VistA-ccr/p/GPLRIMA.m

GPLRIMA   ; CCDCCR/GPL - RIM REPORT ROUTINES; 6/6/08
 ;;0.1;CCDCCR;nopatch;noreleasedate
 ;Copyright 2008 WorldVistA.  Licensed under the terms of the GNU
 ;General Public License See attached copy of the License.
 ;
 ;This program is free software; you can redistribute it and/or modify
 ;it under the terms of the GNU General Public License as published by
 ;the Free Software Foundation; either version 2 of the License, or
 ;(at your option) any later version.
 ;
 ;This program is distributed in the hope that it will be useful,
 ;but WITHOUT ANY WARRANTY; without even the implied warranty of
 ;MERCHANTABILITY or FITNESS FOR A PARTICULAR PURPOSE.  See the
 ;GNU General Public License for more details.
 ;
 ;You should have received a copy of the GNU General Public License along
 ;with this program; if not, write to the Free Software Foundation, Inc.,
 ;51 Franklin Street, Fifth Floor, Boston, MA 02110-1301 USA.
 ;
 ; THESE ROUTINES EXAMINE ONE OR MORE, UP TO ALL, OF THE PATIENTS ON THE
 ; SYSTEM TO DETERMINE HOW COMPLETE THE RESULTING CCR OR CCD WOULD BE FOR
 ; THESE PATIENTS. IT BEGINS TO MEASURE "HL7 RIM COHERENCE" WHICH IS HOW USEFUL
 ; THE VARIABLES WILL BE TO A RIM-MODELED APPLICATION AFTER THEY ARE
 ; CONVEYED VIA THE CCR OR CCD.
 ; FACTORS THAT AFFECT RIM COHERENCE INCLUDE:
 ;    1. THE PRESENSE OF CLINICAL DATA IN A SECTION
 ;    2. ARE THE DATA ELEMENTS TIME-BOUND
 ;    3. ARE THE DATA ELEMENTS CODED WITH SNOMED OR LOINC ETC
 ;    4. ARE SOURCE ACTORS ASSOCIATED WITH THE DATA ELEMENTS
 ;    5. ARE ACTORS IDENTIFIED REGARDING THEIR ROLE
 ;    .. AND OTHER FACTORS YET TO BE DETERMINED
 ;
 ;    SINCE THESE MEASUREMENTS ARE DONE AT THE VARIABLE LEVEL, THEY
 ;    REFLECT ON RIM COHERENCE WHETHER THE CCR OR THE CCD IS USED FOR
 ;    CONVEYANCE TO THE RIM APPLICATION.
 ;
 ;
ANALYZE(BEGDFN,DFNCNT) ; RIM COHERANCE ANALYSIS ROUTINE
    ; BEGINS AT BEGDFN AND GOES FOR DFNCNT PATIENTS
    ; TO RESUME AT NEXT PATIENT, USE BEGDFN=""
    ; USE RESET^GPLRIMA TO RESET TO TOP OF PATIENT LIST
    ;
    N RIMARY,RIMTMP,RIMI,RIMDFN,RATTR
    N CCRGLO
    D ASETUP ; SET UP VARIABLES AND GLOBALS
    D AINIT ; INITIALIZE ATTRIBUTE VALUE TABLE
    I '$D(@RIMBASE@("RESUME")) S @RIMBASE@("RESUME")=$O(^DPT(0)) ; FIRST TIME
    S RESUME=@RIMBASE@("RESUME") ; WHERE WE LEFT OFF LAST RUN
    S RIMDFN=BEGDFN ; BEGIN WITH THE BEGDFN PATIENT
    I RIMDFN="" S RIMDFN=RESUME
    I +RIMDFN=0 D  Q ; AT THE END OF THE PATIENTS
    . W "END OF PATIENT LIST, CALL RESET^GPLRIMA",!
    F RIMI=1:1:DFNCNT  D  Q:+RIMDFN=0 ; FOR DFNCNT NUMBER OF PATIENTS OR END
    . D CCRRPC^GPLCCR(.CCRGLO,RIMDFN,"CCR","","","") ;PROCESS THE CCR
    . W RIMDFN,!
