Dihydropteroate synthase gene mutations in Pneumocystis and sulfa resistance.Pneumocystis pneumonia Pneumocystis Pneumonia Definition Pneumocystis pneumonia is a lung infection that occurs primarily in people with weakened immune systems-especially people who are HIV-positive. (PCP PCP abbr. 1. phencyclidine 2. primary care physician Pneumocystis carinii pneumonia (PCP) ) remains a major cause of illness and death in HIV-infected persons. Sulfa drugs sulfa drugs a group of chemical compounds used as antibacterial agents; called also sulfonamides. , trimethoprim-sulfamethoxazole (TMP-SMX Trimethoprim-sulfamethoxazole (TMP-SMX) An antibiotic used to treat and prevent PCP. Mentioned in: Pneumocystis Pneumonia TMP-SMX, n acronym for trimethoprim-sulfamethoxazole. ), and dapsone dapsone /dap·sone/ (dap´son) an antibacterial bacteriostatic for a broad spectrum of gram-positive and gram-negative organisms; used as a leprostatic, as a dermatitis herpetiformis suppressant, and in the prophylaxis of falciparum are mainstays of PCP treatment and prophylaxis prophylaxis (prō'fĭlăk`sĭs), measures designed to prevent the occurrence of disease or its dissemination. Some examples of prophylaxis are immunization against serious diseases such as smallpox or diphtheria; quarantine to confine . While prophylaxis has reduced the incidence of PCP, its use has raised concerns about development of resistant organisms. The inability to culture human Pneumocystis Pneumocystis /Pneu·mo·cys·tis/ (-sis´tis) a genus of yeastlike fungi. P. cari´nii is the causative agent of interstitial plasma cell pneumonia. pneu·mo·cys·tis n. , Pneumocystis jirovecii, in a standardized culture system prevents routine susceptibility testing and detection of drug resistance. In other microorganisms, sulfa drug sulfa drug, any of a class of synthetic chemical substances derived from sulfanilamide, or para-aminobenzenesulfonamide. Sulfa drugs are used to treat bacterial infections, although they have largely been replaced for this purpose by antibiotics; some are also used resistance has resulted from specific point mutations in the dihydropteroate synthase synthase /syn·thase/ (-thas) a term used in the names of some enzymes, particularly lyases, when the synthetic aspect of the reaction is dominant or emphasized. syn·thase n. (DHPS) gene. Similar mutations have been observed in P. jirovecii. Studies have consistently demonstrated a significant association between the use of sulfa drugs for PCP prophylaxis and DHPS gene mutations. Whether these mutations confer resistance to TMPSMX or dapsone plus trimethoprim trimethoprim /tri·meth·o·prim/ (-meth´o-prim) an antibacterial closely related to pyrimethamine; almost always used in combination with a sulfonamide, primarily for the treatment of urinary tract infections. for PCP treatment remains unclear. We review studies of DHPS mutations in P. jirovecii and summarize the evidence for resistance to sulfamethoxazole sulfamethoxazole /sul·fa·meth·ox·a·zole/ (-meth-ok´sah-zol) a sulfonamideantibacterial and antiprotozoal, particularly used in acute urinary tract infections. sul·fa·me·thox·a·zole n. and dapsone. ********* Although decreasing in incidence as a result of combination antiretroviral therapy and effective prophylaxis, Pneumocystis pneumonia (PCP), caused by Pneumocystis jirovecii (formerly P. carinii f. sp. hominis), remains the most common AIDS-defining opportunistic infection opportunistic infection n. An infection by a microorganism that normally does not cause disease but becomes pathogenic when the body's immune system is impaired and unable to fight off infection, as in AIDS and certain other diseases. , as well as the most frequent serious opportunistic infection in HIV-infected persons, in the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. and Europe. Despite the fact that this infection can be prevented, certain patients continue to be at increased risk for PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) Specifically, PCP frequently signals H1V infection in patients not previously known to be HIV-infected (1). Patients who are not receiving regular medical care, as well as those who are not receiving or responding to antiretroviral therapy or prophylaxis, are also at increased risk for PCP (2). PCP may also develop in other immunosuppressed Immunosuppressed A state in which the immune system is suppressed by medications during the treatment of other disorders, like cancer, or following an organ transplantation. Mentioned in: Fifth Disease populations, such as cancer patients and transplant recipients. Furthermore, PCP remains a leading cause of death among critically ill patients, despite advances in treatment and management (3). The first-line treatment A first-line treatment or first-line therapy is a medical therapy recommended for the initial treatment of a disease, sign or symptom, usually on the basis of empirical evidence for its efficacy. and prophylaxis regimen for PCP is trimethoprim-sulfamethoxazole (TMP-SMX) (4). While prophylaxis has been shown to reduce the incidence of PCP, the widespread and long-term use of TMP-SMX in HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. patients has raised concerns regarding the development of resistant organisms. Even short-term exposure to TMP-SMX can be associated with the emergence of TMPSMX resistance, as has been demonstrated in patients with acute cystitis cystitis (sĭstī`tĭs), common acute or chronic inflammation of the urinary bladder. The disease occurs primarily in young women and frequently results from bacterial invasion of the urethra from the adjacent rectum, most commonly with caused by Escherichia coli Escherichia coli (ĕsh'ərĭk`ēə kō`lī), common bacterium that normally inhabits the intestinal tracts of humans and animals, but can cause infection in other parts of the body, especially the urinary tract. (5). Indeed, an increased number of sulfa-resistant bacteria have been isolated in HIV patients, which coincides with the rise in TMP-SMX prophylaxis for PCP (6,7). In one study, the prevalence of TMP-SMX-resistant Staphylococcus aureus Staphylococcus au·re·us n. A bacterium that causes furunculosis, pyemia, osteomyelitis, suppuration of wounds, and food poisoning. Staphylococcus aureus Staphylococcus pyogenes and Enterobacteriaceae species isolated in all hospitalized patients increased significantly from <5.5% of isolates before 1986 to 20% in 1995, during which time TMPSMX prophylaxis was increasing in HIV-infected patients (6). In addition, the rise in resistant organisms was significantly more prominent in samples obtained from HIV-infected patients, in whom resistant isolates increased from 6.3% in 1988 to 53% in 1995. Another study found that significantly more TMP-SMX-resistant organisms were isolated from HIV-infected patients who had received TMP-SMX than from patients who had not received TMPSMX (7). Given the emergence of resistance to TMP-SMX among many bacteria (8), concern has focused on the potential development of resistant Pneumocystis. Based on animal studies, nearly all of the anti-Pneumocystis activity of TMP-SMX is due to sulfamethoxazole (9). The development of sulfonamide sulfonamide /sul·fon·amide/ (sul-fon´ah-mid) a compound containing the sbondSO2NH2 group. The sulfonamides, or sulfa drugs, are derivatives of sulfanilamide, competitively inhibit folic acid synthesis in microorganisms, and formerly were resistance could result in the failure of sulfamethoxazole as well as dapsone, a sulfone sulfone /sul·fone/ (sul´fon) 1. the radical SO2. 