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OPPORTUNISTIC INFECTIONS
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Title: OPPORTUNISTIC INFECTIONS
1
OPPORTUNISTIC INFECTIONS IN HIV/AIDS
PATIENTS ITS MANAGEMENT.
Dr.K.SREEKANTHAN,
ASSOCIATE PROFESSOR HEAD DPT.OF
INFECTOUS DISEASES
2
HISTORY
- ACQUIRED IMMUNODEFICIENCY SYNDROM (AIDS)
- Â Â Â Â FIRST DESCRIBED IN 5 YOUNG HOMOSEXUAL MEN IN
U.S.A.IN I981. - Â Â PNEUMOCYSTIS CARINII PNEUMONIA KAPOSI'S
SARCOMA WERE DETECTED. - Â Â THE DISEASE IS CHARACTERIZED BY DEPLETION OF
THE IMMUNE CELLS. - CD4 LYMPHOCYTES,THE BANDMASTER OF IMMUNE
SYSTEM.
3
- THE CAUSATIVE AGENT WAS IDENTIFIED IN 1983-84 IN
FRANCE AND USA. - FIRST CALLED AS HTLV-III BY ROBERT HALLOW OF
USA. - THE VIRUS SUBSEQUENTLY NAMED AS HUMAN
IMMUNODEFICIENCY VIRUS(HIV) - IN 1985,THE DIAGNOSTIC KITS BASED ON DETECTION
OF ANTIBODIES AGAINST HIV WAS DISCOVERED.
4
- THE FIRST DRUG ZIDOVUDINE AFFECTING THE VIRUS WAS
DISCOVERED IN 1987. - IN INDIA ,THE DISEASE WAS DETECTED IN 1986.
- THE LATEST ESTIMATE DECEMBER 2003. 40 MILLION
PEOPLE LIVING WITH IV/AIDS. 95 OF THEM IN
DEVELOPING COUNTRIES. - ABOUT 14,000 NEW INFECTIONS OCCUR DAILY.
5
COMMON OI'S IN AIDS PATIENTS
- TUBERCULOSIS BOTH PULMONARY AND EXTRA PULMONARY.
- OROPHARYNGEAL CANDIDIASIS
- HERPES ZOSTER.
- TOXOPLASMOSIS.
- CRYPTOCOCCAL MENINGITIS
- PNEUMOCYSTIS CARINII PNEUMONIA.
- CYTOMEGALOVIRUS RETINITIS.
- CRYPTOSPORIDIAL DIARRHOEA
6
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7
THE COURSE OF INFECTION
- MAY VARY-SOME INDEVIDUALS DEVELOPING
IMMUNODEFICIENCY WITHIN 2 TO 3 YEARS. - OTHERS REMAINING AIDS FREE FOR 10-15 YEARS.
- THE MANIFESTATIONS OF INFECTIONS IN HIV/AIDS
PATIENTS DEPEND ON THE LEVEL OF IMMUNITY. - THIS IS REFLECTED BY THE CD4 T CELL COUNT.
- MAJORITY OF INFECTIONS OCCUR WHEN THE CD4 COUNT
FALLS BELOW 500 CELLS/ MM3.
8
EARLY DISEASE.(CD4 COUNT gt500 CELLS/CMM)
- MAJORITY GENERALLY NO SYMPTOMS.
- SEBORRHIC DERMATITIS
- PRURITIC FOLLICULITIS
- RARELY HSV,VZV, EBV INFECTIONS.
9
MIDDLE STAGE DISEASE ( CD4 COUNT 200-500 CELLS/
CMM)
- MAJORITY ASYMPTOMATIC OR ONLY MILD DISEASE
MANIFESTATIONS. - SEBORRHIC DERMATITIS
- FOLLICULITIS.
- RECURRENT HERPES SIMPLEX INFECTIONS
- ORAL HAIRY LEUKOPLAKIA.
- SHINGLES.
10
- OROPHARYNGEAL OR VAGINAL CANDIDIASIS.
- BACTERIAL INFECTIONS LIKE SINUSITIS,BRONCHITIS,
OR PNEUMONIA - TUBERCULOSIS
- SALMONELLOSIS.
- RARELY PCP.
11
LATE DISEASE ( CD4 COUNT 50-200 CELLS/CMM)
- ALL PATIENTS IN THIS GROUP ARE
- DEFINED AS HAVING AIDS.
- PATIENTS ARE AT HIGH RISK OF DEVELOPING
- TUBERCULOSIS.
- PCP.
- TOXOPLASMA GONDI ENCEPHALITIS
- ESOPHAGEAL CANDIDIASIS.
