Difference between revisions of "Sandbox"

Revision as of 14:16, 25 June 2012

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http://ytoswww/yhteiset/YMAL/Projects/

Edited by ehac

Failed to parse (Missing <code>texvc</code> executable. Please see math/README to configure.): L_{Aeq} = 10 \log \int_{t_0}^{t_1} \frac{p_A^2(t)}{p_0^2} dt

Failed to parse (Missing <code>texvc</code> executable. Please see math/README to configure.): \textstyle L_{Aeq} = 10 \log \int_{t_0}^{t_1} \frac{p_A^2(t)}{p_0^2} dt

Static GoogleMaps test

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#code goes here
library(RgoogleMaps)
library(rgdal)
library(maptools)
library(RColorBrewer)
library(classInt)
library(OpasnetBaseUtils)

shp<-readOGR('PG:host=localhost user=postgres dbname=spatial_db','kuopio_house')
plotvar<-shp@data$ika
nclr<-8
plotclr<-brewer.pal(nclr,"Spectral")
class<-classIntervals(plotvar,nclr,style="quantile")
colcode<-findColours(class,plotclr)

epsg4326String <- CRS("+proj=longlat +ellps=WGS84 +datum=WGS84 +no_defs")
proj4string(shp)<-("+init=epsg:3067")
shp2<-spTransform(shp,epsg4326String)
#get marker information first 10 points
mymarkers<-cbind.data.frame(lat=c(shp2@coords[,2]),lon=c(shp2@coords[,1]),color=colcode);

#get the bounding box:
bb <- qbbox(lat = mymarkers[,"lat"], lon = mymarkers[,"lon"])

#MyMap function without the "file destination" parameter
MyRmap<-function (lonR, latR, center, size = c(640, 640),  
    MINIMUMSIZE = FALSE, RETURNIMAGE = TRUE, GRAYSCALE = FALSE, 
    NEWMAP = TRUE, zoom, verbose = 1, ...) 
{
    if (missing(zoom)) 
        zoom <- min(MaxZoom(latR, lonR, size))
    if (missing(center)) {
        lat.center <- mean(latR)
        lon.center <- mean(lonR)
    }
    else {
        lat.center <- center[1]
        lon.center <- center[2]
    }
    if (MINIMUMSIZE) {
        ll <- LatLon2XY(latR[1], lonR[1], zoom)
        ur <- LatLon2XY(latR[2], lonR[2], zoom)
        cr <- LatLon2XY(lat.center, lon.center, zoom)
        ll.Rcoords <- Tile2R(ll, cr)
        ur.Rcoords <- Tile2R(ur, cr)
        if (verbose > 1) {
            cat("ll:")
            print(ll)
            print(ll.Rcoords)
            cat("ur:")
            print(ur)
            print(ur.Rcoords)
            cat("cr:")
            print(cr)
        }
        size[1] <- 2 * max(c(ceiling(abs(ll.Rcoords$X)), ceiling(abs(ur.Rcoords$X)))) + 
            1
        size[2] <- 2 * max(c(ceiling(abs(ll.Rcoords$Y)), ceiling(abs(ur.Rcoords$Y)))) + 
            1
        if (verbose) 
            cat("new size: ", size, "\n")
    }
    return(GetMap(center = c(lat.center, lon.center), zoom = zoom, 
        size = size, RETURNIMAGE = RETURNIMAGE, 
        GRAYSCALE = GRAYSCALE, verbose = verbose, ...))
}

MyMap<-MyRmap(bb$lonR,bb$latR,maptype="mobile")

PlotOnStaticMap(MyMap)

PlotOnStaticMap(MyMap,lat=mymarkers[,"lat"],lon=mymarkers[,"lon"],pch=19,cex=0.3,col=colcode,add=T)

legend("topleft", legend=names(attr(colcode, "table")),title="Ika", fill=attr(colcode, "palette"),  cex=1.0, bty="y",bg="white")

Kuopio buildings on Google maps test

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library(rgdal)
library(maptools)
library(RColorBrewer)
library(classInt)
library(OpasnetBaseUtils)
library(RODBC)

shp <- spatial_db_query(paste('SELECT * FROM kuopio_house WHERE ika >= ',age,';',sep=''))

coordinates(shp)=c("y_koord","x_koord")