2. a compound containing two hydrocarbon radicals attached to the —SO2— group, especially dapsone and its derivatives, which are potent antibacterials effective antimicrobial antimicrobial /an·ti·mi·cro·bi·al/ (-mi-kro´be-al) 1. killing microorganisms or suppressing their multiplication or growth. 2. an agent with such effects. agent also used in the treatment and prophylaxis of PCP. While separate lines of investigation also suggest that Pneumocystis may be developing resistance to atovaquone, a second-line PCP treatment and prophylaxis regimen (10), we concentrate our review on the evidence for the development of sulfonamide-resistant Pneumocystis. Mechanisms of Sulfonamide Resistance Sulfonamides Sulfonamides Definition Sulfonamides are medicines that prevent the growth of bacteria in the body. Purpose Sulfonamides are used to treat many kinds of infections caused by bacteria and certain other microorganisms. act by interfering with folate folate /fo·late/ (fo´lat) 1. the anionic form of folic acid. 2. more generally, any of a group of substances containing a form of pteroic acid conjugated with l-glutamic acid and having a variety of substitutions. synthesis. Since many microorganisms cannot transport folate into cells as mammalian cells can, most prokaryotes and lower eukaryotes must synthesize To create a whole or complete unit from parts or components. See synthesis. folates de novo [Latin, Anew.] A second time; afresh. A trial or a hearing that is ordered by an appellate court that has reviewed the record of a hearing in a lower court and sent the matter back to the original court for a new trial, as if it had not been previously heard nor decided. (11). Sulfonamides inhibit one of the integral enzymes in folate synthesis, dihydropteroate synthase (DHPS), which catalyzes the condensation of para-aminobenzoic acid para-aminobenzoic acid (pâr`ə-əmē`nōbĕnzōĭk): see vitamin. and pteridine to form dihydropteroic acid di·hy·dro·pte·ro·ic acid n. An intermediate formed during the biosynthesis of folic acid; its formation is inhibited by sulfonamides. (Figure). Since mammalian cells lack DHPS, sulfonamides can selectively inhibit the growth of various microorganisms. Trimethoprim, part of the fixed combination TMP-SMX, inhibits another of the integral enzymes, the dihydrofolate reductase dihydrofolate reductase enzyme catalyzing the conversion of folate to 5,6,7,8-tetrahydrofolate, which is the key carrier of one-carbon units in purine and pyridime synthesis, the pathway for the breakdown of histidine and the synthesis of S-adenosylmethionine from S (DHFR DHFR Dihydrofolate reductase, see there ). Resistance to sulfonamides can emerge by means of a number of mechanisms (12). In most gram-negative enteric bacteria Noun 1. enteric bacteria - rod-shaped Gram-negative bacteria; most occur normally or pathogenically in intestines of humans and other animals enterics, enterobacteria, entric , sulfonamide resistance is largely plasmidborne and related to drug-resistant DHPS variants with substantial sequence divergence (12). Chromosomal mutations in the DHPS locus--such as point mutations, insertions of duplicate amino acids, or larger sequence alterations as a result of recombination--can also lead to resistance (8). In some organisms, several different mechanisms of resistance have been identified in different strains. For example, some strains of Neisseria meningitidis Neisseria men·in·git·i·dis n. The bacteria that is the causative agent of cerebrospinal meningitis; meningococcus. Neisseria meningitidis have acquired a DHPS gene with 10% sequence divergence, postulated pos·tu·late tr.v. pos·tu·lat·ed, pos·tu·lat·ing, pos·tu·lates 1. To make claim for; demand. 2. To assume or assert the truth, reality, or necessity of, especially as a basis of an argument. 3. by others to be due to recombination recombination, process of "shuffling" of genes by which new combinations can be generated. In recombination through sexual reproduction, the offspring's complete set of genes differs from that of either parent, being rather a combination of genes from both parents. (12), whereas other Neisseria strains have acquired a chromosomal insertion, resulting in the addition of two amino acids to DHPS (13). In other organisms, such as E. coil and Plasmodiumfalciparum, nonsynonymous point mutations resulting in amino acid substitutions in DHPS can confer sulfa sul·fa adj. Of, relating to, or containing sulfanilamide or any sulfa drug. sulfa (sul´f resistance (14,15). Furthermore, the accumulation of additional mutations over time can confer increasing levels of sulfa resistance, as has occurred in P. falciparum (16). Dihydropteroate Synthase Mutations in Pneumocystis Similar to other microorganisms, mutations have been identified in the DHPS gene of Pneumocystis jirovecii, which has raised the question of whether P. jirovecii is developing resistance to sulfonamides. The DHPS gene of P.jirovecii has been sequenced and is part of the folic acid folic acid: see coenzyme; vitamin. folic acid or folate Organic compound essential to animal growth and health and needed by bacteria as a growth factor. synthesis gene or fas gene; it encodes a trifunctional protein along with dihydroneopterin aldolase aldolase /al·do·lase/ (al´do-las) 1. aldehyde-lyase. 