Data Wrangling and Analyses with Tidyverse

Last updated on 2024-11-19 | Edit this page

Estimated time: 55 minutes

Overview

Questions

  • How can I manipulate data frames without repeating myself?

Objectives

  • Describe what the dplyr package in R is used for.
  • Apply common dplyr functions to manipulate data in R.
  • Employ the ‘pipe’ operator to link together a sequence of functions.
  • Employ the ‘mutate’ function to apply other chosen functions to existing columns and create new columns of data.
  • Employ the ‘split-apply-combine’ concept to split the data into groups, apply analysis to each group, and combine the results.

Bracket subsetting is handy, but it can be cumbersome and difficult to read, especially for complicated operations.

Luckily, the dplyr package provides a number of very useful functions for manipulating data frames in a way that will reduce repetition, reduce the probability of making errors, and probably even save you some typing. As an added bonus, you might even find the dplyr grammar easier to read.

Here we’re going to cover some of the most commonly used functions as well as using pipes (%>%) to combine them:

  1. glimpse()
  2. select()
  3. filter()
  4. group_by()
  5. summarize()
  6. mutate()
  7. pivot_longer and pivot_wider

Packages in R are sets of additional functions that let you do more stuff in R. The functions we’ve been using, like str(), come built into R; packages give you access to more functions. You need to install a package and then load it to be able to use it.

R

install.packages("dplyr") ## installs dplyr package
install.packages("tidyr") ## installs tidyr package
install.packages("ggplot2") ## installs ggplot2 package
install.packages("readr") ## install readr package

You might get asked to choose a CRAN mirror – this is asking you to choose a site to download the package from. The choice doesn’t matter too much; I’d recommend choosing the RStudio mirror.

R

library("dplyr")          ## loads in dplyr package to use
library("tidyr")          ## loads in tidyr package to use
library("ggplot2")          ## loads in ggplot2 package to use
library("readr")          ## load in readr package to use

You only need to install a package once per computer, but you need to load it every time you open a new R session and want to use that package.

Tip: Installing packages

It may be temping to install the tidyverse package, as it contains many useful collection of packages for this lesson and beyond. However, when teaching or following this lesson, we advise that participants install dplyr, readr, ggplot2, and tidyr individually as shown above. Otherwise, a substaial amount of the lesson will be spend waiting for the installation to complete.

What is dplyr?


The package dplyr is a fairly new (2014) package that tries to provide easy tools for the most common data manipulation tasks. This package is also included in the tidyverse package, which is a collection of eight different packages (dplyr, ggplot2, tibble, tidyr, readr, purrr, stringr, and forcats). It is built to work directly with data frames. The thinking behind it was largely inspired by the package plyr which has been in use for some time but suffered from being slow in some cases.dplyr addresses this by porting much of the computation to C++. An additional feature is the ability to work with data stored directly in an external database. The benefits of doing this are that the data can be managed natively in a relational database, queries can be conducted on that database, and only the results of the query returned.

This addresses a common problem with R in that all operations are conducted in memory and thus the amount of data you can work with is limited by available memory. The database connections essentially remove that limitation in that you can have a database that is over 100s of GB, conduct queries on it directly and pull back just what you need for analysis in R.

Loading .csv files in tidy style

The Tidyverse’s readr package provides its own unique way of loading .csv files in to R using read_csv(), which is similar to read.csv(). read_csv() allows users to load in their data faster, doesn’t create row names, and allows you to access non-standard variable names (ie. variables that start with numbers of contain spaces), and outputs your data on the R console in a tidier way. In short, it’s a much friendlier way of loading in potentially messy data.

Now let’s load our vcf .csv file using read_csv():

Taking a quick look at data frames

Similar to str(), which comes built into R, glimpse() is a dplyr function that (as the name suggests) gives a glimpse of the data frame.