#shp<-readOGR('PG:host=localhost user=postgres dbname=spatial_db','kuopio_house')
plotvar<-shp@data$ika
nclr<-8
plotclr<-brewer.pal(nclr,"BuPu")
class<-classIntervals(plotvar,nclr,style="quantile")
colcode<-findColours(class,plotclr)

epsg4326String <- CRS("+proj=longlat +ellps=WGS84 +datum=WGS84 +no_defs")
proj4string(shp)<-("+init=epsg:3067")
shp2<-spTransform(shp,epsg4326String)


kmlname<-"Kuopio house data"
kmldescription<-"Random stuff about here"
icon<-"http://maps.google.com/mapfiles/kml/pal2/icon18.png"
name<-paste("Value: ",shp2$ika)
description <- paste("<b>Ikä:</b>",shp2$ika,"<br><b>Rakennustunnus:</b>",shp2$rakennustunnus)

MyPointKML<-function(obj = NULL, kmlname = "", kmldescription = "", name = NULL, description = "", icon = "http://maps.google.com/mapfiles/kml/pal4/icon24.png",col=NULL) 
{
    if (is.null(obj)) 
        return(list(header = c("<?xml version=\"1.0\" encoding=\"UTF-8\"?>", 
            "<kml xmlns=\"http://earth.google.com/kml/2.2\">", 
            "<Document>", paste("<name>", kmlname, "</name>", 
                sep = ""), paste("<description><![CDATA[", kmldescription, 
                "]]></description>", sep = "")), footer = c("</Document>", 
            "</kml>")))
    if (class(obj) != "SpatialPointsDataFrame") 
        stop("obj must be of class 'SpatialPointsDataFrame' [package 'sp']")
    if (is.null(name)) {
        name = c()
        for (i in 1:nrow(obj)) name <- append(name, paste("site", 
            i))
    }

    col2kmlcolor <- function(col) paste(rev(sapply(col2rgb(col, TRUE), function(x) sprintf("%02x", x))), collapse = "")
    kml <- kmlStyle <- ""
    kmlHeader <- c("<?xml version=\"1.0\" encoding=\"UTF-8\"?>","<kml xmlns=\"http://earth.google.com/kml/2.2\">", "<Document>")
    kmlFooter <- c("</Document>", "</kml>")
    for (i in 1:nrow(obj)) {
        point <- obj[i, ]
        pt_name = name[i]
        pt_description = description[i]
        pt_style <- paste("#style", ifelse(length(icon) == 1, 1, i), sep = "")
        kml <- append(kml, "<Placemark>")
        kml <- append(kml, paste("  <description><![CDATA[",pt_description, "]]></description>", sep = ""))
	#kml <- append(kml, "<Style><IconStyle>")
	#kml <- append(kml, paste("<color>", col2kmlcolor(col[i]), "</color>", sep =""))
        #kml <- append(kml, paste("  <Icon><href>", icon, "</href></Icon>", sep = ""))
	#kml <- append(kml, "<scale>0.300000</scale>")
	#kml <- append(kml, "</IconStyle></Style>")
        kml <- append(kml, "  <Point>")
        kml <- append(kml, "    <coordinates>")
        kml <- append(kml, paste(point@coords[1], point@coords[2], sep = ","))
        kml <- append(kml, "    </coordinates>")
        kml <- append(kml, "  </Point>")
        kml <- append(kml, "</Placemark>")
    }
    
    return(paste(paste(c(kmlHeader, kmlStyle, kml, kmlFooter), sep = "", collapse = "\n"), collapse="\n", sep = ""))
    
}



data <- MyPointKML(shp2,kmlname,kmldescription,name,description,icon,colcode)
google.show_kml_data_on_maps(data)

GoogleMaps Sorvi MML TEST

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library(OpasnetBaseUtils)
library(sorvi)
library(rgdal)

data(MML)

shp <- MML[["1_milj_Shape_etrs_shape"]][["kunta1_p"]]