2. an enzyme that acts as a catalyst in the production of dihydroxyacetone phosphate and glyceraldehyde phosphate from fructose 1,6-bisphosphate. and hydroxymethyldihydropterin pyrophosphokinase (17). Sulfa medications appear to exert selective pressure on Pneumocystis (18), as the DHPS gene is more likely to display mutations in highly conserved regions in patients with PCP who have previously been exposed to sulfa medications (19-25). These DHPS gene mutations were rarely found in clinical isolates before the early 1990s (19,20,22). Genetic analysis suggests that the mutations arose independently in multiple strains of Pneumocystis, which supports the theory that exposure to sulfa medications selects for DHPS gene mutations (26). Furthermore, DHPS gene mutations have not been found in other mammalian Pneumocystis species that have not been exposed to sulfa medications (18,27). Several factors suggest that the mutations observed in P. jirovecii may confer resistance to sulfa medications. The region of the DHPS gene in which mutations have been identified is one that is highly conserved among other organisms, including Plasmodium falciparum Plasmodium fal·cip·a·rum n. A protozoan that causes falciparum malaria. , Streptococcus pneumoniae Streptococcus pneu·mo·ni·ae n. Pneumococcus. Streptococcus pneumoniae Microbiology A pathogenic streptococcus with 90 serotypes associated with pneumonia, bacteremia, meningitis Transmission Person to person Incidence , E. coli E. coli: see Escherichia coli. E. coli in full Escherichia coli Species of bacterium that inhabits the stomach and intestines. E. coli can be transmitted by water, milk, food, or flies and other insects. , and Bacillus subtilis Noun 1. Bacillus subtilis - a species of bacillus found in soil and decomposing organic matter; some strains produce antibiotics Bacillus globigii, grass bacillus, hay bacillus (18). The most common mutations identified in the Pneumocystis jirovecii DHPS are nonsynonymous point mutations, which result in amino acid substitutions at positions 55, 57, or both. Different strains with single or double amino acid substitutions at these positions have been identified (Table 1). Based on homology homology (hōmŏl`əjē), in biology, the correspondence between structures of different species that is attributable to their evolutionary descent from a common ancestor. to the E. coli DHPS, these point mutations appear to be in an active site of the enzyme involved in substrate binding; thus, amino acid substitutions in these regions could result in structural changes that could interfere with substrate binding and enzyme activity Enzyme activity A measure of the ability of an enzyme to catalyze a specific reaction. Mentioned in: Glucose-6-Phosphate Dehydrogenase Deficiency (21). Likewise, similar point mutations in positions equivalent to this site in Plasmodium falciparum (15) and Mycobacterium leprae Mycobacterium lep·rae n. Hansen's bacillus. Mycobacterium leprae Infectious disease The mycobacterium that causes leprosy. See Leprosy. (28) confer sulfa resistance. Other mutations near this site also cause sulfa resistance in S. pneumoniae and R falciparum (18). However, the inability to reliably culture Pneumocystis jirovecii in a standardized in vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. culture system prevents the routine susceptibility testing of Pneumocystis. The lack of a standardized culture system also hampers research into the development and testing of new antimicrobial agents Antimicrobial agents Chemical compounds biosynthetically or synthetically produced which either destroy or usefully suppress the growth or metabolism of a variety of microscopic or submicroscopic forms of life. with anti-Pneumocystis activity, which highlights our reliance on TMP-SMX as the current mainstay of therapy. Thus, the clinical significance of these DHPS gene mutations must be inferred from correlating the clinical outcome with the presence of DHPS gene mutations in patients with PCP. Association of Sulfamethoxazole and Dapsone with DHPS Gene Mutations Several studies have consistently demonstrated a significant association between the use of TMP-SMX or dapsone for PCP prophylaxis in HIV-infected persons and the presence of DHPS gene mutations (Table 2) (19-25,29). One study extended these findings to the use of pyrimethamine pyrimethamine /pyr·i·meth·amine/ (pir?i-meth´ah-men) a folic acid antagonist, used in the treatment of malaria and of toxoplasmosis. py·ri·meth·a·mine n. plus sulfadoxine for PCP prophylaxis (30). Another study demonstrated an apparent reversal of the DHPS mutant-to-wild-type ratios after the use of TMPSMX was restricted (31). In total, studies report >700 episodes of PCP, span a period from 1976 to 2001, and include patient data and clinical specimens from multiple cities in several different countries. Unfortunately, these studies used different criteria to define PCP prophylaxis with TMP-SMX or dapsone, which effectively limits attempts at data pooling for more direct and detailed analyses. In addition, most of the studies collected data by abstracting information from patient charts. Thus, these studies were unable to assess whether patients adhered to the prescribed prophylaxis. Nevertheless, seven of the nine studies found that most HIV-infected patients with a diagnosis of PCP who had been prescribed TMP-SMX or dapsone for PCP prophylaxis had Pneumocystis that contained DHPS mutations (range 19%-80%, Table 2) (19-24,30). Furthermore, eight of the nine studies reported that PCP patients for whom TMP-SMX or dapsone was prescribed were more likely to have Pneumocystis that contained DHPS mutations than were patients for whom these medications were not prescribed (19 25,30). Of note, in all nine studies, DHPS mutations were observed in PCP patients who were not currently receiving TMP-SMX or dapsone. Whether these patients who failed to meet the defined criteria for TMP-SMX or dapsone prophylaxis had ever received one of these medications for prophylaxis or had received TMP-SMX for a reason other than PCP prophylaxis at some point during their lives was difficult to assess with any degree of confidence. Nevertheless, most of the studies found that only a minority of PCP patients who had not been prescribed TMPSMX or dapsone for PCP prophylaxis had Pneumocystis that contained DHPS mutations. The study that reported the highest proportion (48%) used both chart abstraction and patient interview as sources of clinical information regarding PCP prophylaxis (23). This study also used a broad definition of PCP prophylaxis, including patient report of TMP-SMX use for prophylaxis at any time in life. Thus, despite rigorous attempts to document TMP-SMX or dapsone use for PCP prophylaxis and with the broadest definition of prophylaxis applied, nearly half of the patients without TMP-SMX or dapsone use had evidence of DHPS mutations on their clinical PCP specimen. Among the 26 patients with a new diagnosis of HIV infection at the time PCP was diagnosed and who thus had never received PCP prophylaxis, 14 (54%) had Pneumocystis that contained DHPS gene mutations. The specific city of residence was also an independent predictor