    . K @RIMBASE@("VARS",RIMDFN) ; CLEAR OUT OLD VARS
    . ;
    . ; COPY ALL THE VARIABLES TO THE RIM MAP AREA INDEXED BY PATIENT
    . ;
    . I $D(^TMP("GPLCCR",$J,"PROBVALS",1)) D  ; PROBLEM VARS EXISTS
    . . M @RIMBASE@("VARS",RIMDFN,"PROBLEMS")=^TMP("GPLCCR",$J,"PROBVALS")
    . I $D(^TMP("GPLCCR",$J,"VITALS",1)) D  ; VITALS VARS EXISTS
    . . M @RIMBASE@("VARS",RIMDFN,"VITALS")=^TMP("GPLCCR",$J,"VITALS")
    . I $D(^TMP("GPLCCR",$J,"MEDICATIONS",1)) D  ; MEDS VARS EXISTS
    . . M @RIMBASE@("VARS",RIMDFN,"MEDS")=^TMP("GPLCCR",$J,"MEDICATIONS")
    . ;
    . ; EVALUATE THE VARIABLES AND CREATE AN ATTRIBUTE MAP
    . ;
    . S RATTR=$$SETATTR(RIMDFN) ; SET THE ATTRIBUTE STRING BASED ON THE VARS
    . S @RIMBASE@("ATTR",RIMDFN)=RATTR ; SAVE THE ATRIBUTES FOR THIS PAT
    . ;
    . ; INCREMENT THE COUNT OF PATIENTS WITH THESE ATTRIBUTES IN ATTRTBL
    . ;
    . I '$D(@RIMBASE@("ATTRTBL",RATTR)) D  ; IF FIRST PAT WITH THESE ATTRS
    . . S @RIMBASE@("ATTRTBL",RATTR)=0 ; DEFAULT VALUE TO BE INCREMENTED
    . S @RIMBASE@("ATTRTBL",RATTR)=@RIMBASE@("ATTRTBL",RATTR)+1 ; INCREMENT
    . ;
    . S RIMDFN=$O(^DPT(RIMDFN)) ; NEXT PATIENT
    S @RIMBASE@("RESUME")=RIMDFN ; WHERE WE ARE LEAVING OFF THIS RUN
    ; D PARY^GPLXPATH(@RIMBASE@("ATTRTBL"))
    Q
    ;
SETATTR(SDFN) ; SET ATTRIBUTES BASED ON VARS
    N SBASE,SATTR
    S SBASE=$NA(@RIMBASE@("VARS",SDFN))
    D APOST("SATTR","RIMTBL","HEADER")
    I $D(@SBASE@("PROBLEMS",1)) D  ;
    . D APOST("SATTR","RIMTBL","PROBLEMS")
    . W "POSTING PROBLEMS",!
    I $D(@SBASE@("VITALS",1)) D APOST("SATTR","RIMTBL","VITALS")
    I $D(@SBASE@("MEDS",1)) D APOST("SATTR","RIMTBL","MEDS")
    W "ATTRIBUTES: ",SATTR,!