OUTPUT

Rows: 801
Columns: 29
$ sample_id     <chr> "SRR2584863", "SRR2584863", "SRR2584863", "SRR2584863", …
$ CHROM         <chr> "CP000819.1", "CP000819.1", "CP000819.1", "CP000819.1", …
$ POS           <dbl> 9972, 263235, 281923, 433359, 473901, 648692, 1331794, 1…
$ ID            <lgl> NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, …
$ REF           <chr> "T", "G", "G", "CTTTTTTT", "CCGC", "C", "C", "G", "ACAGC…
$ ALT           <chr> "G", "T", "T", "CTTTTTTTT", "CCGCGC", "T", "A", "A", "AC…
$ QUAL          <dbl> 91.0000, 85.0000, 217.0000, 64.0000, 228.0000, 210.0000,…
$ FILTER        <lgl> NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, …
$ INDEL         <lgl> FALSE, FALSE, FALSE, TRUE, TRUE, FALSE, FALSE, FALSE, TR…
$ IDV           <dbl> NA, NA, NA, 12, 9, NA, NA, NA, 2, 7, NA, NA, NA, NA, NA,…
$ IMF           <dbl> NA, NA, NA, 1.000000, 0.900000, NA, NA, NA, 0.666667, 1.…
$ DP            <dbl> 4, 6, 10, 12, 10, 10, 8, 11, 3, 7, 9, 20, 12, 19, 15, 10…
$ VDB           <dbl> 0.0257451, 0.0961330, 0.7740830, 0.4777040, 0.6595050, 0…
$ RPB           <dbl> NA, 1.000000, NA, NA, NA, NA, NA, NA, NA, NA, 0.900802, …
$ MQB           <dbl> NA, 1.0000000, NA, NA, NA, NA, NA, NA, NA, NA, 0.1501340…
$ BQB           <dbl> NA, 1.000000, NA, NA, NA, NA, NA, NA, NA, NA, 0.750668, …
$ MQSB          <dbl> NA, NA, 0.974597, 1.000000, 0.916482, 0.916482, 0.900802…
$ SGB           <dbl> -0.556411, -0.590765, -0.662043, -0.676189, -0.662043, -…
$ MQ0F          <dbl> 0.000000, 0.166667, 0.000000, 0.000000, 0.000000, 0.0000…
$ ICB           <lgl> NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, …
$ HOB           <lgl> NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, NA, …
$ AC            <dbl> 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1,…
$ AN            <dbl> 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1,…
$ DP4           <chr> "0,0,0,4", "0,1,0,5", "0,0,4,5", "0,1,3,8", "1,0,2,7", "…
$ MQ            <dbl> 60, 33, 60, 60, 60, 60, 60, 60, 60, 60, 25, 60, 10, 60, …
$ Indiv         <chr> "/home/dcuser/dc_workshop/results/bam/SRR2584863.aligned…
$ gt_PL         <dbl> 1210, 1120, 2470, 910, 2550, 2400, 2080, 2550, 11128, 19…
$ gt_GT         <dbl> 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1, 1,…
$ gt_GT_alleles <chr> "G", "T", "T", "CTTTTTTTT", "CCGCGC", "T", "A", "A", "AC…

In the above output, we can already gather some information about variants, such as the number of rows and columns, column names, type of vector in the columns, and the first few entries of each column. Although what we see is similar to outputs of str(), this method gives a cleaner visual output.

Selecting columns and filtering rows

To select columns of a data frame, use select(). The first argument to this function is the data frame (variants), and the subsequent arguments are the columns to keep.

R

select(variants, sample_id, REF, ALT, DP)

OUTPUT

# A tibble: 801 × 4
   sample_id  REF                              ALT                            DP
   <chr>      <chr>                            <chr>                       <dbl>
 1 SRR2584863 T                                G                               4
 2 SRR2584863 G                                T                               6
 3 SRR2584863 G                                T                              10
 4 SRR2584863 CTTTTTTT                         CTTTTTTTT                      12
 5 SRR2584863 CCGC                             CCGCGC                         10
 6 SRR2584863 C                                T                              10
 7 SRR2584863 C                                A                               8
 8 SRR2584863 G                                A                              11
 9 SRR2584863 ACAGCCAGCCAGCCAGCCAGCCAGCCAGCCAG ACAGCCAGCCAGCCAGCCAGCCAGCC…     3
10 SRR2584863 AT                               ATT                             7
# ℹ 791 more rows

To select all columns except certain ones, put a “-” in front of the variable to exclude it.

R

select(variants, -CHROM)

OUTPUT

# A tibble: 801 × 28
   sample_id      POS ID    REF      ALT    QUAL FILTER INDEL   IDV    IMF    DP
   <chr>        <dbl> <lgl> <chr>    <chr> <dbl> <lgl>  <lgl> <dbl>  <dbl> <dbl>
 1 SRR2584863    9972 NA    T        G        91 NA     FALSE    NA NA         4
 2 SRR2584863  263235 NA    G        T        85 NA     FALSE    NA NA         6
 3 SRR2584863  281923 NA    G        T       217 NA     FALSE    NA NA        10
 4 SRR2584863  433359 NA    CTTTTTTT CTTT…    64 NA     TRUE     12  1        12
 5 SRR2584863  473901 NA    CCGC     CCGC…   228 NA     TRUE      9  0.9      10
 6 SRR2584863  648692 NA    C        T       210 NA     FALSE    NA NA        10
 7 SRR2584863 1331794 NA    C        A       178 NA     FALSE    NA NA         8
 8 SRR2584863 1733343 NA    G        A       225 NA     FALSE    NA NA        11
 9 SRR2584863 2103887 NA    ACAGCCA… ACAG…    56 NA     TRUE      2  0.667     3
10 SRR2584863 2333538 NA    AT       ATT     167 NA     TRUE      7  1         7
# ℹ 791 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

dplyr also provides useful functions to select columns based on their names. For instance, ends_with() allows you to select columns that ends with specific letters. For instance, if you wanted to select columns that end with the letter “B”:

R

select(variants, ends_with("B"))