associated with the risk for Pneumocystis that contained DHPS gene mutations. Patients who lived in San Francisco San Francisco (săn frănsĭs`kō), city (1990 pop. 723,959), coextensive with San Francisco co., W Calif., on the tip of a peninsula between the Pacific Ocean and San Francisco Bay, which are connected by the strait known as the Golden were five times more likely, and patients who lived in Seattle were more than three times as likely to have mutant DHPS than patients who resided in Atlanta, even when factors including sulfonamide or dapsone PCP prophylaxis and prior PCP were controlled for. The presence of DHPS mutations in patients without prior TMPSMX or dapsone use for PCP prophylaxis, the absence of similar mutations in Pneumocystis isolated from other mammalian species, and the impact of geography on DHPS genotype genotype (jēn`ətīp'): see genetics. genotype Genetic makeup of an organism. The genotype determines the hereditary potentials and limitations of an individual. have substantial implications for disease transmission (i.e., person-to-person transmission) that are beyond the scope of this review (32 35). Lack of Association of Trimethoprim with DHFR Gene dhfr gene see dhfrgene. Mutations Trimethoprim inhibits another of the integral enzymes in folate synthesis, DHFR (Figure). In other microorganisms, point mutations in the DHFR gene are an important mechanism of drug resistance. This finding has led researchers to examine the DHFR gene of P. jirovecii to evaluate whether DHFR mutations contribute to TMP-SMX resistance. To date, two studies have failed to demonstrate an association between the use of TMP-SMX for PCP prophylaxis in HIV-infected persons and the presence of DHFR gene mutations (21,36). In one study, 36 of 37 specimens (from 35 patients, 26 of whom were HIV-infected) demonstrated identical DHFR sequences, with a single specimen showing one synonymous nucleotide change (21). In the second study, 16 (59%) of 27 specimens (from 27 patients, 19 of whom were HIV-infected) had DHFR gene mutations, 14 had synonymous changes, and 2 had nonsynonymous changes (36). Neither of the two patients whose PCP specimen had nonsynonymous DHFR changes had prior exposure to DHFR inhibitors, yet both patients were treated successfully for PCP with TMP-SMX. In addition, this study aligned the Pneumocystis DHFR sequences with those of E. coli, Staphylococcus aureus, Streptococcus pneumoniae, and Plasmodium falciparum and reported that the observed nonsynonymous changes in Pneumocystis DHFR were not in the highly conserved regions of the enzyme as are the amino acid substitutions that confer resistance to TMP TMP (thymidine monophosphate): see thymine. (or pyrimethamine) in these other organisms. Thus, the presence and association of DHPS, but not DHFR, gene mutations with the use of specific PCP prophylaxis regimens argue strongly both for the importance of SMX SMX Search Marketing Expo SMX Sulfamethoxazole SMX Server Macro Expansion SMX Santa Maria, CA, USA - Santa Maria Public Airport (Airport Code) SMX SonicsMX SMX Smithway Motor Xpress, Inc. and dapsone against Pneumocystis and the central role of DHPS mutations in the potential development of TMP-SMX or dapsone resistance. Clinical Importance of DHPS Gene Mutations in Pneumocystis jirovecii A number of studies have examined the effect of DHPS gene mutations on clinical outcomes such as death, death specifically attributable to PCP, and PCP treatment failure with TMP-SMX or dapsone plus trimethoprim (Table 3) (19-22,24,25,37-39). Whether the presence of DHPS gene mutations confers clinical resistance to TMP-SMX or dapsone plus trimethoprim for PCP treatment remains unclear and requires further study. In a multivariate analysis multivariate analysis, n a statistical approach used to evaluate multiple variables. multivariate analysis, n a set of techniques used when variation in several variables has to be studied simultaneously. , Helweg-Larsen and colleagues found that DHPS mutations were an independent predictor associated with increased death rates (20). In this study, DHPS mutation was the strongest predictor of death, and patients who had Pneumocystis that contained DHPS mutations had a greater than threefold increased risk for death within 3 months compared to patients with the wild-type DHPS, after important mortality cofactors such as age, CD[4.sup.+]/cell count, and arterial oxygen partial pressure (Pa[O.sub.2]) were controlled for. Whether this increased death rate was due to failure of TMP-SMX for PCP treatment is unclear. In fact, 12 (63%) of 19 PCP patients with Pneumocystis that contained DHPS gene mutations responded to PCP treatment with TMP-SMX. Kazanjian and co-workers found that the presence of DHPS mutations was associated with an increased risk for PCP treatment failure with TMP-SMX or dapsone plus trimethoprim (22). In univariate analysis, PCP patients who had Pneumocystis that contained DHPS gene mutations had a greater than twofold increased risk for treatment failure with one of these regimens, compared to patients with the wild-type DHPS. In this study, treatment failure was defined as worsening of clinical features after 7 days of therapy, failure to improve after 10 days of therapy, or a change in therapy because the treating physician perceives failure. Patients who responded clinically to therapy but who switched therapies because of adverse effects were considered to have been treated successfully. Similar to the findings of Helweg-Larsen, most patients with Pneumocystis that contained DHPS gene mutations responded to PCP treatment with TMP-SMX or dapsone plus trimethoprim. Overall, 15 (71%) of 21 PCP patients with Pneumocystis that contained DHPS gene mutations responded to PCP treatment with one of these two regimens. In addition, this study found no association between the presence of DHPS mutations and death at 4 weeks. In contrast to these prior two studies, Navin and colleagues found no association between the presence of DHPS mutations and overall number of deaths at 6 weeks, death attributable specifically to PCP, or PCP treatment failure (39). Overall, 16 (17%) of 94 PCP patients with DHPS mutations died compared to 9 (25%) of 36 PCP patients with wild-type DHPS (p = 0.30). Similarly, seven patients (7%) with PCP with DHPS mutations died as a result of PCP compared to four patients (11%) with wild-type DHPS. Among the 66 patients with PCP with DHPS mutations who were treated with TMP-SMX, 56 (85%) responded to this treatment. In this study, patients were classified as having been successfully treated if they completed a full course of therapy and responded or if they responded sufficiently to be switched