- CYTOMEGALOVIRUS INFECTION.
12
- CRYPTOSPORIDIASIS
- ISOSPORIASIS.
- HUMAN PAPILLOMA VIRUS ASSOCIATED MALIGNANCIES.
- CERVICAL CANCER IN WOMEN CARCINOMA RECTUM IN
MEN. - MYCOBACTERIUM AVIUM COMPLEX (MAC).
- CRYPTOCOCCUS
- HISTOPLASMOSIS
- NOCARDIA
- ASPERGILLUS
- LYMPHOMA,KAPOSIS SARCOMA,
- PROGRESSIVE MULTIFOCAL LEUCOENCEHALOPATHY(PML)
-J.C VIRUS.
13
ADVANCED HIV DISEASE. CD4 COUNTS lt 50 CELLS/ CMM.
- CYTOMEGALOVIRUS RETINITIS.
- Â DISSEMINATED MYCOBACTERIUM AVIUM
- COMPLEX Â DISEASE CRYPTOCOCCAL
- MENINGITIS.
- Â Â Â Â Â Â Â PROGRESSIVE MULTIFOCAL
- LEUCOENCEPHALOPATHY.
- Â Â Â Â Â Â Â INVASIVE ASPERGILLOSIS.
- Â Â Â Â Â Â Â DISSEMINATED HISTOPLASMOSIS
- Â Â Â Â Â Â Â DISSEMINATED COCCIDIOIDOMYCOSIS.
- Â Â Â Â Â Â Â INVASIVE PENICILLIUM MARNEFFI DISEASE.
14
COMMON OI'S IN AIDS PATIENTS
- TUBERCULOSIS BOTH PULMONARY AND
- EXTRA PULMONARY.
- OROPHARYNGEAL CANDIDIASIS
- HERPES ZOSTER
- HERPES SIMPLEX.
- Â TOXOPLASMOSIS.
- Â CRYPTOCOCCAL MENINGITIS
- Â PNEUMOCYSTIS CARINII PNEUMONIA.
- Â CYTOMEGALOVIRUS RETINITIS
15
   PNEUMOCYSTIS CARINII PNEUMONIA
- INITIALLY DESCRIBED IN 1909 BY CHAGAS.
- INITIALLY CONSIDERED AS A PROTOZOA
- NOW INCLUDED UNDER FUNGUS ASCOMYCETES YEASTS.
- UNTIL 1980 OCCURED SPORADICALLY IN
- IIMMUNOCOMPROMISED PATIENTS ON CANCER
CHEMOTHERAPY,LYMPHOMAS, MARASMIC CHILDREN ,
B.M.TRANSPLANTS. - WITH THE BEGINNING OF AIDS IN 1981 AN EXPLOSION
OF CASES OF PCP.
16
PATHOGENESIS
- AIR-BORN TRANSMISSION.
- NO CLINICAL INFECTION IN IMMUNOCOMPETENT.
- ATTACHES TO TYPE1 PNEUMOCYTES OF ALVEOLI AND
CAUSE - EXUDATIVE REACTION IMPAIRING GAS EXCHANGE.
17
INCIDENCE
- COMMONEST RESPIRATORY INFECTION EARLIER IN AIDS
- INCIDENCE CAME DOWN WITH P.PROPHYLAXIS A.R.T.
18
CLINICAL PRESENTATION
- Â FEVER,COUGH,DYSPNOEA,SPUTUM,
- CHEST PAIN.
19
RADIOLOGY
- DIFFUSE ALVEOLAR OR INTERSTITIAL PULMONARY
INFILTRATES - HRCT FINE DIFFUSE ALVEOLAR CONSOLIDATION WITH
BRONCHIAL WALL THICKENING.
20
DIAGNOSIS.
- BRONCHO ALVEOLAR LAVAGE
- Â Â SPUTUM INDUCTION.
- TRANSBRONCHIAL BIOPSY.
- STAINIG FOR P.CARINII.
- Â Â MOLECULAR IDENTIFICATION.
21
TREATMENT-FIRST LINE.
- TMP-SMX- IS THE DRUG OF CHOICE.
- TRIMETHOPRIM 20MG/KG/D
- SMX100MG/KG/D IN 3-4 DEVIDED DOSE.x 21 DAYS.
ROUTE ORAL OR IV. - ORAL 5-6 DS TABLETS DAILY FOR ADULTS
22
SECOND LINEÂ Â
PENTAMIDINE4MG/KG/D, INFUSED OVER 1H
ONCE DAILY X 21 DAYS.