OUTPUT

# A tibble: 801 × 8
      VDB   RPB   MQB   BQB   MQSB    SGB ICB   HOB
    <dbl> <dbl> <dbl> <dbl>  <dbl>  <dbl> <lgl> <lgl>
 1 0.0257    NA    NA    NA NA     -0.556 NA    NA
 2 0.0961     1     1     1 NA     -0.591 NA    NA
 3 0.774     NA    NA    NA  0.975 -0.662 NA    NA
 4 0.478     NA    NA    NA  1     -0.676 NA    NA
 5 0.660     NA    NA    NA  0.916 -0.662 NA    NA
 6 0.268     NA    NA    NA  0.916 -0.670 NA    NA
 7 0.624     NA    NA    NA  0.901 -0.651 NA    NA
 8 0.992     NA    NA    NA  1.01  -0.670 NA    NA
 9 0.902     NA    NA    NA  1     -0.454 NA    NA
10 0.568     NA    NA    NA  1.01  -0.617 NA    NA
# ℹ 791 more rows

Challenge

Create a table that contains all the columns with the letter “i” and column “POS”, without columns “Indiv” and “FILTER”. Hint: look at for a function called contains(), which can be found in the help documentation for ends with we just covered (?ends_with). Note that contains() is not case sensistive.

R

# First, we select "POS" and all columns with letter "i". This will contain columns Indiv and FILTER. 
variants_subset <- select(variants, POS, contains("i"))
# Next, we remove columns Indiv and FILTER
variants_result <- select(variants_subset, -Indiv, -FILTER)
variants_result

OUTPUT

# A tibble: 801 × 7
       POS sample_id  ID    INDEL   IDV    IMF ICB
     <dbl> <chr>      <lgl> <lgl> <dbl>  <dbl> <lgl>
 1    9972 SRR2584863 NA    FALSE    NA NA     NA
 2  263235 SRR2584863 NA    FALSE    NA NA     NA
 3  281923 SRR2584863 NA    FALSE    NA NA     NA
 4  433359 SRR2584863 NA    TRUE     12  1     NA
 5  473901 SRR2584863 NA    TRUE      9  0.9   NA
 6  648692 SRR2584863 NA    FALSE    NA NA     NA
 7 1331794 SRR2584863 NA    FALSE    NA NA     NA
 8 1733343 SRR2584863 NA    FALSE    NA NA     NA
 9 2103887 SRR2584863 NA    TRUE      2  0.667 NA
10 2333538 SRR2584863 NA    TRUE      7  1     NA
# ℹ 791 more rows

Challenge (continued)

We can also get to variants_result in one line of code:

R

variants_result <- select(variants, POS, contains("i"), -Indiv, -FILTER)
variants_result

OUTPUT

# A tibble: 801 × 7
       POS sample_id  ID    INDEL   IDV    IMF ICB
     <dbl> <chr>      <lgl> <lgl> <dbl>  <dbl> <lgl>
 1    9972 SRR2584863 NA    FALSE    NA NA     NA
 2  263235 SRR2584863 NA    FALSE    NA NA     NA
 3  281923 SRR2584863 NA    FALSE    NA NA     NA
 4  433359 SRR2584863 NA    TRUE     12  1     NA
 5  473901 SRR2584863 NA    TRUE      9  0.9   NA
 6  648692 SRR2584863 NA    FALSE    NA NA     NA
 7 1331794 SRR2584863 NA    FALSE    NA NA     NA
 8 1733343 SRR2584863 NA    FALSE    NA NA     NA
 9 2103887 SRR2584863 NA    TRUE      2  0.667 NA
10 2333538 SRR2584863 NA    TRUE      7  1     NA
# ℹ 791 more rows

To choose rows, use filter():

R

filter(variants, sample_id == "SRR2584863")

OUTPUT

# A tibble: 25 × 29
   sample_id  CHROM        POS ID    REF   ALT    QUAL FILTER INDEL   IDV    IMF
   <chr>      <chr>      <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl>  <dbl>
 1 SRR2584863 CP000819… 9.97e3 NA    T     G        91 NA     FALSE    NA NA
 2 SRR2584863 CP000819… 2.63e5 NA    G     T        85 NA     FALSE    NA NA
 3 SRR2584863 CP000819… 2.82e5 NA    G     T       217 NA     FALSE    NA NA
 4 SRR2584863 CP000819… 4.33e5 NA    CTTT… CTTT…    64 NA     TRUE     12  1
 5 SRR2584863 CP000819… 4.74e5 NA    CCGC  CCGC…   228 NA     TRUE      9  0.9
 6 SRR2584863 CP000819… 6.49e5 NA    C     T       210 NA     FALSE    NA NA
 7 SRR2584863 CP000819… 1.33e6 NA    C     A       178 NA     FALSE    NA NA
 8 SRR2584863 CP000819… 1.73e6 NA    G     A       225 NA     FALSE    NA NA
 9 SRR2584863 CP000819… 2.10e6 NA    ACAG… ACAG…    56 NA     TRUE      2  0.667
10 SRR2584863 CP000819… 2.33e6 NA    AT    ATT     167 NA     TRUE      7  1
# ℹ 15 more rows
# ℹ 18 more variables: DP <dbl>, VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>,
#   MQSB <dbl>, SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>,
#   AN <dbl>, DP4 <chr>, MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>,
#   gt_GT_alleles <chr>

filter() will keep all the rows that match the conditions that are provided. Here are a few examples:

R

# rows for which the reference genome has T or G
filter(variants, REF %in% c("T", "G"))

OUTPUT

# A tibble: 340 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 9.97e3 NA    T     G      91   NA     FALSE    NA    NA     4
 2 SRR25848… CP00… 2.63e5 NA    G     T      85   NA     FALSE    NA    NA     6
 3 SRR25848… CP00… 2.82e5 NA    G     T     217   NA     FALSE    NA    NA    10
 4 SRR25848… CP00… 1.73e6 NA    G     A     225   NA     FALSE    NA    NA    11
 5 SRR25848… CP00… 2.62e6 NA    G     T      31.9 NA     FALSE    NA    NA    12
 6 SRR25848… CP00… 3.00e6 NA    G     A     225   NA     FALSE    NA    NA    15
 7 SRR25848… CP00… 3.91e6 NA    G     T     225   NA     FALSE    NA    NA    10
 8 SRR25848… CP00… 9.97e3 NA    T     G     214   NA     FALSE    NA    NA    10
 9 SRR25848… CP00… 1.06e4 NA    G     A     225   NA     FALSE    NA    NA    11
10 SRR25848… CP00… 6.40e4 NA    G     A     225   NA     FALSE    NA    NA    18
# ℹ 330 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

R

# rows that have TRUE in the column INDEL
filter(variants, INDEL)

OUTPUT

# A tibble: 101 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 4.33e5 NA    CTTT… CTTT…  64   NA     TRUE     12 1        12
 2 SRR25848… CP00… 4.74e5 NA    CCGC  CCGC… 228   NA     TRUE      9 0.9      10
 3 SRR25848… CP00… 2.10e6 NA    ACAG… ACAG…  56   NA     TRUE      2 0.667     3
 4 SRR25848… CP00… 2.33e6 NA    AT    ATT   167   NA     TRUE      7 1         7
 5 SRR25848… CP00… 3.90e6 NA    A     AC     43.4 NA     TRUE      2 1         2
 6 SRR25848… CP00… 4.43e6 NA    TGG   T     228   NA     TRUE     10 1        10
 7 SRR25848… CP00… 1.48e5 NA    AGGGG AGGG… 122   NA     TRUE      8 1         8
 8 SRR25848… CP00… 1.58e5 NA    GTTT… GTTT…  19.5 NA     TRUE      6 1         6
 9 SRR25848… CP00… 1.73e5 NA    CAA   CA    180   NA     TRUE     11 1        11
10 SRR25848… CP00… 1.75e5 NA    GAA   GA    194   NA     TRUE     10 1        10
# ℹ 91 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

R

# rows that don't have missing data in the IDV column
filter(variants, !is.na(IDV))

OUTPUT

# A tibble: 101 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 4.33e5 NA    CTTT… CTTT…  64   NA     TRUE     12 1        12
 2 SRR25848… CP00… 4.74e5 NA    CCGC  CCGC… 228   NA     TRUE      9 0.9      10
 3 SRR25848… CP00… 2.10e6 NA    ACAG… ACAG…  56   NA     TRUE      2 0.667     3
 4 SRR25848… CP00… 2.33e6 NA    AT    ATT   167   NA     TRUE      7 1         7
 5 SRR25848… CP00… 3.90e6 NA    A     AC     43.4 NA     TRUE      2 1         2
 6 SRR25848… CP00… 4.43e6 NA    TGG   T     228   NA     TRUE     10 1        10
 7 SRR25848… CP00… 1.48e5 NA    AGGGG AGGG… 122   NA     TRUE      8 1         8
 8 SRR25848… CP00… 1.58e5 NA    GTTT… GTTT…  19.5 NA     TRUE      6 1         6
 9 SRR25848… CP00… 1.73e5 NA    CAA   CA    180   NA     TRUE     11 1        11
10 SRR25848… CP00… 1.75e5 NA    GAA   GA    194   NA     TRUE     10 1        10
# ℹ 91 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

We have a column titled “QUAL”. This is a Phred-scaled confidence score that a polymorphism exists at this position given the sequencing data. Lower QUAL scores indicate low probability of a polymorphism existing at that site. filter() can be useful for selecting mutations that have a QUAL score above a certain threshold:

R

# rows with QUAL values greater than or equal to 100
filter(variants, QUAL >= 100)

OUTPUT

# A tibble: 666 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 2.82e5 NA    G     T       217 NA     FALSE    NA  NA      10
 2 SRR25848… CP00… 4.74e5 NA    CCGC  CCGC…   228 NA     TRUE      9   0.9    10
 3 SRR25848… CP00… 6.49e5 NA    C     T       210 NA     FALSE    NA  NA      10
 4 SRR25848… CP00… 1.33e6 NA    C     A       178 NA     FALSE    NA  NA       8
 5 SRR25848… CP00… 1.73e6 NA    G     A       225 NA     FALSE    NA  NA      11
 6 SRR25848… CP00… 2.33e6 NA    AT    ATT     167 NA     TRUE      7   1       7
 7 SRR25848… CP00… 2.41e6 NA    A     C       104 NA     FALSE    NA  NA       9
 8 SRR25848… CP00… 2.45e6 NA    A     C       225 NA     FALSE    NA  NA      20
 9 SRR25848… CP00… 2.67e6 NA    A     T       225 NA     FALSE    NA  NA      19
10 SRR25848… CP00… 3.00e6 NA    G     A       225 NA     FALSE    NA  NA      15
# ℹ 656 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

filter() allows you to combine multiple conditions. You can separate them using a , as arguments to the function, they will be combined using the & (AND) logical operator. If you need to use the | (OR) logical operator, you can specify it explicitly:

R

# this is equivalent to:
#   filter(variants, sample_id == "SRR2584863" & QUAL >= 100)
filter(variants, sample_id == "SRR2584863", QUAL >= 100)

OUTPUT

# A tibble: 19 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 2.82e5 NA    G     T       217 NA     FALSE    NA  NA      10
 2 SRR25848… CP00… 4.74e5 NA    CCGC  CCGC…   228 NA     TRUE      9   0.9    10
 3 SRR25848… CP00… 6.49e5 NA    C     T       210 NA     FALSE    NA  NA      10
 4 SRR25848… CP00… 1.33e6 NA    C     A       178 NA     FALSE    NA  NA       8
 5 SRR25848… CP00… 1.73e6 NA    G     A       225 NA     FALSE    NA  NA      11
 6 SRR25848… CP00… 2.33e6 NA    AT    ATT     167 NA     TRUE      7   1       7
 7 SRR25848… CP00… 2.41e6 NA    A     C       104 NA     FALSE    NA  NA       9
 8 SRR25848… CP00… 2.45e6 NA    A     C       225 NA     FALSE    NA  NA      20
 9 SRR25848… CP00… 2.67e6 NA    A     T       225 NA     FALSE    NA  NA      19
10 SRR25848… CP00… 3.00e6 NA    G     A       225 NA     FALSE    NA  NA      15
11 SRR25848… CP00… 3.34e6 NA    A     C       211 NA     FALSE    NA  NA      10
12 SRR25848… CP00… 3.40e6 NA    C     A       225 NA     FALSE    NA  NA      14
13 SRR25848… CP00… 3.48e6 NA    A     G       200 NA     FALSE    NA  NA       9
14 SRR25848… CP00… 3.49e6 NA    A     C       225 NA     FALSE    NA  NA      13
15 SRR25848… CP00… 3.91e6 NA    G     T       225 NA     FALSE    NA  NA      10
16 SRR25848… CP00… 4.10e6 NA    A     G       225 NA     FALSE    NA  NA      16
17 SRR25848… CP00… 4.20e6 NA    A     C       225 NA     FALSE    NA  NA      11
18 SRR25848… CP00… 4.43e6 NA    TGG   T       228 NA     TRUE     10   1      10
19 SRR25848… CP00… 4.62e6 NA    A     C       185 NA     FALSE    NA  NA       9
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

R

# using `|` logical operator
filter(variants, sample_id == "SRR2584863", (MQ >= 50 | QUAL >= 100))

OUTPUT

# A tibble: 23 × 29
   sample_id  CHROM        POS ID    REF   ALT    QUAL FILTER INDEL   IDV    IMF
   <chr>      <chr>      <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl>  <dbl>
 1 SRR2584863 CP000819… 9.97e3 NA    T     G        91 NA     FALSE    NA NA
 2 SRR2584863 CP000819… 2.82e5 NA    G     T       217 NA     FALSE    NA NA
 3 SRR2584863 CP000819… 4.33e5 NA    CTTT… CTTT…    64 NA     TRUE     12  1
 4 SRR2584863 CP000819… 4.74e5 NA    CCGC  CCGC…   228 NA     TRUE      9  0.9
 5 SRR2584863 CP000819… 6.49e5 NA    C     T       210 NA     FALSE    NA NA
 6 SRR2584863 CP000819… 1.33e6 NA    C     A       178 NA     FALSE    NA NA
 7 SRR2584863 CP000819… 1.73e6 NA    G     A       225 NA     FALSE    NA NA
 8 SRR2584863 CP000819… 2.10e6 NA    ACAG… ACAG…    56 NA     TRUE      2  0.667
 9 SRR2584863 CP000819… 2.33e6 NA    AT    ATT     167 NA     TRUE      7  1
10 SRR2584863 CP000819… 2.41e6 NA    A     C       104 NA     FALSE    NA NA
# ℹ 13 more rows
# ℹ 18 more variables: DP <dbl>, VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>,
#   MQSB <dbl>, SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>,
#   AN <dbl>, DP4 <chr>, MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>,
#   gt_GT_alleles <chr>

Challenge

Select all the mutations that occurred between the positions 1e6 (one million) and 2e6 (inclusive) that have a QUAL greater than 200, and exclude INDEL mutations. Hint: to flip logical values such as TRUE to a FALSE, we can use to negation symbol “!”. (eg. !TRUE == FALSE).