    Q SATTR
    ;
RESET ; KILL RESUME INDICATOR TO START OVER. ALSO KILL RIM TMP VALUES
    K ^TMP("GPLRIM","RESUME")
    K ^TMP("GPLRIM")
    Q
    ;
APUSH(AMAP,AVAL) ; ADD AVAL TO ATTRIBUTE MAP AMAP (AMAP PASSED BY NAME)
    ; AMAP IS FORMED FOR ARRAY ACCESS: AMAP(0) IS THE COUNT
    ; AND AMAP(N)=AVAL IS THE NTH AVAL
    ; ALSO HASH ACCESS AMAP(AVAL)=N WHERE N IS THE ASSIGNED ORDER OF THE
    ; MAP VALUE. INSTANCES OF THE MAP WILL USE $P(X,U,N)=AVAL TO PLACE
    ; THE ATTRIBUTE IN ITS RIGHT PLACE. THE ATTRIBUTE VALUE IS STORED
    ; SO THAT DIFFERENT MAPS CAN BE AUTOMATICALLY CROSSWALKED
    ;
    I '$D(@AMAP) D  ; IF THE MAP DOES NOT EXIST
    . S @AMAP@(0)=0 ; HAS ZERO ELEMENTS
    S @AMAP@(0)=@AMAP@(0)+1 ;INCREMENT ELEMENT COUNT
    S @AMAP@(@AMAP@(0))=AVAL ; ADD THE VALUE TO THE ARRAY
    S @AMAP@(AVAL)=@AMAP@(0) ; ADD THE VALUE TO THE HASH WITH ARRAY REF
    Q
    ;
ASETUP ; SET UP GLOBALS AND VARS RIMBASE AND RIMTBL
      I '$D(RIMBASE) S RIMBASE=$NA(^TMP("GPLRIM"))
      I '$D(@RIMBASE) S @RIMBASE=""
      I '$D(RIMTBL) S RIMTBL=$NA(^TMP("GPLRIM","RIMTBL")) ;BASE FOR ATTR TABLE
      S ^TMP("GPLRIM","TABLES","RIMTBL")=RIMTBL ; FOR COMMAND LINE PROCESSING
      Q
      ;
AINIT ; INITIALIZE ATTRIBUTE TABLE
      I '$D(RIMBASE) D ASETUP ; FOR COMMAND LINE CALLS
      K @RIMTBL
      D APUSH(RIMTBL,"HEADER")
      D APUSH(RIMTBL,"NOPCP")
      D APUSH(RIMTBL,"PCP")
      D APUSH(RIMTBL,"PROBLEMS")
      D APUSH(RIMTBL,"PROBCODE")
      D APUSH(RIMTBL,"PROBNOCODE")
      D APUSH(RIMTBL,"PROBDATE")
      D APUSH(RIMTBL,"PROBNODATE")
      D APUSH(RIMTBL,"VITALS")
      D APUSH(RIMTBL,"VITALSCODE")
      D APUSH(RIMTBL,"VITALSNOCODE")
      D APUSH(RIMTBL,"VITALSDATE")
      D APUSH(RIMTBL,"VITALSNODATE")
      D APUSH(RIMTBL,"MEDS")
      D APUSH(RIMTBL,"MEDSCODE")
      D APUSH(RIMTBL,"MEDSNOCODE")
      D APUSH(RIMTBL,"MEDSDATE")
      D APUSH(RIMTBL,"MEDSNODATE")
      Q
      ;
APOST(PRSLT,PTBL,PVAL) ; POST AN ATTRIBUTE PVAL TO PRSLT USING PTBL
    ; PSRLT AND PTBL ARE PASSED BY NAME. PVAL IS A STRING
    ; PTBL IS THE NAME OF A TABLE IN @RIMBASE@("TABLES") - "RIMTBL"=ALL VALUES
    ; PVAL WILL BE PLACED IN THE STRING PRSLT AT $P(X,U,@PTBL@(PVAL))
    I '$D(RIMBASE) D ASETUP ; FOR COMMANDLINE PROCESSING
    N USETBL
    I '$D(@RIMBASE@("TABLES",PTBL)) D  Q ; NO TABLE
    . W "ERROR NO SUCH TABLE",!