#epsg3857String <- CRS("+proj=merc +lon_0=0 +k=1 +x_0=0 +y_0=0 +a=6378137 +b=6378137 +towgs84=0,0,0,0,0,0,0 +units=m +no_defs")
epsg4326String <- CRS("+proj=longlat +ellps=WGS84 +datum=WGS84 +no_defs")
proj4string(shp)<-("+init=epsg:3047")
shp2<-spTransform(shp,epsg4326String)

out<-sapply(slot(shp2,"polygons"),function(x){kmlPolygon(x,name="nimi",col='#df0000aa',lwd=1,border='black',description="selite") })

data<-paste(
paste(kmlPolygon(kmlname="This will be layer name", kmldescription="<i>More info about layer here</i>")$header, collapse="\n"),
paste(unlist(out["style",]), collapse="\n"),
paste(unlist(out["content",]), collapse="\n"),
paste(kmlPolygon()$footer, collapse="\n"),
sep=''
)

google.show_kml_data_on_maps(data)

GoogleMaps PostgreSQL test 2

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library(rgdal)
library(maptools)
library(RColorBrewer)
library(classInt)
library(OpasnetBaseUtils)

shp<-readOGR('PG:host=localhost user=postgres dbname=spatial_db','watson_wkt')

plotvar<-shp@data$value_inhalation
nclr<-8
plotclr<-brewer.pal(nclr,"BuPu")
class<-classIntervals(plotvar,nclr,style="quantile")
colcode<-findColours(class,plotclr)
epsg4326String <- CRS("+proj=longlat +ellps=WGS84 +datum=WGS84 +no_defs")
proj4string(shp)<-("+init=epsg:3035")
shp2<-spTransform(shp,epsg4326String)


out<-sapply(slot(shp2,"polygons"),function(x){kmlPolygon(x,name=as(shp2,"data.frame")[slot(x,"ID"),"country_code"],col=colcode[[((as.numeric(slot(x,"ID"))+1))]],lwd=1,border='black',description=paste("Value:",as(shp2,"data.frame")[slot(x,"ID"),"value_inhalation"])) })

data<-paste(
paste(kmlPolygon(kmlname="This will be layer name", kmldescription="<i>More info about layer here</i>")$header, collapse="\n"),
paste(unlist(out["style",]), collapse="\n"),
paste(unlist(out["content",]), collapse="\n"),
paste(kmlPolygon()$footer, collapse="\n"),
sep=''
)

google.show_kml_data_on_maps(data)

GoogleMaps PostgreSQL test

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library('OpasnetBaseUtils')
cat("<span style='font-size: 1.2em;font-weight:bold;'>PostgreSQL Test</span>\n")
google.show_data_on_maps()


google.show_data_on_maps(table='kuopio_house',database='spatial_db',fields=c('ika','ika','the_geom'))

Opasnet.csv test

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library(OpasnetBaseUtils)

csv <- opasnet.csv("2/25/Russian_elections_2011_results.csv")

print(csv[1:10,1:10])

Opasnet.data and BUGS test

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library(OpasnetBaseUtils)
pumps.model <- opasnet.data('c/cc/Test_bugs_model.txt')

library('rbugs')
data(pumps)
pumps.data <- list(t = pumps$t, x = pumps$x, N = nrow(pumps))
inits <- list(alpha = 1, beta = 1)
parameters <- c("theta", "alpha", "beta")
pumps.sim <- bugs.run(data = pumps.data, list(inits), parameters,pumps.model, n.chains = 1, n.iter = 1000)
## MCMC Analysis
library("coda")
pumps.mcmc <- as.mcmc(pumps.sim$chain1)
summary(pumps.mcmc)
effectiveSize(pumps.mcmc)
## End(Not run)

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# This code does not work. Should test the one in test wiki but i don't remember the location.
library(rjags)
N <- 1000
x <- rnorm(N, 0, 5)
 
example.bug <- "model {
	for (i in 1:N) {
		x[i] ~ dnorm(mu, tau)
	}
	mu ~ dnorm(0, .0001)
	tau <- pow(sigma, -2)
	sigma ~ dunif(0, 100)
}"

jags.model

jags <- jags.model(example1.bug,
                   data = list('x' = x,
                               'N' = N),
                   n.chains = 4,
                   n.adapt = 100)
 
update(jags, 1000)
 
jags.samples(jags,
             c('mu', 'tau'),
             1000)

Failed to parse (Missing <code>texvc</code> executable. Please see math/README to configure.): \alpha 444 + 9999 / 123

Hello

this works

Bluebox

works
ok

R-tools code include example

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cat("Above should be included code\n")