23
ALTERNATIVE THERAPIES
- TRIMETHOPRIM-DAPSONE
- TRIMETHOPRIM20MG/KG/D IN 3 DEVIDED DOSE
DAPSONE 100MG x 21DAYS ORAL. - CLINDAMYCIN 600-900 MG IV EVERY 6-8H OR 300-450
MG ORALLY PRIMAQUIN,15-30 MG ORALLY x 21DAYS - ATAVAQUONE 750MG TIDx21 DAYS ORALLY.
- TRIMETHOTREXATE45MG/M2X21 DAYS IV LEUCOVORIN 20
MG /M2 4 TIMES DAILY
24
CORTICOSTEROIDS
- ORAL OR IV STEROIDS SHOULD BE GIVENT O ALL HIV
PATIENTS WITH MODERATE OR SEVERE PCP (WITH A
PO2lt70mmHg). - 4 CONTROLLED STUDIES ESTABLISHED
- THAT ADDITION OF STEROIDS WITHIN 72H OF
BEGINNING CONVENTIONAL THERAPY IMPROVES OUTCOME
AND REDUCES MORTALITY. - BETTER TO START WITH INITIATION OF ANTI PCP
THERAPY - PREDNISOLONE 40MG ORALLY BD/D x 5d THEN 20MG BD/D
x5d THEN 20MG OD UNTIL COMPLETION OF ANTI PCP
THERAPYÂ Â Â . - IF PARENTERAL THERAPY IS INDICATED
- METHYLPREDNISOLONE 75 OF ABOVE RECOMMENDED
DOSE.
25
PROPHYLAXIS-
- PRIMARY PROPHYLAXIS
- SECONDARY PROPHYLAXIS.
26
INDICATIONS FOR PROPHYLAXIS
- CD4 COUNT lt 200CELLS/Cmm.
- Â Â UNEXPLAINED FEVER gt100DF FORgt2W.
- Â Â HISTORY OF OROPHARYNGEAL CANDIDIASIS.
- Â Â Â PRIOR EPISODE OF PCP.
27
PREFERRED REGIMEN
- TMP-SMX IS THE DRUG OF CHOICE.
- Â Â 1 DOUBLE STRENGTH TABLET
- DAILY (160mg OF TMP 800mg SMX).
28
TUBERCULOSIS
- THE MOST COMMEN OI IN HIV/AIDS PATIENT
- Â THE AIDS PANDEMIC HAS STALLED THE
- ELIMINATION OF TB IN USA.
- Â HIV MOST SIGNIFICANT RISK FACTOR FOR
- PROGRESSION OF LATENT M.TUBERCULOSIS
- INFECTION TO ACTIVE TB.
- 10 OF PERSONS INFECTED WITH M.TB WILL
- DEVELOP ACTIVE TB IN LIFE TIME.
- IN HIV INFECTED AS MANY AS 50 WILL
- DEVELOP ACTIVE TB DURING A SHORTENED
- LIFETIME
29
CLINICAL PRESENTATION
- ASSOCIATED WITH INCREASED TUBERCULOUS
DISSEMINATION. - Â Â AN INCREASE IN THE NUMBER SEVERITY OF
SYMPTOMS. - Â Â RAPID PROGRESSION TO DEATH UNLESS TREATMENT IS
BEGUN.
30
SITES OF DISEASE
- PULMONARY TB IN 70-90 OF HIV PTS. MOSTLY
ASSOCIATED WITH EXTRA PULMONARY. - Â Â DISSEMINATED TB AND LYMPHADENITIS ARE THE
MOST COMMON EXTRA PULMONARY. - Â Â CERVICAL AXILLARY COMMONLY AFFECTED WITH
TENDENCY TO CASEATE. - Â INTRATHORACIC INTRAABDOMINAL TB
- LYMPHADENITIS ARE PARTICULARLY
- COMMON
- Â Â CNS TB OCCURS IN 5-10 AS MENINGITIS
- TUBERCULOMAS.
31
OTHER SITES
- PLEURA, PERICARDIUM, B.MARROW
- SKIN, G.U TRACT, LIVER, ADRENALS.
32
RADIOLOGY
- RATHER THAN HAVING APICAL DISEASE AND CAVITY
DISEASE MAY REVEALADENOPATHY-(HILAR,MEDIASTINAL,PA
RATRACHEAL), - Â Â ATYPICAL INFILTRATES,P.EFFUSIONS, MILIARY
DISEASE, OR NO ABNORMALITY AT ALL. - Â Â SPUTUM SMEARS MAY LESS COMMONLY BE AFB VE.