    S USETBL=@RIMBASE@("TABLES",PTBL)
    S $P(@PRSLT,U,@USETBL@(PVAL))=PVAL
    Q
add initial batch RIM Coherence analysis programs 2008-08-19 19:53:29 -04:00			`GPLRIMA ; CCDCCR/GPL - RIM REPORT ROUTINES; 6/6/08`
			`;;0.1;CCDCCR;nopatch;noreleasedate`
			`;Copyright 2008 WorldVistA. Licensed under the terms of the GNU`
			`;General Public License See attached copy of the License.`
			`;`
			`;This program is free software; you can redistribute it and/or modify`
			`;it under the terms of the GNU General Public License as published by`
			`;the Free Software Foundation; either version 2 of the License, or`
			`;(at your option) any later version.`
			`;`
			`;This program is distributed in the hope that it will be useful,`
			`;but WITHOUT ANY WARRANTY; without even the implied warranty of`
			`;MERCHANTABILITY or FITNESS FOR A PARTICULAR PURPOSE. See the`
			`;GNU General Public License for more details.`
			`;`
			`;You should have received a copy of the GNU General Public License along`
			`;with this program; if not, write to the Free Software Foundation, Inc.,`
			`;51 Franklin Street, Fifth Floor, Boston, MA 02110-1301 USA.`
			`;`
			`; THESE ROUTINES EXAMINE ONE OR MORE, UP TO ALL, OF THE PATIENTS ON THE`
			`; SYSTEM TO DETERMINE HOW COMPLETE THE RESULTING CCR OR CCD WOULD BE FOR`
			`; THESE PATIENTS. IT BEGINS TO MEASURE "HL7 RIM COHERENCE" WHICH IS HOW USEFUL`
			`; THE VARIABLES WILL BE TO A RIM-MODELED APPLICATION AFTER THEY ARE`
			`; CONVEYED VIA THE CCR OR CCD.`
			`; FACTORS THAT AFFECT RIM COHERENCE INCLUDE:`
			`; 1. THE PRESENSE OF CLINICAL DATA IN A SECTION`
			`; 2. ARE THE DATA ELEMENTS TIME-BOUND`
			`; 3. ARE THE DATA ELEMENTS CODED WITH SNOMED OR LOINC ETC`
			`; 4. ARE SOURCE ACTORS ASSOCIATED WITH THE DATA ELEMENTS`
			`; 5. ARE ACTORS IDENTIFIED REGARDING THEIR ROLE`
			`; .. AND OTHER FACTORS YET TO BE DETERMINED`
			`;`
			`; SINCE THESE MEASUREMENTS ARE DONE AT THE VARIABLE LEVEL, THEY`
			`; REFLECT ON RIM COHERENCE WHETHER THE CCR OR THE CCD IS USED FOR`
			`; CONVEYANCE TO THE RIM APPLICATION.`
			`;`
			`;`
			`ANALYZE(BEGDFN,DFNCNT) ; RIM COHERANCE ANALYSIS ROUTINE`
			`; BEGINS AT BEGDFN AND GOES FOR DFNCNT PATIENTS`
			`; TO RESUME AT NEXT PATIENT, USE BEGDFN=""`
			`; USE RESET^GPLRIMA TO RESET TO TOP OF PATIENT LIST`
			`;`
			`N RIMARY,RIMTMP,RIMI,RIMDFN,RATTR`
			`N CCRGLO`
			`D ASETUP ; SET UP VARIABLES AND GLOBALS`
			`D AINIT ; INITIALIZE ATTRIBUTE VALUE TABLE`