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library(OpasnetBaseUtils)
library(ggplot2)
library(xtable)

saanto.siemenet <- op_baseGetData("opasnet_base", "Op_fi2633")[,-c(1,2,7)] # Jatropan siementen saanto viljelystä
saanto.öljy     <- op_baseGetData("opasnet_base", "Op_fi2634")[,-c(1,2,5)] # Öljyn saanto jatropan siemenistä
saanto.diesel   <- op_baseGetData("opasnet_base", "Op_fi2632")[,-c(1,2,5)] # Biodieselin saanto jatropaöljystä
viljelyala      <- op_baseGetData("opasnet_base", "Op_fi2642")[,-c(1,2)] # Jatropan viljelyalueet
päästö.ilmasto  <- op_baseGetData("opasnet_base", "Op_fi2547")[,-c(1,2)] # Jatropan viljelyn ilmastovaikutukset
päästö.sosiaali <- op_baseGetData("opasnet_base", "Op_fi2552")[,-c(1,2)] # Jatropan viljelyn sosiaaliset vaikutukset
päästö.ekosyst  <- op_baseGetData("opasnet_base", "Op_fi2548")[,-c(1,2)] # Jatropan viljelyn ekosysteemivaikutukset
P               <- op_baseGetData("opasnet_base", "Op_fi2539")[,-c(1,2,7)] # Jatropan käyttö bioenergian lähteenä

colnames(saanto.siemenet)[4] <- "siemenet"
colnames(saanto.öljy)[2] <- "öljy"
colnames(saanto.diesel)[2] <- "diesel"
saanto <- merge(saanto.siemenet, saanto.öljy)
saanto <- merge(saanto, saanto.diesel)
saanto[,9] <- saanto$siemenet * saanto$öljy * saanto$diesel * ala
colnames(saanto)[9] <- "saanto (kg/a)"

P <- PTable(P, n)
saanto <- merge(P, saanto)

if(length(divisions)>1) divisions <- as.list(saanto[, divisions]) else divisions <- saanto[, divisions]
out1 <- as.data.frame(as.table(tapply(saanto[, 10], divisions, mean))) 
out1 <- dropall(out1[!is.na(out1$Freq), ])

print(xtable(out1), type = 'html')

out2 <- as.data.frame(as.table(tapply(saanto[, 10], list(saanto[, divisions2], saanto$obs), mean))) 
out2 <- dropall(out2[!is.na(out2$Freq), ])
out2[1:10, ]
ggplot(out2, aes(x = Freq, weight = 1, fill = Var1)) +geom_density() 
## Jostain syystä vain osa kuvista piirtyy oikein, riippuen mitä parametreja valitaan. En ymmärrä syytä.

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######################################
## dropall pudottaa data.framesta pois kaikki faktorien sellaiset levelit, joita ei käytetä.
## parametrit: x = data.frame 

dropall <- function(x){
    isFac <- NULL
    for (i in 1:dim(x)[2]){isFac[i] = is.factor(x[ , i])}

    for (i in 1:length(isFac)){
        x[, i] <- x[, i][ , drop = TRUE]
        }
    return(x)
    }
########################################

#########################################
## PTable muuntaa arvioinnin todennäköisyystaulun sopivaan muotoon arviointia varten.
## Parametrit: P = todennäköisyystaulu Opasnet-kannasta kaivettuna.
##             n = iteraatioiden lukumäärä Monte Carlossa
## Todennäköisyystaulun sarakkeiden on oltava: Muuttuja, Selite, Lokaatio, P
## Tuotteena on Monte Carloa varten tehty taulu, jonka sarakkeina ovat
## n (iteraatio) ja kaikki todennäköisyystaulussa olleet selitteet, joiden riveille on arvottu
## lokaatiot niiden todennäköisyyksien mukaisesti, jotka todennäköisyystaulussa oli annettu.