33
DIAGNOSIS
- DEMONSTRATION OF AFB IN SPUTUM. RESULT MAY VARY
FROM 20-80 - Â Â CULTURE OF SPUTUM, URINE, BLOOD, CSF, P.FLUID,
PURULENT MATERIAL, BIOPSY MATERIAL. - Â DNA PROBES. PCR.
34
TREATMENT
- HIV-RELATED IMMUNOSUPPRESSION DOES NOT INTERFERE
WITH THE INITIAL EFFECTIVENESS OF ANT-TB THERAPY. - Â Â TREATMENT OF HIV-INFECTED TB PATIENTS IS
IDENTICAL TO THAT OF HIV-NEGATIVE. - Â Â BECAUSE OF WEAKER IMMUNE SYSTEM, IT IS
PARTICULARLY IMPORTANT THAT TREATMENT
RECOMMENDATIONS BE FULLY ADHERED TO. - Â Â ALSO APPEAR MORE SUSCEPTIBLE TO DEVELOPING
DRUG RESISTANT STRAINS OF THE DISEASE. - Â Â FOR THESE REASONS, PATIENTS WITH HIV SHOULD
RECEIVE TREATMENT WITH DOTS.
35
CAUSES OF FAILURED THERAPY
- Â DRUG RESISTANCE.
- Â Â Â Â POOR ADHERENCE TO THERAPY.
- Â Â Â Â Â MALABSORPTION OF ANTI TB DRUGS.
- Â Â Â Â FAILURE TO DRAIN TUBERCULOUS
- ABSCESSES.
- Â Â Â Â Â UNEXPLAINED TREATMENT FAILURE
- RELAPSE.
36
PREFERRED REGIMEN
- SHORT COURSE CHEMOTHERAPY INCLUDING
- INH, RIFAMPICIN, ETHAMBUTOL, PZA, STREPTOMYCIN IS
THE PREFERRED ONE. - Â DIRECTLY OBSERVED TREATMENT (DOT) SHOULD BE
CONSIDERES FOR ALL PATIENTS WITH TB. - Â DURATION OF TREATMENT 6-9 MONTHS.
- Â THE DURATION OF THERAPY CAN BE INDEVIDUALIZED
DEPENDING ON THE SEVERITY OF TB,SEVERITY OF
IMMUNO-DEFICIENCY, INITIAL RESPONSE TO THERAPY, - DROG TOXICITY CONSEQUENCES TO THE PATIENT.
37
MOST OF THE PATIENTS WITH HIV AND TB COME UNDER
CATEGORY I.
- NEW SMEAR -POSITIVE.
- Â NEW SMEAR-NEGATIVE.(SERIOUSLY ILL).
- Â Â EXTRA-PULMONARY(SERIOUSLY ILL).
- Â THESE ARE MENINGITIS, DISSEMINATED TB,
38
- TUBERCULOUS PERICARDITIS, PERITONITIS,
- Â Â BILATERAL OR EXTENSIVE PLEURISY,
- Â SPINAL TB WITH NEUROLOGICAL COMPLICATIONS, AND
INTESTINAL GENITO-URINARY TB. - Â Â Â Â Â Â Â Â Â Â Â Â Â Â
39
RNTCP TREATMENT REGIMEN
                   INTENSIVE PHASE
2(HRZE)3. Â Â Â Â Â Â Â Â Â Â Â Â CONTINUATION PHASE
4(HR)3. Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â H ISONIAZID
(600MG), Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â R RIFAMPICIN (450
MG), Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Z PYRAZINAMIDE
(1500MG), Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â E ETHAMBUTOL
(1200MG). Â Â Â TREATMENT FOR 2 MONTHS 3
DOSES PER WEEK FOLLOWED BY 4 MONTH TREATMENT WITH
ISONIAZID AND RIFAMPICIN.
40
DRUG TOXICITY AND INTERACTIONS
- Â AS MANY AS 20-30 MAY DEVELOP ADVERSE
REACTIONS PROMPTING A CHANGE IN THERAPY. - Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â RASH HEPATITIS .
- Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â GIT DISTURBANCES.
- RIFAMPICIN IS APOTENT INDUCER OF THE HEPATIC
CYTOCHROME P450 ENZYME SYSTEM IN HUMANS. - Â Â RIFAMPICIN THUS REDUCES THE ACTIVITY OF
SEVERAL MEDICATIONS COMMONLY USED IN HIV INFECTED
PATIENTS( FLUCONAZOLE,ART) -
41
FUNGAL INFECTIONS
- A MAJOR CAUSE OF MORBIDITY MORTALITY
- IN PATIENTS WITH HIV INFECTION.
- Â Â Â Â Â CANDIDA AND CRYPTOCOCCUS ARE THE MOST
- COMMON CAUSES OF MYCOTIC DISEASES.