from intravenous to oral therapy and be discharged. Similar to the Kazanjian study, patients who responded clinically to therapy but who switched therapies because of adverse effects were considered to have been treated successfully. This noted TMP-SMX response rate was significantly better than the rate for patients with DHPS mutation who were treated with intravenous pentamidine pentamidine /pen·tam·i·dine/ (pen-tam´i-den) an antiinfective used as the isethionate salt in the treatment of pneumonia, leishmaniasis, and early African trypanosomiasis. or clindamycin plus primaquine primaquine /prim·a·quine/ (prim´ah-kwen) an 8-aminoquinoline compound used as an antimalarial in the form of the phosphate salt. (14 [50%] of 28) and for patients with the wild-type DHPS who were treated with TMP-SMX (23 [64%] of 36). These results were similar when the analysis was restricted to patients who had been treated for at least 7 days with their initial therapy. Although these three patient groups did not differ in terms of age, CD4-cell count, serum albumin serum albumin n. See seralbumin. , serum lactate dehydrogenase lactate dehydrogenase n. Abbr. LDH Any of a class of enzymes found in the liver, kidneys, striated muscle, and heart muscle that catalyze the reversible conversion of pyruvate and lactate. (LDH LDH -lactate dehydrogenase. LDH abbr. lactate dehydrogenase LDH lactic acid dehydrogenase; see lactate dehydrogenase. ), or proportion who required corticosteroids Corticosteroids Definition Corticosteroids are group of natural and synthetic analogues of the hormones secreted by the hypothalamic-anterior pituitary-adrenocortical (HPA) axis, more commonly referred to as the pituitary gland. , no multivariate analysis was performed to determine independent predictors associated with death (or PCP treatment failure). Instead, a series of stratified stratified /strat·i·fied/ (strat´i-fid) formed or arranged in layers. strat·i·fied adj. Arranged in the form of layers or strata. analyses were performed and failed to detect any subsets of PCP patients in whom DHPS mutations were associated with a worse outcome. Summary and Future Directions Whether Pneumocystis DHPS gene mutations confer clinical resistance to TMP-SMX or dapsone plus trimethoprim for PCP treatment remains unclear. Published studies offer conflicting results. Each study used different definitions for PCP prophylaxis and PCP treatment success or failure, and each examined patient deaths at different time-points, with different methods of statistical analysis. These methodologic differences limit attempts at data pooling for more direct and detailed analyses. The outcome of HIV-infected patients with PCP is a complex issue, with multiple factors affecting death, including those related to the patient (e.g., age), the patient's overall health status (e.g., serum albumin), the underlying HIV/AIDS HIV/AIDS Human Immunodeficiency Virus/Acquired Immune Deficiency Syndrome (e.g., coexisting opportunistic infections Opportunistic infections Infections that cause a disease only when the host's immune system is impaired. The classic opportunistic infection never leads to disease in the normal host. or conditions), and, of course, those specific factors related to PCP (e.g., disease severity, presence of respiratory failure Respiratory Failure Definition Respiratory failure is nearly any condition that affects breathing function or the lungs themselves and can result in failure of the lungs to function properly. , need for mechanical ventilation mechanical ventilation n. A mode of assisted or controlled ventilation using mechanical devices that cycle automatically to generate airway pressure. , and development of serious complications such as pneumothorax pneumothorax (n  mōthôr`ăks), collapse of a lung with escape of air into the pleural cavity between the lung and the chest wall. The cause may be traumatic (e.g. ). In each individual report, the
overall number of patients studied and the subset of patients who had
Pneumocystis that contained DHPS mutations and were treated with TMP-SMX
or dapsone plus trimethoprim were too small to account for these factors
and to detect small differences in outcome that may be related to drug
resistance. Furthermore, these and future observational studies observational studies,n.pl an investigational method involving description of the associations be-tween interventions and outcomes. Outcomes research and practice audits are examples of this investigational method. that examine DHPS genotype and PCP treatment outcome are complicated by the absence of validated PCP clinical treatment guidelines, practice standards, and definitions of treatment success or failure. While the declining incidence of PCP in the United States and Europe, as a result of combinations of antiretroviral therapy and PCP prophylaxis, might lessen the enthusiasm for continued study of this issue, brief consideration of a number of factors that warn of a future "perfect storm" suggests that continued study is important. First, most HIV-infected persons worldwide reside in sub-Saharan Africa, Southeast Asia Southeast Asia, region of Asia (1990 est. pop. 442,500,000), c.1,740,000 sq mi (4,506,600 sq km), bounded roughly by the Indian subcontinent on the west, China on the north, and the Pacific Ocean on the east. , and Latin America Latin America, the Spanish-speaking, Portuguese-speaking, and French-speaking countries (except Canada) of North America, South America, Central America, and the West Indies. , places where access to antiretroviral therapy and PCP prophylaxis are limited. Second, PCP is increasingly being recognized as an important cause of illness in these regions. In many of these regions, programs to use TMP-SMX as multiopportunistic infection prophylaxis are being implemented, and Pneumocystis that contains DHPS mutations can be expected. Next, the treatment options for PCP in these regions are often limited to TMP-SMX, since regimens such as pentamidine, clindamycin plus primaquine, trimetrexate, and atovaquone are unavailable. The existence of TMP-SMX-resistant Pneumocystis in these regions, combined with the general absence of invasive diagnostic procedures (e.g., bronchoscopy Bronchoscopy Definition Bronchoscopy is a procedure in which a cylindrical fiberoptic scope is inserted into the airways. This scope contains a viewing device that allows the visual examination of the lower airways. that might establish an earlier diagnosis of PCP when the outcome is better) and intensive care facilities (e.g., mechanical ventilation that might support patients until PCP treatment can be effective), stresses the importance of further study (40).