PTable <- function(P, n) {
Pt <- unique(P[,c("Muuttuja", "Selite")])
Pt <- data.frame(Muuttuja = rep(Pt$Muuttuja, n), Selite = rep(Pt$Selite, n), obs = rep(1:n, each = nrow(Pt)), P = runif(n*nrow(Pt), 0, 1))
for(i in 2:nrow(P)){P$Result[i] <- P$Result[i] + ifelse(P$Muuttuja[i] == P$Muuttuja[i-1] & P$Selite[i] == P$Selite[i-1], P$Result[i-1], 0)}
P <- merge(P, Pt)
P <- P[P$P <= P$Result, ]
Pt <- as.data.frame(as.table(tapply(P$Result, as.list(P[, c("Muuttuja", "Selite", "obs")]), min)))
colnames(Pt) <- c("Muuttuja", "Selite", "obs", "Result")
Pt <- Pt[!is.na(P$Result), ]
P <- merge(P, Pt)
P <- P[, !colnames(P) %in% c("Result", "P", "Muuttuja")]
P <- reshape(P, idvar = "obs", timevar = "Selite", v.names = "Lokaatio", direction = "wide")
colnames(P) <- ifelse(substr(colnames(P), 1, 9) == "Lokaatio.", substr(colnames(P), 10,30), colnames(P))
return(P)
}
######################################

Rectangle area test

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# The area of the rect is
width *  height

Kristiina telmii

You have error(s) in your data:

You have invalid number of data cells in row 61
You have invalid number of data cells in row 62