R

filter(variants, POS >= 1e6 & POS <= 2e6, QUAL > 200, !INDEL)

OUTPUT

# A tibble: 77 × 29
   sample_id CHROM    POS ID    REF   ALT    QUAL FILTER INDEL   IDV   IMF    DP
   <chr>     <chr>  <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl> <dbl> <dbl>
 1 SRR25848… CP00… 1.73e6 NA    G     A       225 NA     FALSE    NA    NA    11
 2 SRR25848… CP00… 1.00e6 NA    A     G       225 NA     FALSE    NA    NA    15
 3 SRR25848… CP00… 1.02e6 NA    A     G       225 NA     FALSE    NA    NA    12
 4 SRR25848… CP00… 1.06e6 NA    C     T       225 NA     FALSE    NA    NA    17
 5 SRR25848… CP00… 1.06e6 NA    A     G       206 NA     FALSE    NA    NA     9
 6 SRR25848… CP00… 1.07e6 NA    G     T       225 NA     FALSE    NA    NA    11
 7 SRR25848… CP00… 1.07e6 NA    T     C       225 NA     FALSE    NA    NA    12
 8 SRR25848… CP00… 1.10e6 NA    C     T       225 NA     FALSE    NA    NA    15
 9 SRR25848… CP00… 1.11e6 NA    C     T       212 NA     FALSE    NA    NA     9
10 SRR25848… CP00… 1.11e6 NA    A     G       225 NA     FALSE    NA    NA    14
# ℹ 67 more rows
# ℹ 17 more variables: VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>, MQSB <dbl>,
#   SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>, AN <dbl>, DP4 <chr>,
#   MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>, gt_GT_alleles <chr>

Pipes

But what if you wanted to select and filter? We can do this with pipes. Pipes, are a fairly recent addition to R. Pipes let you take the output of one function and send it directly to the next, which is useful when you need to many things to the same data set. It was possible to do this before pipes were added to R, but it was much messier and more difficult. Pipes in R look like %>% and are made available via the magrittr package, which is installed as part of dplyr. If you use RStudio, you can type the pipe with Ctrl + Shift + M if you’re using a PC, or Cmd + Shift + M if you’re using a Mac.

R

variants %>%
  filter(sample_id == "SRR2584863") %>%
  select(REF, ALT, DP)

OUTPUT

# A tibble: 25 × 3
   REF                              ALT                                       DP
   <chr>                            <chr>                                  <dbl>
 1 T                                G                                          4
 2 G                                T                                          6
 3 G                                T                                         10
 4 CTTTTTTT                         CTTTTTTTT                                 12
 5 CCGC                             CCGCGC                                    10
 6 C                                T                                         10
 7 C                                A                                          8
 8 G                                A                                         11
 9 ACAGCCAGCCAGCCAGCCAGCCAGCCAGCCAG ACAGCCAGCCAGCCAGCCAGCCAGCCAGCCAGCCAGC…     3
10 AT                               ATT                                        7
# ℹ 15 more rows

In the above code, we use the pipe to send the variants data set first through filter(), to keep rows where sample_id matches a particular sample, and then through select() to keep only the REF, ALT, and DP columns. Since %>% takes the object on its left and passes it as the first argument to the function on its right, we don’t need to explicitly include the data frame as an argument to the filter() and select() functions any more.

Some may find it helpful to read the pipe like the word “then”. For instance, in the above example, we took the data frame variants, then we filtered for rows where sample_id was SRR2584863, then we selected the REF, ALT, and DP columns. The dplyr functions by themselves are somewhat simple, but by combining them into linear workflows with the pipe, we can accomplish more complex manipulations of data frames.

If we want to create a new object with this smaller version of the data we can do so by assigning it a new name:

R

SRR2584863_variants <- variants %>%
  filter(sample_id == "SRR2584863") %>%
  select(REF, ALT, DP)

This new object includes all of the data from this sample. Let’s look at just the first six rows to confirm it’s what we want:

R

SRR2584863_variants

OUTPUT

# A tibble: 25 × 3
   REF                              ALT                                       DP
   <chr>                            <chr>                                  <dbl>
 1 T                                G                                          4
 2 G                                T                                          6
 3 G                                T                                         10
 4 CTTTTTTT                         CTTTTTTTT                                 12
 5 CCGC                             CCGCGC                                    10
 6 C                                T                                         10
 7 C                                A                                          8
 8 G                                A                                         11
 9 ACAGCCAGCCAGCCAGCCAGCCAGCCAGCCAG ACAGCCAGCCAGCCAGCCAGCCAGCCAGCCAGCCAGC…     3
10 AT                               ATT                                        7
# ℹ 15 more rows

Similar to head() and tail() functions, we can also look at the first or last six rows using tidyverse function slice(). Slice is a more versatile function that allows users to specify a range to view:

R

SRR2584863_variants %>% slice(1:6)

