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ICD-10-CM Specific Coding Guidelines - (begin 21:31) Neoplasms Part TWO

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let's continue our discussion your poll

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question asked you whether or not you

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knew that there

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were six classifications of neoplasms

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when coding and you all knew that so

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let's

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review we have primary cancer or

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malignancy this is where the cancer

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origin

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originates we also have secondary cancer

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or

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malignancy this secondary cancer results

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from the primary and we call this

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metastasis or it has

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metastasized also we have

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insitu this is a form of malignancy but

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it's not always malignant just to let

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you know that it can be malignant or it

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may not be malignant

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but this type of malany is confined to

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us to the site of origin without

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invading the ne neighboring tissue so

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it's pretty much

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contained also we have

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benign the this is not a malignancy but

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these are abnormal non-cancerous

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cells we also have uncertain neoplasms

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that means the provider can't determine

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the nature of the neoplasm so they don't

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know if it's malignant or not and

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finally

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unspecified there's insufficient

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information in the medical record to

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assign a specific

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code these are the meanings of these

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classifications and some I just want to

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kind of drive

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home a little bit about the nature or

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the evolution of

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cancer so in this um this represents the

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prostate and I'm going to try and show

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you how cancer evolves I'm going to try

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all right so the first image represents

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normal cells found within the prostate

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gland the

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second this is where you see the normal

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cells begin to grow and multiply and

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these are benign cells they're not

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cancerous so we're going to call them

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benign but when those benign cells

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continue to grow and

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multiply and they begin to damage other

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cells within the prostate

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gland and they

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even these start becoming classified as

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malignancy or they can be malignant or

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they are are okay in this

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exercise and this is lowgrade

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malignancy now they become highgrade

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when you have significant structural

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damage of that gland and it's caused by

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these cells becoming aggressive and look

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at the mutation they've mutated into

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something that could look like a

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tumor right and at this stage the

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Cancer's aggressive and the patient is

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really

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sick and if that isn't enough the

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aggressive cancer cells begin to move to

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other parts of the body like bone and

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this is what we

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call secondary cancer another word for

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secondary

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metastasis or the cancer has metastasi

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so the first two images are benign cells

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um they're uncertain cells or

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unspecified

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cells the next two represent primary

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cancer or insitu or insitu cancer and

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then the last image represents secondary

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cancer and I'm finished and I'mma let

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that Marin

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hopefully it helps understand helps you

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as a coder understand how prostate or

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how cancer

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evolves how normal cells

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evolve better now let's get to

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our icd1 CM let's take a look at

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it and let's just observe the columns in

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the neoplasm

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table this neoplasms table is in the

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index it's in the alphabetic index it's

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after the guidelines it's yeah it's

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after the guidelines right there and

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these six

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classifications are found at the top of

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the um table so the First Column all of

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the codes within the first

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colum Cancer all of the

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second secondary cancer and we also call

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this cancer Mets or metastasize

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or um secondary cancer then you have

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your cancer in

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situ

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benign

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uncertain and

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unspecified

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behavior and when your documentation

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specifies the type of cancer that's

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where you get your

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code now let's talk a little more about

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this neoplasms

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table well the first thing all cancers

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are not coded from this table not all

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cancers but your malignancies pretty

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much are the types of cancers that are

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not coated using this table are

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typically your om your

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saroma lipoma that's not necessarily a

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cancer but it could be

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neoplasma also adoma

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carcinoma they are not from this

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chart or table but where can you find

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it of course you can find it in the

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alphabetic

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index so you may say well don't we go to

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the alphabetic index first

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anyway

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right not for neoplasms you can go right

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to the neoplasms table and then verify

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in the tabular

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list I'mma say it again you can go right

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to the neoplasms table look up your code

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then verify it in the tabular

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list all right coders I'm a lot and I

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want to know how you're doing you're

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doing

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good people say they're doing great okay

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another thing I want to tell you about

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these um columns the first three are

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cancerous cancer and situ um can be

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cancerous or or not so we're going to

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put it in the cancerous um section and

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the last three are not cancerous they're

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not considered

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cancerous now let's go ahead and let's

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code together using this neoplasms

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table all

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right a patient arrives to the

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oncologist to receive treatment for

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prostate

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cancer all right I got a question which

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cancer are we coding

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for well it's pretty obvious right we

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only have one cancer and that's prostate

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cancer and this prostate cancer it

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defaults to primary when you're coding

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for the exam if there's no mention

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that this is secondary cancer the

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default is

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primary all right so let's go look up

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this code all right so the patient

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arrives for prostate cancer so we know

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this is primary so our code is going to

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we're going to take our code from the

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First Column but I do want to point out

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that these cancers these neoplasms are

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arranged

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alphabetically so you just pretty much

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look for your cancer in alphabetical

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order so we're going to go down until we

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get to the P's and we find prostate

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cancer um c um

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CC1 c61 c79 D7 etc etc but where we find

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our code we just make sure we're in the

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correct column we know this is primary

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so we're going to look in the primary

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column and you can see what the answer

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is so we've seen that c61 is our code

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let's go ahead and

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verify so when we look in the tabular

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list c61 malignant neoplasm of

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prostate and it tells you to use

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additional code

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if applicable to identify the hormone

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sensitivity

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status and Rising PSA following

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treatment for malignant neoplasm of

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prostate so this is inapplicable our

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