Difference between revisions of "Sandbox"(no unit)
Obs	Substance	CASRN	WOE 86 Guidelines	WOE Narrative	IRIS identifier
1	Acenaphthene	83-32-9	Not Assessed under the IRIS program.		0442
2	Acenaphthylene	208-96-8	D, Not classifiable as to human carcinogenicity	Based on no human data and inadequate data from animal bioassays.	0443
3	Acephate	30560-19-1	C, Possible human carcinogen	The classification is based on increased incidence of hepatocellular carcinomas and adenomas in female mice.	0354
4	Acetaldehyde	75-07-0	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Based on increased incidence of nasal tumors in male and female rats and laryngeal tumors in male and female hamsters after inhalation exposure.	0290
5	Acetochlor	34256-82-1	Not Assessed under the IRIS program.		0521
6	Acetone	67-64-1	NA, Not applicable. This substance was not assessed using the 1986 cancer guidelines (U.S. EPA, 1986).	In accordance with the Draft Revised Guidelines for Carcinogen Risk Assessment (U.S. EPA, 1999) data are inadequate for an assessment of the human carcinogenic potential of acetone.	0128
7	Acetonitrile	75-05-8	D, Not classifiable as to human carcinogenicity	Under the Proposed Guidelines for Carcinogen Risk Assessment (U.S. EPA, 1996), the carcinogenic potential of ACN following inhalation, oral, or dermal exposure is best characterized as "cannot be determined because the existing evidence is composed of conflicting data (e.g., some evidence is suggestive of carcinogenic effects, but other equally pertinent evidence does not confirm any concern)."	0205
8	Acetophenone	98-86-2	D, Not classifiable as to human carcinogenicity	Based on no human data and no animal data.	0321
9	Acetyl chloride	75-36-5	D, Not classifiable as to human carcinogenicity	No human data or animal data.	0518
10	Acifluorfen, sodium	62476-59-9	Not Assessed under the IRIS program.		0192
11	Acrolein	107-02-8	NA, Not applicable. This substance was not assessed using the 1986 cancer guidelines (U.S. EPA, 1986).	Under the Draft Revised Guidelines for Carcinogen Risk Assessment (U.S. EPA, 1999), the potential carcinogenicity of acrolein cannot be determined because the existing data are inadequate for an assessment of human carcinogenic potential for either the oral or inhalation route of exposure. There are no adequate human studies of the carcinogenic potential of acrolein. Collectively, experimental studies provide inadequate evidence that acrolein causes cancer in laboratory animals.	0364
12	Acrylamide	79-06-1	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Based on inadequate human data and sufficient evidence of carcinogenicity in animals; significantly increased incidences of benign and/or malignant tumors at multiple sites in both sexes of rats, and carcinogenic effects in a series of one-year limited bioassays in mice by several routes of exposures. The classification is supported by positive genotoxicity data, adduct formation activity, and structure-activity relationships to vinyl carbamate and acrylonitrile.	0286
13	Acrylic acid	79-10-7	Not Assessed under the IRIS program.		0002
14	Acrylonitrile	107-13-1	B1, Probable human carcinogen - based on limited evidence of carcinogenicity in humans	The observation of a statistically significant increase in incidence of lung cancer in exposed workers and observation of tumors, generally astrocytomas in the brain, in studies in two rat strains exposed by various routes (drinking water, gavage, and inhalation) forms the basis for this classification.	0206
15	Adiponitrile	111-69-3	D, Not classifiable as to human carcinogenicity	No human and no animal cancer data were available. Adiponitrile was negative for mutagenicity in Salmonella with and without activation.	0515
16	Alachlor	15972-60-8	Not Assessed under the IRIS program.		0129
17	Alar	1596-84-5	Not Assessed under the IRIS program.		0287
18	Aldicarb	116-06-3	D, Not classifiable as to human carcinogenicity	Aldicarb was not found to induce statistically significant increases in tumor incidence in mice or rats in feeding studies or mice in a skin painting study. In the feeding studies there were, however, significant trends in pituitary tumors in female rats and fibrosarcomas in the male mouse. This evidence, together with the fact that less than maximum tolerated doses were used, indicates that the available assays are inadequate to assess the carcinogenic potential of aldicarb.	0003
19	Aldicarb sulfone	1646-88-4	Not Assessed under the IRIS program.		0312
20	Aldrin	309-00-2	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Orally administered aldrin produced significant increases in tumor responses in three different strains of mice in both males and females. Tumor induction has been observed for structurally related chemicals, including dieldrin, a metabolite.	0130
21	Ally	74223-64-6	Not Assessed under the IRIS program.		0288
22	Allyl alcohol	107-18-6	Not Assessed under the IRIS program.		0004
23	Allyl chloride	107-05-1	C, Possible human carcinogen	Classification is based on a low (but biologically important) incidence of forestomach tumors in female mice and positive results in a variety of genetic toxicity tests. Allyl chloride is an alkylating agent and structurally related to probable human carcinogens.	0387
24	Aluminum phosphide	20859-73-8	Not Assessed under the IRIS program.		0005
25	Amdro	67485-29-4	Not Assessed under the IRIS program.		0207
26	Ametryn	834-12-8	Not Assessed under the IRIS program.		0208
27	4-Aminopyridine	504-24-5	D, Not classifiable as to human carcinogenicity	No human data and no animal data available.	0440
28	Amitraz	33089-61-1	Not Assessed under the IRIS program.		0334
29	Ammonia	7664-41-7	Not Assessed under the IRIS program.		0422