			`I '$D(@RIMBASE@("RESUME")) S @RIMBASE@("RESUME")=$O(^DPT(0)) ; FIRST TIME`
			`S RESUME=@RIMBASE@("RESUME") ; WHERE WE LEFT OFF LAST RUN`
			`S RIMDFN=BEGDFN ; BEGIN WITH THE BEGDFN PATIENT`
			`I RIMDFN="" S RIMDFN=RESUME`
			`I +RIMDFN=0 D Q ; AT THE END OF THE PATIENTS`
			`. W "END OF PATIENT LIST, CALL RESET^GPLRIMA",!`
			`F RIMI=1:1:DFNCNT D Q:+RIMDFN=0 ; FOR DFNCNT NUMBER OF PATIENTS OR END`
			`. D CCRRPC^GPLCCR(.CCRGLO,RIMDFN,"CCR","","","") ;PROCESS THE CCR`
			`. W RIMDFN,!`
			`. K @RIMBASE@("VARS",RIMDFN) ; CLEAR OUT OLD VARS`
			`. ;`
			`. ; COPY ALL THE VARIABLES TO THE RIM MAP AREA INDEXED BY PATIENT`
			`. ;`
			`. I $D(^TMP("GPLCCR",$J,"PROBVALS",1)) D ; PROBLEM VARS EXISTS`
			`. . M @RIMBASE@("VARS",RIMDFN,"PROBLEMS")=^TMP("GPLCCR",$J,"PROBVALS")`
			`. I $D(^TMP("GPLCCR",$J,"VITALS",1)) D ; VITALS VARS EXISTS`
			`. . M @RIMBASE@("VARS",RIMDFN,"VITALS")=^TMP("GPLCCR",$J,"VITALS")`
			`. I $D(^TMP("GPLCCR",$J,"MEDICATIONS",1)) D ; MEDS VARS EXISTS`
			`. . M @RIMBASE@("VARS",RIMDFN,"MEDS")=^TMP("GPLCCR",$J,"MEDICATIONS")`
			`. ;`
			`. ; EVALUATE THE VARIABLES AND CREATE AN ATTRIBUTE MAP`
			`. ;`
			`. S RATTR=$$SETATTR(RIMDFN) ; SET THE ATTRIBUTE STRING BASED ON THE VARS`
			`. S @RIMBASE@("ATTR",RIMDFN)=RATTR ; SAVE THE ATRIBUTES FOR THIS PAT`
			`. ;`
			`. ; INCREMENT THE COUNT OF PATIENTS WITH THESE ATTRIBUTES IN ATTRTBL`
			`. ;`
			`. I '$D(@RIMBASE@("ATTRTBL",RATTR)) D ; IF FIRST PAT WITH THESE ATTRS`
			`. . S @RIMBASE@("ATTRTBL",RATTR)=0 ; DEFAULT VALUE TO BE INCREMENTED`
			`. S @RIMBASE@("ATTRTBL",RATTR)=@RIMBASE@("ATTRTBL",RATTR)+1 ; INCREMENT`
			`. ;`
			`. S RIMDFN=$O(^DPT(RIMDFN)) ; NEXT PATIENT`
			`S @RIMBASE@("RESUME")=RIMDFN ; WHERE WE ARE LEAVING OFF THIS RUN`
			`; D PARY^GPLXPATH(@RIMBASE@("ATTRTBL"))`
			`Q`
			`;`
			`SETATTR(SDFN) ; SET ATTRIBUTES BASED ON VARS`
			`N SBASE,SATTR`
			`S SBASE=$NA(@RIMBASE@("VARS",SDFN))`
killed value arrays at beginning of processing for Vitals and Problems 2008-08-19 20:47:22 -04:00			`D APOST("SATTR","RIMTBL","HEADER")`
add initial batch RIM Coherence analysis programs 2008-08-19 19:53:29 -04:00			`I $D(@SBASE@("PROBLEMS",1)) D ;`
			`. D APOST("SATTR","RIMTBL","PROBLEMS")`
			`. W "POSTING PROBLEMS",!`
			`I $D(@SBASE@("VITALS",1)) D APOST("SATTR","RIMTBL","VITALS")`
			`I $D(@SBASE@("MEDS",1)) D APOST("SATTR","RIMTBL","MEDS")`
			`W "ATTRIBUTES: ",SATTR,!`
			`Q SATTR`
			`;`