Table 1. Amino acid substitutions observed in Pneumocystis
jirovecii (a)
Amino acid Amino acid
DHPS genotype position 55 position 57
Wild-type
1 Threonine Proline
Mutant
2 Alanine Proline
3 Threonine Serine
4 (double mutant) Alanine Serine
Mixed
5 Threonine Proline/serine
6 Threonine/alanine Proline/serine
7 Threonine/alanine Proline
8 Alanine Proline/serine
(a) DHPS, dihydropteroate synthase.
Table 2. Association between sulfonamide or sulfone for PCP
prophylaxis and DHPS gene mutations (a)
Prophylaxis (b)
Location definition
Author PCP (time period), (source of
(y) (ref) cases, no. country information)
Kazanjian 27 (20 Ann Arbor, MI
(1998) (19) HIV-infected) (1991-1997), USA
Indianapolis, IN At least 1 out
(1976-1997), USA of 4 months
preceding PCP
(chart)
Helweg-Larsen 152 Copenhagen Exposure (e)
(1999) (20) (1989-1999), (chart)
Denmark
Prophylaxis (f)
(chart)
Ma 37 (26 Bethesda, MD Any (chart)
(1999) (21) HIV-infected) (1985-1998), USA
Kazanjian 97 Denver, CO, At least 1 out
(2000) (22) Indianapolis, IN, of 4 months
Boston, MA, preceding PCP
Detroit, MI (chart)
(1991-1997), USA
Huang 111 Atlanta, GA, Ever (interview),
(2000) (23) Seattle, WA, Any in the 3
San Francisco, months preceding
CA (1996-1999), PCP (chart and
USA interview)
Visconti 20 Rome (Chart)
(2001) (24) (1992-1997),
Italy
Ma 107 Milan Any in the
(2002) (25) (1994-2001), 6 months
Italy preceding PCP
(chart)
Costa 89 (83 Lisbon Prophylaxis (h)
(2003) (29) HIV-infected) (1994-2001), Exposure (i)
Portugal
Nahimana 158 (120 Lyon (1993-1996), Prophylaxis (j)
(2003) (30) HIV-infected) France
DHPS mutations DHPS mutations
among persons among persons not
Author using prophylaxis using prophylaxis
(y) (ref) N (%) N (%) p value
Kazanjian 5/7 (71) (c) 2/20 (10) (c) 0.0032
(1998) (19)
5/7 (71) (d) 2/13 (15) (d) 0.022
Helweg-Larsen 18/29 (62) 13/123 (11) <0.0001
(1999) (20)
5/7 (71) (g) 15/125 (12) 0.01
Ma 11/14 (79) 2/18 (11) <0.001
(1999) (21)
Kazanjian 28/37 (76) 14/60 (23) <0.001
(2000) (22)
Huang 57/71 (80) 19/40 (48) <0.001
(2000) (23)
Visconti 4/5(80) 4/15 (27) 0.031
(2001) (24)
Ma 6/31 (19) 3/76 (4) 0.017
(2002) (25)
Costa 6/17 (35) 18/72 (25) 0.39
(2003) (29)
Nahimana 16/20 (80) 41/138 (30) <0.001
(2003) (30)
(a) PCP, Pneumocystis pneumonia; dihydropteroate synthase (DPHS);
TMP-SMX, trimethoprim-sulfamethoxazole.
(b) Prophylaxis refers to persons using TMP-SMX or dapsone who
met the specific criteria described.
(c) The seven specimens with DHPS gene mutations were from
1995 to 1997.
(d) Analysis restricted to 20 HIV-infected persons.
(e) Exposure, continuous use for at least 1 week at any time
after the diagnosis of HIV infection.
(f) Prophylaxis at least 8 weeks preceding PCP.
(g) Analysis restricted to patients receiving TMP-SMX or dapsone
prophylaxis versus no prophylaxis.
(h) Prophylaxis, adherence to the same regimen for a minimum
of 2 months preceding PCP.
(i) Exposure, use for at least 1 week in the 6 months preceding PCP.
(j) Prophylaxis 3 months preceding PCP. Includes patients who
received pyrimethamine/sulfadoxine for PCP prophylaxis.
Table 3 Association between DHPS gene mutations and important
clinical outcomes (a)
PCP DHPS Increased PCP
cases, mutations, Increased treatment
Author (y) (ref) no. no. death rate? failure?