30	Ammonium acetate	631-61-8	D, Not classifiable as to human carcinogenicity	No human data and no animal data	0517
31	Ammonium methacrylate	16325-47-6	D, Not classifiable as to human carcinogenicity	No human data and no animal data	0516
32	Ammonium sulfamate	7773-06-0	Not Assessed under the IRIS program.		0007
33	Aniline	62-53-3	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Induction of tumors of the spleen and the body cavity in two strains of rat, and some supporting genetic toxicological evidence.	0350
34	ortho-Anisidine	90-04-0	Not Assessed under the IRIS program.		0610
35	Anthracene	120-12-7	D, Not classifiable as to human carcinogenicity	Based on no human data and inadequate data from animal bioassays.	0434
36	Antimony	7440-36-0	Not Assessed under the IRIS program.		0006
37	Antimony trioxide	1309-64-4	Not Assessed under the IRIS program.		0676
38	Apollo	74115-24-5	C, Possible human carcinogen	Based on an increase in thyroid gland follicular cell tumors in male rats and supportive findings in pituitary/thyroid hormone activity.	0008
39	Aramite	140-57-8	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Based on no human data and sufficient data from animal bioassays including increased incidence of liver tumors and/or neoplastic nodules in three strains of male and female rats and males of one strain of mice, and extrahepatic biliary system tumors in dogs following chronic oral exposure.	0473
40	Aroclor 1016	12674-11-2	Not Assessed under the IRIS program.		0462
41	Aroclor 1248	12672-29-6	Not Assessed under the IRIS program.		0649
42	Aroclor 1254	11097-69-1	Not Assessed under the IRIS program.		0389
43	Arsenic, inorganic	7440-38-2	A, Human Carcinogen	Based on sufficient evidence from human data. An increased lung cancer mortality was observed in multiple human populations exposed primarily through inhalation. Also, increased mortality from multiple internal organ cancers (liver, kidney, lung, and bladder) and an increased incidence of skin cancer were observed in populations consuming drinking water high in inorganic arsenic.	0278
44	Arsine	7784-42-1	Not Assessed under the IRIS program.		0672
45	Asbestos	1332-21-4	A, Human Carcinogen	Observation of increased mortality and incidence of lung cancer, mesotheliomas and gastrointestinal cancer in occupationally exposed workers are consistent across investigators and study populations. Animal studies by inhalation in two strains of rats showed similar findings for lung cancer and mesotheliomas. Animal evidence for carcinogenicity via ingestion is limited (male rats fed intermediate-range chrysotile fibers; i.e., >10 um length, developed benign polyps), and epidemiologic data in this regard are inadequate.	0371
46	Assure	76578-14-8	D, Not classifiable as to human carcinogenicity	Based on no human data and inadequate animal data.	0335
47	Asulam	3337-71-1	Not Assessed under the IRIS program.		0284
48	Atrazine	1912-24-9	Not Assessed under the IRIS program.		0209
49	Avermectin B1	65195-55-3	Not Assessed under the IRIS program.		0381
50	Azobenzene	103-33-3	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Azobenzene induced invasive sarcomas in the spleen and other abdominal organs in male and female F344 rats following dietary administration. It is genotoxic and may be converted to benzidine, a known human carcinogen, under the acidic conditions in the stomach.	0351
51	Barium and Compounds	7440-39-3	D, Not classifiable as to human carcinogenicity	Under the Proposed Guidelines for Carcinogenic Risk Assessment (U.S. EPA, 1996), barium is considered not likely to be carcinogenic to humans following oral exposure and its carcinogenic potential cannot be determined following inhalation exposure.	0010
52	Barium cyanide	542-62-1	Not Assessed under the IRIS program.		0009
53	Baygon	114-26-1	Not Assessed under the IRIS program.		0210
54	Bayleton	43121-43-3	Not Assessed under the IRIS program.		0131
55	Baythroid	68359-37-5	Not Assessed under the IRIS program.		0132
56	Benefin	1861-40-1	Not Assessed under the IRIS program.		0133
57	Benomyl	17804-35-2	Not Assessed under the IRIS program.		0011
58	Bentazon (Basagran)	25057-89-0	E, Evidence of non-carcinogenicity for humans	Under EPA's proposed guidelines for carcinogen risk assessment (U.S. EPA, 1996), Bentazon would be characterized as not likely to be carcinogenic to humans by any route of exposure.	0134
59	Benz[a]anthracene	56-55-3	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Based on no human data and sufficient data from animal bioassays. Benz[a]anthracene produced tumors in mice exposed by gavage; intraperitoneal, subcutaneous or intramuscular injection; and topical application. Benz[a]anthracene produced mutations in bacteria and in mammalian cells, and transformed mammalian cells in culture.	0454
60	Benzaldehyde	100-52-7	Not Assessed under the IRIS program.		0332
61	Benzene	71-43-2	A, Human Carcinogen	Under the proposed revised Carcinogen Risk Assessment Guidelines (U.S. EPA, 1996), benzene is characterized as a known human carcinogen for all routes of exposure based upon convincing human evidence as well as supporting evidence from animal studies. (U.S. EPA, 1979, 1985, 1998; ATSDR, 1997).
62		0276
63	Benzidine	92-87-5	A, Human Carcinogen	Observation of increased incidence of bladder cancer and bladder cancer-related deaths in exposed workers	0135
64	Benzo[a]pyrene (BaP)	50-32-8	B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals	Human data specifically linking benzo[a]pyrene (BAP) to a carcinogenic effect are lacking. There are, however, multiple animal studies in many species demonstrating BAP to be carcinogenic following administration by numerous routes. BAP has produced positive results in numerous genotoxicity assays.