- CANDIDIASIS-
- Â Â Â Â Â MOST COMMON FUNGAL INFECTION OBSERVED
- IN HIV-INFECTED PATIENTS.
- Â Â Â Â Â DISEASE OF M.MEMBRANE OCCURS INgt90 OF
- PATIENTS AT SOME POINT IN THEIR ILLNESS.
42
C.MANIFESTATIONS
- ORAL CANDIDIASIS-ONE OF THE INITIAL
- MANIFESTIONS.
- Â INCIDENCE INCREASES WHEN CD4 COUNT FALL BELOW
200-300/CMM. - Â Â CAN OCCUR REGARDLESS OF CD4 COUNT ALSO.
- Â Â Â OESOPHAGEAL CANDIDIASIS-AN AIDS DEFINING
ILLNESS. OCCURS MOSTLY IN PATIENTS WITH CD4lt
100/CMM. - Â Â Â MAY BE ASYMPTOMATIC,BUT MORE COMPLAIN OF
ODYNOPHAGIA,
43
OTHER MANIFESTATIONS
- VAGINAL CANDIDIASIS.
- Â Â PULMONARY INVOLVING, TRACHEA, BRONCHI, AND
LUNG CAN OCCUR AS A LATE OR TERMINAL
MANIFESTION. - Â Â Â INVASIVE CANDIDIASIS IS RARE IN HIV
- INFECTED PATIENTS.
- Â Â Â RARELY HEART,CNS EYES AFFECTED.
44
DIAGNOSIS
- CHARACTERISTIC APPEARANCE.
- Â Â Â DEMONSTRATION OF THE ORGANISM.
45
TREATMENT
- TOPICAL CLOTRIMAZOLE.
- Â Â Â Â SYSTEMIC TREATMENT IS PREFERRED IN
- MANY PATIENTS.
- Â Â Â Â ORALFLUCONAZOLE 100-200MG DAILY
- ORALLY.
- Â Â Â ITRACONAZOLE 200 MG DAILY.
- USUALLY GIVEN FOR 10-14 DAYS.
46
 ESOPHAGEAL AND ADVANCED INFECTION
- INITIAL IV FLUCONAZOLE 200-400 MG DAILY Â FOLLOWED
BY ORAL TREATMENT FOR 14-28DAYS. - Â Â IN ADVANCED DISESE AND RESISTANT CASES,
AMPHOTERICIN MAY BE NECESSARY. - Â Â 0.5MG/KG 20-30MG/DAY IV INFUSION FOR 7-14
DAYS.
47
PROPHYLAXIS
- ROUTINE PROPHYLAXIS FOR ORAL AND VAGINAL
CANDIDIASIS IS NOT RECOMMENDED BECAUSE OF THE
EMERGENCE OF DRUG RESISTANCE. - Â Â IF RECURRENCE IS FREQUENT OR SEVERE TOPICAL OR
ORAL TREATMENT MAY BE USED. - Â Â OESOPHAGEAL CANDIDIASIS AND VERY LOW CD4 COUNT
MAY BE PUT ON FLUCONAZOLE 100MG/DAY.
48
CRYPTOCOCCOSIS
- A LEADING CAUSE OF MORBIDITY
- MORTALITY.
- Â Â Â Â ORGANISM CRYPTOCOCCUS NEOFORMANS.
- CLINICAL MANIFESTATIONS
- Â Â Â Â Â MENINGITIS -MOST COOMON INITIAL
- MANIFESTATION.
- Â Â Â Â Â PULMONARY-FOCAL AND DIFFUSE,
- Â Â Â Â Â SKIN LESIONS,ENDOPHTHALMITIS,
- DISSEMINATION ARE OTHER MANIFESTATIONS.
49
DIAGNOSIS
- CT MRI OF BRAIN TO EXCLUDE SOL.
- Â CSF STUDY.ANTIGEN DETECTION, INDIA INK STAIN,
CULTURE. - Â CAN BE DETECTED FROM SERUM, URINE OR SPUTUM
ALSO.
50
TREATMENT
- DRUGS USED ARE AMPHOTERICIN-B, BOTH CONVENTIONAL
AND LIPOSOMAL - Â FLUCYTOSINE AND FLUCONAZOLE.
- Â MANY COMPARATIVE STUDIES DONE.
51
BEST RECOMMENDED REGIMEN.