Kazanjian (1998) 27 7 NA NA
(19)
Mei (1998) (37) 2 2 NA NA
Helweg-Larsen 144 29 Yes (b) NA
(1999) (20) 3 months
Ma (1999) (21) 37 13 No NA
Kazanjian (2000) 97 42 No (c) Yes (d)
(22) 4 weeks
Takahashi (2000) 22 4 NA Yes
(38)
Navin (2001) (39) 136 97 No (e) No (f)
weeks
Visconti (2001) 20 8 NA No
(24)
Ma (2002) (25) 107 9 No (g) No
4 weeks
Author (y) (ref) Comments
Kazanjian (1998) Both patients with DHPS mutations who were
(19) treated with TMP-SMX responded to
treatment.
Mei (1998) (37) 2 patients with DHPS mutations were treated
with TMP-SMX: 1 did not respond to TMP-SMX
(but responded to pentamidine); 1
responded to TMP-SMX.
Helweg-Larsen DHPS mutation was an independent predictor
(1999) (20) associated with increased deaths (OR = 3.1,
p = 0.01).
19 patients with DHPS mutations were
treated with TMP-SMX: 7 died; 12 (63%)
responded and survived.
Ma (1999) (21)
Kazanjian (2000) Patients with DHPS mutations were more
(22) likely (RR = 2.1, p = 0.01) to fail
TMP-SMX or dapsone-containing treatment.
Nevertheless, 15 (71%) of 21 patients
with DHPS mutations who were treated with
TMP-SMX or dapsone-containing regimen
responded to treatment.
Takahashi (2000) All 4 patients with DHPS mutations who were
(38) treated with TMP-SMX did not respond to
treatment.
Navin (2001) (39) 66 patients with DHPS mutations were
treated with TMP-SMX: 56 (85%) responded.
Visconti (2001) 1 of 3 patients with DHPS mutations did not
(24) respond to TMP-SMX treatment.
Ma (2002) (25)
(a) DHPS, dihydropteroate synthase; PCP, Pneumocystis pneumonia;
TMP-SMX, trimethoprim-sulfamethoxazole; NA, not available.
(b) Assessed at 3 months.
(c) Assessed at 4 weeks.
(d) Defined as the following: a) deterioration after 7 days
of therapy (worsening clinical features or gas exchange
parameters--alveolar-arterial [O.sub.2] gradient increase
[greater than or equal to] 20 mm Hg from baseline--when
available); b) failure of clinical findings to improve after
10 days of therapy; c) physician perception of failure.
(e) Assessed at 6 weeks. Results were similar whether deaths
were defined as from all cause or restricted to cases in
which PCP was the primary cause of death.
(f) PCP treatment response defined as the following: a) patient
completed full course of initial treatment and responded;
b) patient responded sufficiently to be discharged on oral
medication; c) patient responded to initial treatment but was
given another medication because of adverse effects. Results
were similar when analysis was restricted to patients who had
received at least 7 days of initial PCP treatment.
(g) Assessed at 4 weeks. Deaths included were restricted
to cases in which PCP was the primary cause of death.
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Antimicrob Agents Chemother. 2000;44:991-6. (17.) Volpe F, Dyer M, Scaife JG, Darby G, Stammers DK, Delves CJ. The multifunctional folic acid synthesis fas gene of Pneumocystis carinii appears to encode dihydropteroate synthase and hydroxymethyldihydropterin pyrophosphokinase. Gene. 1992;112:213-8. (18.) Lane BR, Ast JC, Hossler PA, Mindell DP, Bartlett MS, Smith JW, et al. Dihydropteroate synthase polymorphisms in Pneumocystis carinii. J Infect Dis. 1997;175:482-5. (19.) Kazanjian P, Locke AB, Hossler PA, Lane BR, Bartlett MS, Smith JW, et al. Pneumocystis carinii mutations associated with sulfa and sulfone prophylaxis failures in AIDS patients. AIDS. 1998;12:873-8. (20.) Helweg-Larsen J, Benfield TL, Eugen-Olsen J, Lundgren JD, Lundgren B. Effects of mutations in Pneumocystis carinii dihydropteroate synthase gene on outcome of AIDS-associated P. carinii pneumonia. Lancet. 1999;354:1347-51. (21.) Ma L, Borio L, Masur H, Kovacs JA. 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Mutations in the dihydropteroate synthase gene of human-derived Pneumocystis carinii isolates from Italy are infrequent but correlate with prior sulfa prophylaxis. J Infect Dis. 2002;185:1530-2. (26.) Ma L, Kovacs JA. Genetic analysis of multiple loci loci [L.] plural of locus. loci Plural of locus, see there suggests that mutations in the Pneumocysis carinii f. sp. hominis dihydropteroate synthase gene arose independently in multiple strains. Antimicrob Agents Chemother. 2001;45:3213-5. (27.) Demanche C, Guillot J, Berthelemy M, Petitt T, Roux Roux , Pierre Paul Émile 1853-1933. French bacteriologist. His work with the diphtheria bacillus led to the development of antitoxins to neutralize pathogenic toxins. P, Wakefield AE. Absence of mutations associated with sulfa resistance in Pneumocystis carinii dihydropteroate synthase gene from non-human primates. Med Mycol. 2002;40:315-8. (28.) Kai M, Matsuoka M, Nakata N, Maeda S, Gidoh M, Maeda Y, et al. Diaminodiphenylsulfone resistance of Mycobacterium leprae due to mutations in the dihydropteroate synthase gene. FEMS FEMS Federation of European Microbiological Societies FEMS Federation of European Materials Societies FEMS Fabrication Engineering Management System FEMS Facility Equipment Maintenance System (PMEL/TMDE) Microbiol Lett. 1999;177:231-5. (29.) Costa MC, Helweg-Larsen J, Lundgren B, Antunes F, Matos O. Mutations in the dihydropteroate synthase gene of Pneumocystis jirovecii isolates from Portuguese patients with Pneumocystis pneumonia. Int J Antimicrob Agents. 