@@ Line 489: / Line 489: @@
 Aroclor 1254|11097-69-1|Not Assessed under the IRIS program.||0389
 Arsenic, inorganic|7440-38-2|A, Human Carcinogen|	 Based on sufficient evidence from human data. An increased lung cancer mortality was observed in multiple human populations exposed primarily through inhalation. Also, increased mortality from multiple internal organ cancers (liver, kidney, lung, and bladder) and an increased incidence of skin cancer were observed in populations consuming drinking water high in inorganic arsenic.|0278
-Arsine|7784-42-1|Not Assessed under the IRIS program.||
+Arsine|7784-42-1|Not Assessed under the IRIS program.||0672
+Asbestos|1332-21-4|A, Human Carcinogen|Observation of increased mortality and incidence of lung cancer, mesotheliomas and gastrointestinal cancer in occupationally exposed workers are consistent across investigators and study populations. Animal studies by inhalation in two strains of rats showed similar findings for lung cancer and mesotheliomas. Animal evidence for carcinogenicity via ingestion is limited (male rats fed intermediate-range chrysotile fibers; i.e., >10 um length, developed benign polyps), and epidemiologic data in this regard are inadequate.|0371
+Assure|76578-14-8|D, Not classifiable as to human carcinogenicity|Based on no human data and inadequate animal data.|0335
+Asulam|3337-71-1|Not Assessed under the IRIS program.||0284
+Atrazine|1912-24-9|Not Assessed under the IRIS program.||0209
+Avermectin B1|65195-55-3|Not Assessed under the IRIS program.||0381
+Azobenzene|103-33-3|B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals|Azobenzene induced invasive sarcomas in the spleen and other abdominal organs in male and female F344 rats following dietary administration. It is genotoxic and may be converted to benzidine, a known human carcinogen, under the acidic conditions in the stomach.|0351
+Barium and Compounds|7440-39-3|D, Not classifiable as to human carcinogenicity|Under the Proposed Guidelines for Carcinogenic Risk Assessment (U.S. EPA, 1996), barium is considered not likely to be carcinogenic to humans following oral exposure and its carcinogenic potential cannot be determined following inhalation exposure.|0010
+Barium cyanide|542-62-1|Not Assessed under the IRIS program.||0009
+Baygon|114-26-1|Not Assessed under the IRIS program.||0210
+Bayleton|43121-43-3|Not Assessed under the IRIS program.||0131
+Baythroid|68359-37-5|Not Assessed under the IRIS program.||0132
+Benefin|1861-40-1|Not Assessed under the IRIS program.||0133
+Benomyl|17804-35-2|Not Assessed under the IRIS program.||0011
+Bentazon (Basagran)|25057-89-0|E, Evidence of non-carcinogenicity for humans|Under EPA's proposed guidelines for carcinogen risk assessment (U.S. EPA, 1996), Bentazon would be characterized as not likely to be carcinogenic to humans by any route of exposure.|0134
+Benz[a]anthracene|56-55-3|B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals|Based on no human data and sufficient data from animal bioassays. Benz[a]anthracene produced tumors in mice exposed by gavage; intraperitoneal, subcutaneous or intramuscular injection; and topical application. Benz[a]anthracene produced mutations in bacteria and in mammalian cells, and transformed mammalian cells in culture.|0454
+Benzaldehyde|100-52-7|Not Assessed under the IRIS program.||0332
+Benzene|71-43-2|A, Human Carcinogen|Under the proposed revised Carcinogen Risk Assessment Guidelines (U.S. EPA, 1996), benzene is characterized as a known human carcinogen for all routes of exposure based upon convincing human evidence as well as supporting evidence from animal studies. (U.S. EPA, 1979, 1985, 1998; ATSDR, 1997).
+|0276
+Benzidine|92-87-5|A, Human Carcinogen|Observation of increased incidence of bladder cancer and bladder cancer-related deaths in exposed workers|0135
+Benzo[a]pyrene (BaP)|50-32-8|B2, Probable human carcinogen - based on sufficient evidence of carcinogenicity in animals|Human data specifically linking benzo[a]pyrene (BAP) to a carcinogenic effect are lacking. There are, however, multiple animal studies in many species demonstrating BAP to be carcinogenic following administration by numerous routes. BAP has produced positive results in numerous genotoxicity assays.|
 </t2b>

Difference between revisions of "Sandbox"

Revision as of 14:16, 25 June 2012

Contents

Static GoogleMaps test

Kuopio buildings on Google maps test

GoogleMaps Sorvi MML TEST

GoogleMaps PostgreSQL test 2

GoogleMaps PostgreSQL test

Opasnet.csv test

Opasnet.data and BUGS test

Hello

Bluebox

R-tools code include example

Rectangle area test

Kristiina telmii

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