- AMPHOTERICIN 0.7MG/KG/DAY FLUCYTOSINE
100MG/KG/DAY FOR AT LEAST 2 WEEKS. - Â IF THE PATIENT HAS IMPROVED FLUCONAZOLE 400
MG/DAY FOR FURTHER 8-10 WEEKS. - Â Â IN PATIENTS WHO ARE NOT RESPONDING DURING
INITIAL COURSE, AMPHOTERICIN CAN BE GIVEN FOR
UPTO 6 WEEKS. IF TOXICITY DEVELOPS ONE OF THE
LIPOSOMAL PREPARATION CAN BE USED IF AVAILABLE
AND AFFORDABLE.
52
OTHER REGIMENS
- FLUCONAZOLE 400MG/DAY OR
- Â Â Â ITRACONAZOLE 400MG/DAY.
- Â Â Â BUT RESPONSE RATE LOWER THAN THAT
- CONTAINING INITIAL AMPHOTERICIN.
- Â Â Â FLUCONAZOLE 400MG/DAY FLUCYTOSINE
- 150MG/KG/DAY-
- Â Â Â ENCOURAGING RESULT IN SMALL NUMBER OF
- PATIENTS.
- Â Â Â ALL TREATED PATIENTS SHOULD BE PUT ON
FLUCONAZOLE 200 MG/D TO PREVENT RELAPSE.
53
- MAINLY CAUSY TOXOPLASMA ENCEPHALITIS MANIFESTED
AS A FOCAL LESION. - Â Â INCIDENCE INCREASES AS CD4 CELL COUNT REACHES
AROUND100-200/CMM. - Â Â SEIZURE FOCAL NEUROLOGICAL SYPTOMS OCCUR.
- Â Â IT IS THE COMMONEST CAUSE OF A SPACE OCCUPYING
LESION IN A PATIENT WITH AIDS.
54
ADJUNCTIVE TREATMENT-
- INTRACRANIAL PRESSURE MAY INCREASE DUE DUE TO
REDUCED REABSORPTION OF CSF BY ARACHNOID VILLI
BLOCKED BY YEAST CELLS LEADS TO HYDROCEPHALUS.
- THIS CAN CAUSE BLINDNESS CAN BE PREVENTED TO
SOME EXTEND BY - Â Â Â Â Â Â Â Â Â Â Â Â Â FREQUENT LUMBAR PUNCTURE.
- Â Â Â Â Â Â Â Â Â Â Â Â Â ACETAZOLAMIDE 250MG QID.
- Â Â Â Â Â Â Â Â Â Â Â Â Â HIGH DOSE CORTICOSTEROIDS.
- Â Â Â Â Â Â Â Â Â Â Â Â Â VENTRICULAR SHUNTING.
55
TOXOPLASMOSIS
- TOXOPLASMOSIS REFERS TO THE CLINICAL AND/OR
PATHOLOGICAL EVIDENCE OF DISEASE CAUSED BY
TOXOPLASMA GONDII. - Â Â AN OBLIGATE INTRACELLULAR PATHOGEN.
- Â Â CAUSES ASYMPTOMATIC OR MILDLY SYMPTOMATIC
INFECTIONS IN NORMAL HOSTS. - Â Â CAUSES RAPIDLY PROGRESSIVE FATAL DISEASE IN
IMMUNOCOMPROMISED PATIENTS. - Â Â ZOONOTIC DISEASE.
- Â Â DEFINITIVE HOST CAT.
56
TRANSMISSION TO HUMANS
- ORAL ROUTE.
- Â Â BY EATINGPOORLY COOKED MEAT
- CONTAINING TISSUE CYSTS
- Â Â FOOD CONTAMINATED WITH SOIL CONTAINING
OOCYSTS EXCRETED BY CATS. - Â Â ACUTE ACQUIRED TOXOPLASMOSIS IS MOST
- COMMONLY ASYPTOMATIC.
- Â Â IN HIV-INFECTED PERSONS CAUSE A REACTIVATION
OF THE DISEASE WHEN IMMUNITY FADES.
57
- MAINLY CAUSY TOXOPLASMA ENCEPHALITIS MANIFESTED
AS A FOCAL LESION. - Â INCIDENCE INCREASES AS CD4 CELL COUNT REACHES
AROUND100-200/CMM. - Â SEIZURE FOCAL NEUROLOGICAL SYPTOMS OCCUR.
- Â IT IS THE COMMONEST CAUSE OF A SPACE OCCUPYING
LESION IN A PATIENT WITH AIDS.
58
D. DIAGNOSIS
- LYMPHOMA,TUBERCULOMA, PML, FUNGAL
- ABSCESS, CVA, HSV ENCEPHALITIS.
- DIAGNOSIS
- Â Â Â Â Â MRI AND CT SCAN WITH CONTRAST.