			`RESET ; KILL RESUME INDICATOR TO START OVER. ALSO KILL RIM TMP VALUES`
			`K ^TMP("GPLRIM","RESUME")`
			`K ^TMP("GPLRIM")`
			`Q`
			`;`
			`APUSH(AMAP,AVAL) ; ADD AVAL TO ATTRIBUTE MAP AMAP (AMAP PASSED BY NAME)`
			`; AMAP IS FORMED FOR ARRAY ACCESS: AMAP(0) IS THE COUNT`
			`; AND AMAP(N)=AVAL IS THE NTH AVAL`
			`; ALSO HASH ACCESS AMAP(AVAL)=N WHERE N IS THE ASSIGNED ORDER OF THE`
			`; MAP VALUE. INSTANCES OF THE MAP WILL USE $P(X,U,N)=AVAL TO PLACE`
			`; THE ATTRIBUTE IN ITS RIGHT PLACE. THE ATTRIBUTE VALUE IS STORED`
			`; SO THAT DIFFERENT MAPS CAN BE AUTOMATICALLY CROSSWALKED`
			`;`
			`I '$D(@AMAP) D ; IF THE MAP DOES NOT EXIST`
			`. S @AMAP@(0)=0 ; HAS ZERO ELEMENTS`
			`S @AMAP@(0)=@AMAP@(0)+1 ;INCREMENT ELEMENT COUNT`
			`S @AMAP@(@AMAP@(0))=AVAL ; ADD THE VALUE TO THE ARRAY`
			`S @AMAP@(AVAL)=@AMAP@(0) ; ADD THE VALUE TO THE HASH WITH ARRAY REF`
			`Q`
			`;`
			`ASETUP ; SET UP GLOBALS AND VARS RIMBASE AND RIMTBL`
			`I '$D(RIMBASE) S RIMBASE=$NA(^TMP("GPLRIM"))`
			`I '$D(@RIMBASE) S @RIMBASE=""`
			`I '$D(RIMTBL) S RIMTBL=$NA(^TMP("GPLRIM","RIMTBL")) ;BASE FOR ATTR TABLE`
			`S ^TMP("GPLRIM","TABLES","RIMTBL")=RIMTBL ; FOR COMMAND LINE PROCESSING`
			`Q`
			`;`
			`AINIT ; INITIALIZE ATTRIBUTE TABLE`
			`I '$D(RIMBASE) D ASETUP ; FOR COMMAND LINE CALLS`
			`K @RIMTBL`
			`D APUSH(RIMTBL,"HEADER")`
			`D APUSH(RIMTBL,"NOPCP")`
			`D APUSH(RIMTBL,"PCP")`
			`D APUSH(RIMTBL,"PROBLEMS")`
			`D APUSH(RIMTBL,"PROBCODE")`
			`D APUSH(RIMTBL,"PROBNOCODE")`
			`D APUSH(RIMTBL,"PROBDATE")`
			`D APUSH(RIMTBL,"PROBNODATE")`
			`D APUSH(RIMTBL,"VITALS")`
			`D APUSH(RIMTBL,"VITALSCODE")`
			`D APUSH(RIMTBL,"VITALSNOCODE")`
			`D APUSH(RIMTBL,"VITALSDATE")`
			`D APUSH(RIMTBL,"VITALSNODATE")`
			`D APUSH(RIMTBL,"MEDS")`
			`D APUSH(RIMTBL,"MEDSCODE")`
			`D APUSH(RIMTBL,"MEDSNOCODE")`
			`D APUSH(RIMTBL,"MEDSDATE")`
			`D APUSH(RIMTBL,"MEDSNODATE")`
			`Q`
			`;`
			`APOST(PRSLT,PTBL,PVAL) ; POST AN ATTRIBUTE PVAL TO PRSLT USING PTBL`
			`; PSRLT AND PTBL ARE PASSED BY NAME. PVAL IS A STRING`
			`; PTBL IS THE NAME OF A TABLE IN @RIMBASE@("TABLES") - "RIMTBL"=ALL VALUES`
			`; PVAL WILL BE PLACED IN THE STRING PRSLT AT $P(X,U,@PTBL@(PVAL))`
			`I '$D(RIMBASE) D ASETUP ; FOR COMMANDLINE PROCESSING`
			`N USETBL`
			`I '$D(@RIMBASE@("TABLES",PTBL)) D Q ; NO TABLE`
			`. W "ERROR NO SUCH TABLE",!`
			`S USETBL=@RIMBASE@("TABLES",PTBL)`
			`S $P(@PRSLT,U,@USETBL@(PVAL))=PVAL`
			`Q`