Alcohol
Seat Belts
57. Question: STDs A 24 yoF presents to your clinic asking for a refill of birth control pills. She is monogamous with one partner. She denies h/o STDs, vaginal discharge, or other symptoms and has no PMH. You recommend which of the following?
Mammogram
Clinical breast exam
Chlamydia screening
Gonorrhea screening
HIV screening
58. STDs Chlamydia
ALL sexually active women aged 24 or less regardless of symptoms (A)
ALL ages women at increased risk (A)
Insufficient evidence for asymptomatic men (I)
Gonorrhea
All sexually active women if increased risk (B)
Insufficient evidence for men at risk (I)
HIV & syphilis at increased risk & pregnant (A)
59. Universal HIV screening? September 2006, CDC published
All individuals age 13-64 be screened for HIV regardless of risk*
USPSTF reviewed the quality and strength of the evidence and maintains C (no recommendation) for those not at increased risk
60. Question: STDs A 24 yoF presents to your clinic asking for a refill of birth control pills. She is monogamous with one partner. She denies h/o STDs, vaginal discharge, or other symptoms and has no PMH. You recommend which of the following?
Mammogram
Clinical breast exam
Chlamydia screening
Gonorrhea screening
HIV screening
61. Question: STDs A 24 yoF presents to clinic asking for a refill of birth control pills. She is monogamous with one partner. She denies h/o STDs, vaginal discharge, or other symptoms and has no PMH. You recommend which of the following?
Mammogram
Clinical breast exam
Chlamydia screening
Gonorrhea screening
HIV screening
62. Tobacco, alcohol, seat belts Tobacco
Screen all adult patients, including pregnant women, and provide cessation interventions (A)
Alcohol
Screen all adult patients, including pregnant women, and provide cessation interventions (A)
Seat belts (B)
64. Lipid Background Why screen?
Primary and secondary prevention trials for CHD
Epidemiology
Prevalence estimated at 17.5% of men, 20% of women had total cholesterol (TC) = 240
According to
National Center for Health Statistics data from 1988
to 1994, 17.5% of men and 20% of women aged 20
to 74 years had high levels of TC (240 mg/dL or greater)
According to
National Center for Health Statistics data from 1988
to 1994, 17.5% of men and 20% of women aged 20
to 74 years had high levels of TC (240 mg/dL or greater)