- Â Â Â Â Â DEMONSTRATION OF LATENT INFECTION BY
- RAISED SERUM IgG TITRES. BRAIN BIOPSY FOR
- HISTOLOGICAL CONFIRMATION
59
TREATMENT-
- THE GENERAL TREND IS TO RELY ON THERAPEUTIC TRIAL
FOR A DIAGNOSIS, RESERVING BRAIN BIOPSY FOR
TREATMENT FAILURES OR ATYPICAL PATIENTS WHO ARE
SERO NEGATIVE. - REGIMEN OF CHOICE-
- Â Â Â Â Â Â Â Â Â Â SULFADIAZINE AND PYREMETHAMINE.
- Â Â Â Â Â Â Â Â Â Â SULFADIAZINE- INITIAL DOSE IS1-1.5G
- ORALLY EVERY 6H.
- Â Â Â Â Â Â Â Â Â Â IN COMATOSE PATIENT S.D.CAN ALSO BE
- GIVEN 1G ( 75mg/Kg IN 4 DEVIDED
DOSES) IN - 500 ML SALINE EVERY 6HRS.
60
SIDE EFFECTS
- Â Â NAUSEA,VOMITING,DIARRHOEA,
- Â Â Â Â Â Â Â Â Â Â Â Â NEUTROPENIA,
- Â Â Â Â Â Â Â Â Â Â Â Â Â INTERSTITIAL NEPHRITIS,
- Â Â Â Â Â Â Â Â Â Â Â Â Â CRYSTALLURIA, AND
- NEPHROLITHIASIS,
- Â Â Â Â Â Â Â Â Â Â Â Â Â ACUTE RENAL FAILURE
- Â Â Â Â Â Â Â Â Â Â Â Â Â SKIN RASH.
61
PYREMETHAMINE
- INITIAL LOADING DOSE OF 200Mg FOLLOWED by 50-100
mg ORALLY/D. - Â Â TO REDUCE INCIDENCE OF PANCYTOPENIA, 10MG OF
FOLINIC ACID DAILY.
62
ALTERNATIVE THERAPIES-
- FANSIDAR (PYREMETHAMINE25MG SULFADOXINE500mg)
6-8 TABLETS DAILY IN DIVIDED DOSES FOR FIRST 2
DAYS FOLLOWED BY 2-3 TABLET DAILY. FOLINIC ACID
AS ABOVE. - Â Â DAPSONE100MG ORALLY,PYREMETHAMINE AND FOLINIC
ACID AS ABOVE. - Â Â TRETMENT IN THIS DOSE TO BE CONTINUED FOR 6
WEEKS. - Â Â PYREMETHAMINE 100-200MG PO LOAD THEN 50-75
MG/D ORAL OR IV CLINDAMYCIN 600MG QID
LEUCOVORIN 10MG OD.
63
- AZITHROMYCIN 1200-1500 MG QD PYREMETHAMINE
LEUCOVORIN. - Â Â CLARITHROMYCIN 1000MG PO BID PYREMETHAMINE
LEUCOVORINÂ Â Â Â Â Â Â Â Â Â Â Â Â - Â Â ATOVAQUONE 750MgPO TID PYREMETHAMINE
LEUCOVORIN. - Â Â MAINTENANCE TREATMENT
- Â FULL DOSE THERAPY TO BE GIVEN FOR 6-8
WEEKS,WEEKS,WITH FOLLOW UP IMAGING SHOWING
DECREASE IN SIZE OF LESION, THEN - CONTINUETHERAPY
- Â Â SD.2GM PMN 25-50 MG, OR
- Â Â FANSIDAR 1 OD, OR 2 THRICE WEEKLY,
- Â CO TRIMOXAZOLE DS 1OD,
64
CRYPTOSPORIDIASIS
- PREFERRED REGIMEN
- Â PARAMOMYCIN 500 MG PO TID OR 100MG PO BID WITH
FOOD X 14-28 DAYS.THEN 500MG PO BID. - Â Â PARAMOMYCIN 1GM BID/ AZITHROMYCIN600MG QD x 4
WEEKS, - Â Â THEN PMN ALONE x 8 WEEKS.
65
ALTERNATIVE REGIMENS
- NITAZOXANIDE 500Mg PO BID.
- Â Â Â Â OCTREOTIDE (SANDOSTATIN) 50-500 MicGm TID
- SC/ IV AT 1Mic Gm/HR.
- Â Â Â AZITHROMYCIN 1200MG X2 PO 1ST DAY,1200Mg/D X
27 D, - THEN 600 Mg/D
- Â Â Â ATOVAQUONE 750 Mg PO SUSPENSION WITH MEAL
BID. - Â Â Â OF THESE ONLY PMN AZN SHOWED GOOD RESPONSE
IN - TERMS OF CLINICAL SYMPTOMS AND OOCYST
- EXCRETION.