2003;22:516-20. (30.) Nahimana A, Rabodonirina M, Zanetti G, Meneau I, Francioli P, Bille J, et al. Association between a specific Pneumocystis jiroveci dihydropteroate synthase mutation and failure of pyrimethamine/sulfadoxine prophylaxis in human immunodeficiency virus-positive and -negative patients. J Infect Dis. 2003;188:1017-23. (31.) Miller RF, Lindley AR, Ambrose HE, Malin AS, Wakefield AE. Genotypes of Pneumocystis jiroveci isolates obtained in Harare, Zimbabwe, and London, United Kingdom. Antimicrob Agents Chemother. 2003;47:3979-81. (32.) Beard CB, Carter JL, Keely SP, Huang L, Pieniazek NJ, Moura IN, et al. Genetic variation in Pneumocystis carinii isolates from different geographic regions: implications for transmission. Emerg Infect Dis. 2000;6:265-72. (33.) Huang L, Friedly J, Morris AM, Carter JL, Turner JR, Merrifield C, et al. Pneumocystis carinii dihydropteroate synthase genotypes in HIV-infected persons residing in San Francisco: possible implications for disease transmission. J Eukaryot Microbiol. 2001;48:137S-8. (34.) Latouche S, Lacube P, Maury E, Bolognini J, Develous M, Girard PM, et al. Pneumocystis jirovecii dihydropteroate synthase genotypes in French patients with pneumocystosis: a 1998-2001 prospective study. Med Mycol. 2003;41:533-7. (35.) Crothers K, Huang L, Morris A, Fox M, Groner G, Turner JR, et al. Pneumocystis dihydropteroate synthase mutations in patients with Pneumocystis pneumonia who are newly diagnosed with HIV infection. J Eukaryot Microbiol. 2003;50(Suppl):609-10. (36.) Takahashi T, Endo T, Nakamura T, Sakashitat H, Kimurat K, Ohnishit K, et al. Dihydrofolate reductase gene polymorphisms in Pneumocystis carinii f. sp. hominis in Japan. J Med Microbiol. 2002;51:510-5. (37.) Mei Q, Gurunathan S, Masur H, Kovacs JA. Failure of co-trimoxazole in Pneumocystis carinii infection and mutations in dihydropteroate synthase gene. Lancet. 1998;351:1631-2. (38.) Takahashi T, Hosoya N, Endo T, Nakamura T, Sakashita H, Kimura K, et al. Relationship between mutations in dihydropteroate synthase Of Pneumocystis carinii f. sp. hominis isolates in Japan and resistance to sulfonamide therapy. J Clin Microbiol. 2000;38:3161-4. (39.) Navin TR, Beard CB, Huang L, del Rio Del Rio (rē`ō), city (1990 pop. 30,705), seat of Val Verde co., W Tex., on the Rio Grande opposite Ciudad Acuña, Mexico; founded 1868, inc. 1911. C, Lee S, Pieniazek NJ, et al. Effect of mutations in Pneumocystis carinii dihydropteroate synthase gene on outcome of P. carinii pneumonia in patients with HIV-1: a prospective study. Lancet. 2001;358:545-9. (40.) Huang L, Morris AM, Beard CB. Pneumocystis carinii dihydropteroate synthase mutations and treatment with sulfa or sulfone regimens: a proposal for standardized definitions for clinical evaluation clinical evaluation Medtalk An evaluation of whether a Pt has symptoms of a disease, is responding to treatment, or is having adverse reactions to therapy . J Eukaryot Microbiol. 2001;48:180S-1. Address for correspondence: Laurence Huang, Positive Health Program, Ward 84, San Francisco General Hospital San Francisco General Hospital is the main public hospital in San Francisco, California, and the only Level I Trauma Center serving San Francisco and San Mateo. The hospital budget is for only 302 beds at SFGH. , 995 Potrero Avenue, San Francisco, CA 94110, USA; fax: 415-476-6953; email: lhuang@ php.ucsf.edu Dr. Huang is supported by the National Institutes of Health K23 HL072117. Dr. Huang is an associate professor of medicine at the University of California The University of California has a combined student body of more than 191,000 students, over 1,340,000 living alumni, and a combined systemwide and campus endowment of just over $7.3 billion (8th largest in the United States). San Francisco and an attending physician in the Department of Medicine at San Francisco General Hospital. He holds dual appointments in the Positive Health Program for HIV/AIDS and the Division of Pulmonary and Critical Care Medicine at San Francisco General Hospital. His clinical and research interests are focused on HIV-associated pulmonary diseases, especially Pneumocystis pneumonia. Laurence Huang, * Kristina Crothers, * Chiara Atzori, ([dagger]) Thomas Benfield, ([double dagger double dagger n. A reference mark (  ) used in printing and writing. Also called diesis.Noun 1. ]) Robert Miller, ([section]) Meja Rabodonirina, ([paragraph]) and Jannik Helweg-Larsen (#) * University of California San Francisco, San Francisco, California “San Francisco” redirects here. For other uses, see San Francisco (disambiguation). The City and County of San Francisco (EN IPA: [sænfrənˈsɪskoʊ] , USA; ([dagger]) Luigi Sacco Hospital, Milan, Italy; ([double dagger]) HS Rigshospitalet, Copenhagen, Denmark; ([section]) University College London “UCL” redirects here. For other uses, see UCL (disambiguation). University College London, commonly known as UCL, is the oldest multi-faculty constituent college of the University of London, one of the two original founding colleges, and the first British , London, United Kingdom; ([paragraph]) Hospital de la Croiz-Rousse, Lyon, France; and (#) Hvidovre University Hospital, Copenhagen, Denmark |
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