OUTPUT

# A tibble: 6 × 3
  REF      ALT          DP
  <chr>    <chr>     <dbl>
1 T        G             4
2 G        T             6
3 G        T            10
4 CTTTTTTT CTTTTTTTT    12
5 CCGC     CCGCGC       10
6 C        T            10

R

SRR2584863_variants %>% slice(10:25)

OUTPUT

# A tibble: 16 × 3
   REF   ALT      DP
   <chr> <chr> <dbl>
 1 AT    ATT       7
 2 A     C         9
 3 A     C        20
 4 G     T        12
 5 A     T        19
 6 G     A        15
 7 A     C        10
 8 C     A        14
 9 A     G         9
10 A     C        13
11 A     AC        2
12 G     T        10
13 A     G        16
14 A     C        11
15 TGG   T        10
16 A     C         9

Exercise: Pipe and filter

Starting with the variants data frame, use pipes to subset the data to include only observations from SRR2584863 sample, where the filtered depth (DP) is at least 10. Showing only 5th through 11th rows of columns REF, ALT, and POS.

R

 variants %>%
 filter(sample_id == "SRR2584863" & DP >= 10) %>%
 slice(5:11) %>%
 select(sample_id, DP, REF, ALT, POS)

OUTPUT

# A tibble: 7 × 5
  sample_id     DP REF   ALT       POS
  <chr>      <dbl> <chr> <chr>   <dbl>
1 SRR2584863    11 G     A     1733343
2 SRR2584863    20 A     C     2446984
3 SRR2584863    12 G     T     2618472
4 SRR2584863    19 A     T     2665639
5 SRR2584863    15 G     A     2999330
6 SRR2584863    10 A     C     3339313
7 SRR2584863    14 C     A     3401754

Mutate

Frequently you’ll want to create new columns based on the values in existing columns, for example to do unit conversions or find the ratio of values in two columns. For this we’ll use the dplyr function mutate().

For example, we can convert the polymorphism confidence value QUAL to a probability value according to the formula:

Probability = 1- 10 ^ -(QUAL/10)

We can use mutate to add a column (POLPROB) to our variants data frame that shows the probability of a polymorphism at that site given the data.

R

variants %>%
  mutate(POLPROB = 1 - (10 ^ -(QUAL/10)))

OUTPUT

# A tibble: 801 × 30
   sample_id  CHROM        POS ID    REF   ALT    QUAL FILTER INDEL   IDV    IMF
   <chr>      <chr>      <dbl> <lgl> <chr> <chr> <dbl> <lgl>  <lgl> <dbl>  <dbl>
 1 SRR2584863 CP000819… 9.97e3 NA    T     G        91 NA     FALSE    NA NA
 2 SRR2584863 CP000819… 2.63e5 NA    G     T        85 NA     FALSE    NA NA
 3 SRR2584863 CP000819… 2.82e5 NA    G     T       217 NA     FALSE    NA NA
 4 SRR2584863 CP000819… 4.33e5 NA    CTTT… CTTT…    64 NA     TRUE     12  1
 5 SRR2584863 CP000819… 4.74e5 NA    CCGC  CCGC…   228 NA     TRUE      9  0.9
 6 SRR2584863 CP000819… 6.49e5 NA    C     T       210 NA     FALSE    NA NA
 7 SRR2584863 CP000819… 1.33e6 NA    C     A       178 NA     FALSE    NA NA
 8 SRR2584863 CP000819… 1.73e6 NA    G     A       225 NA     FALSE    NA NA
 9 SRR2584863 CP000819… 2.10e6 NA    ACAG… ACAG…    56 NA     TRUE      2  0.667
10 SRR2584863 CP000819… 2.33e6 NA    AT    ATT     167 NA     TRUE      7  1
# ℹ 791 more rows
# ℹ 19 more variables: DP <dbl>, VDB <dbl>, RPB <dbl>, MQB <dbl>, BQB <dbl>,
#   MQSB <dbl>, SGB <dbl>, MQ0F <dbl>, ICB <lgl>, HOB <lgl>, AC <dbl>,
#   AN <dbl>, DP4 <chr>, MQ <dbl>, Indiv <chr>, gt_PL <dbl>, gt_GT <dbl>,
#   gt_GT_alleles <chr>, POLPROB <dbl>

Exercise

There are a lot of columns in our data set, so let’s just look at the sample_id, POS, QUAL, and POLPROB columns for now. Add a line to the above code to only show those columns.

R

variants %>%
 mutate(POLPROB = 1 - 10 ^ -(QUAL/10)) %>%
 select(sample_id, POS, QUAL, POLPROB)

OUTPUT

# A tibble: 801 × 4
   sample_id      POS  QUAL POLPROB
   <chr>        <dbl> <dbl>   <dbl>
 1 SRR2584863    9972    91    1.00
 2 SRR2584863  263235    85    1.00
 3 SRR2584863  281923   217    1
 4 SRR2584863  433359    64    1.00
 5 SRR2584863  473901   228    1
 6 SRR2584863  648692   210    1
 7 SRR2584863 1331794   178    1
 8 SRR2584863 1733343   225    1
 9 SRR2584863 2103887    56    1.00
10 SRR2584863 2333538   167    1
# ℹ 791 more rows

group_by() and summarize() functions

Many data analysis tasks can be approached using the “split-apply-combine” paradigm: split the data into groups, apply some analysis to each group, and then combine the results. dplyr makes this very easy through the use of the group_by() function, which splits the data into groups.