- Â Â Â HEART WITH IMMUNE RECONSTITUTION IS THE MOST
- EFFECTIVE TREATMENT.
66
CYTOMEGALOVIRUS RETINITIS
- SYMPTOMS VISUAL DISTURBANCE, FLOATERS, FLASHING
LIGHTS, FEVER. - Â Â Dx OPHTHALMOLOGIC EXAM WITH CHARACTERESTIC
LESIONS.,CD4 lt100. - Â Â Rx GANCYCLOVIR 5Mg/Kg IV Q 12 HRS INDUCTION
DOSE FOR 2 WEEKS FOLLOWED BY LIFE LONG
GANCYCLOVIR 5Mg/KG IV QD. - Â Â TOXICTYNEUTROPENIA 20-40,
- Â Â THROMBOCYTOPENIA- 5.
- Â Â GIT SYMPTOMS,RASHNEPHROTOXOCITY RARELY.
67
- ALTERNATIVE FOSCARNET 90Mg/Kg IV Q12Hrs
INDUCTION FOR 2 Wks THEN QD DOSING. - Â Â TOXICITY MOST COMMON-NEPHROTOXICITY,
RARE-HYPOCALCEMIA, HYPOKALEMIA, HYPOMAGNESEMIA,
NAUSEA, SEIZURE, ANAEMIA. - Â Â CIDOFOVIR 5MG/KG IV Q WEEK FOR 2 WEEKS THEN
EVERY 2 WEEKS THEREAFTER WITH PROBENECID 2GM PO 3
HR BEFORE AND 1GM PO 2 AND 8HRS AFTER INFUSION. - TOXICITY NEPHROTOXICITY.
- Â Â LIFELONG THERAPY WITH CONTINUED FOLLOWUP.
68
DISSEMINATED MAC
- Â Â Dx CD4 lt100,BLOOD CULTURE, OR BM BIOPSY VE.
- Â Â Rx CLARITHROMYCIN 500 MGPO BID OR
AZITHROMYCIN 500MG PO QD PLUS ETHAMBUTOL 15-25
MG/KG/D PLUS RIFABUTIN 300 MG PO QD. - SIGNS AND SYMPTOMS FEVER, WT LOSS NIGHT SWEATS.
69
        ALTERNATIVES TO ADD IF NO RESPONSE OR
SIDE EFFECTS TO ABOVE
- CIPROFLOXACIN 750MG PO BID, OFLOXACIN 400MG PO
BID, AMIKACIN 7.5-15MG/KG IV QD FOR 1-2 MKONTHS. - Â Â DURATION OF THERAPY IS LIFELONG.
70
PRIMARY PROPHYLAXIS OF OPPORTUNISTIC INFECTIONS
IN ADULTS ADOLESCENTS WITH HIV.
- PNEUMOCYSTIS CARINII
- INDICATION
- Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â CD4 COUNT lt200/MicL OR
- Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â OESOPHAGEAL CANDIASIS.
- Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â FIRST CHOICETMP-SMZ,1DS
ORALLY OD. - Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â Â ALTERNATIVE DAPSONE 50Mg BD
OR 100Mg OD, DAPSONE 50 Mg OD PYREMETHAMINE50
Mg/WEEK LEUCOVORIN25Mg /WEEK. - Â
- Â AEROSOLIZED PENTAMIDINE,300MG EVERY MONTH VIA
RESPIGARD 11 NEBULIZER. - Â ATOVAQUONE. 1500MG MG ORALLY OD.
- Â TMP-SMZ,1DS ORALLY 3 TIMES/WEEK.
71
TOXOPLASMA GONDII
- IgG Ab TO TOXOPLASMA CD4 COUNTlt100/MicL.
- Â Â CO-TRIMOXAZOLE DS TABLET I DAILY.
72
MYCOBACTERIUM AVIUM COMPLEX
- CD4 COUNT lt50 /MicL.
- Â Â Â Â AZITHROMYCIN 1200M ORALLY / WEEK.
- Â Â Â Â OR CLARITHROMYCIN 500MG BID OD.
73
CRYPTOCOCCUS NEOFORMANS
- CD4 COUNT lt50/Cumm.
- Â Â Â Â Â Â FLUCONAZOLE 100-200MG OD.
- Â Â Â Â Â Â A.RITRACONAZOLE 200MG OD
74
CYTO MEGALO VIRUS
- CD4 lt50/Cumm CMV Ab ve.
- Â Â ORAL GANCYCLOVIR 1GM TID.
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