We can use group_by() to tally the number of mutations detected in each sample using the function tally():

R

variants %>%
  group_by(sample_id) %>%
  tally()

OUTPUT

# A tibble: 3 × 2
  sample_id      n
  <chr>      <int>
1 SRR2584863    25
2 SRR2584866   766
3 SRR2589044    10

Since counting or tallying values is a common use case for group_by(), an alternative function was created to bypasses group_by() using the function count():

R

variants %>%
  count(sample_id)

OUTPUT

# A tibble: 3 × 2
  sample_id      n
  <chr>      <int>
1 SRR2584863    25
2 SRR2584866   766
3 SRR2589044    10

Challenge

  • How many mutations are INDELs?

R

variants %>%
  count(INDEL)

OUTPUT

# A tibble: 2 × 2
  INDEL     n
  <lgl> <int>
1 FALSE   700
2 TRUE    101

When the data is grouped, summarize() can be used to collapse each group into a single-row summary. summarize() does this by applying an aggregating or summary function to each group.

It can be a bit tricky at first, but we can imagine physically splitting the data frame by groups and applying a certain function to summarize the data.

rstudio default session

1

We can also apply many other functions to individual columns to get other summary statistics. For example,we can use built-in functions like mean(), median(), min(), and max(). These are called “built-in functions” because they come with R and don’t require that you install any additional packages. By default, all R functions operating on vectors that contains missing data will return NA. It’s a way to make sure that users know they have missing data, and make a conscious decision on how to deal with it. When dealing with simple statistics like the mean, the easiest way to ignore NA (the missing data) is to use na.rm = TRUE (rm stands for remove).

So to view the mean, median, maximum, and minimum filtered depth (DP) for each sample:

R

variants %>%
  group_by(sample_id) %>%
  summarize(
    mean_DP = mean(DP),
    median_DP = median(DP),
    min_DP = min(DP),
    max_DP = max(DP))

OUTPUT

# A tibble: 3 × 5
  sample_id  mean_DP median_DP min_DP max_DP
  <chr>        <dbl>     <dbl>  <dbl>  <dbl>
1 SRR2584863    10.4      10        2     20
2 SRR2584866    10.6      10        2     79
3 SRR2589044     9.3       9.5      3     16

Grouped Data Frames in Tidyverse

When you group a data frame with group_by(), you get a grouped data frame. This is a special type of data frame that has all the properties of a regular data frame but also has an additional attribute that describes the grouping structure. The primary advantage of a grouped data frame is that it allows you to work with each group of observations as if they were a separate data frame.

Operations like summarise() and mutate() will be applied to each group separately. This is particularly useful when you want to perform calculations on subsets of your data.

To remove the grouping structure from a grouped data frame, you can use the ungroup() function. This will return a regular data frame.

For more details, refer to the dplyr documentation on grouping.

Reshaping data frames

It can sometimes be useful to transform the “long” tidy format, into the wide format. This transformation can be done with the pivot_wider() function provided by the tidyr package (also part of the tidyverse).

pivot_wider() takes a data frame as the first argument, and two arguments: the column name that will become the columns and the column name that will become the cells in the wide data.

R

variants_wide <- variants %>%
  group_by(sample_id, CHROM) %>%
  summarize(mean_DP = mean(DP)) %>%
  pivot_wider(names_from = sample_id, values_from = mean_DP)

OUTPUT

`summarise()` has grouped output by 'sample_id'. You can override using the
`.groups` argument.

R

variants_wide

OUTPUT

# A tibble: 1 × 4
  CHROM      SRR2584863 SRR2584866 SRR2589044
  <chr>           <dbl>      <dbl>      <dbl>
1 CP000819.1       10.4       10.6        9.3

The opposite operation of pivot_wider() is taken care by pivot_longer(). We specify the names of the new columns, and here add -CHROM as this column shouldn’t be affected by the reshaping:

R

variants_wide %>%
  pivot_longer(-CHROM, names_to = "sample_id", values_to = "mean_DP")

OUTPUT

# A tibble: 3 × 3
  CHROM      sample_id  mean_DP
  <chr>      <chr>        <dbl>
1 CP000819.1 SRR2584863    10.4
2 CP000819.1 SRR2584866    10.6
3 CP000819.1 SRR2589044     9.3

Resources

Key Points

  • Use the dplyr package to manipulate data frames.
  • Use glimpse() to quickly look at your data frame.
  • Use select() to choose variables from a data frame.
  • Use filter() to choose data based on values.
  • Use mutate() to create new variables.
  • Use group_by() and summarize() to work with subsets of data.

  1. The figure was adapted from the Software Carpentry lesson, R for Reproducible Scientific Analysis↩︎